Wednesday, November 29, 2006

Opexa Therapeutics to Present at BMO Capital Markets Focus on Healthcare Conference

BMO Capital Markets Focus on Healthcare Conference

THE WOODLANDS, Texas--(BUSINESS WIRE)--Opexa Therapeutics, Inc. (NASDAQ:OPXA), a company involved in the development and commercialization of cell therapies, today announced that its chief executive officer, David McWilliams, will present at the upcoming BMO Capital Markets Focus on Healthcare Conference. The presentation is scheduled for 4:30 PM (Eastern Time) on Wednesday, December 6, 2006. The conference will be held from December 6-7, 2006 at the Millennium Broadway Hotel in New York City.

Individuals may listen to a live web cast of the presentation by logging on to the Investor Relations section of Opexas web site at www.opexatherapeutics.com a few minutes prior to start time to download any necessary software.

About Opexa Therapeutics

Opexa Therapeutics develops and commercializes cell therapies to treat autoimmune diseases such as MS, rheumatoid arthritis, and diabetes. The Company is focused on autologous cellular therapy applications of its proprietary T-cell and stem cell therapies. The Companys lead product, Tovaxin, a T-cell therapy for multiple sclerosis is in Phase IIb trials. The Company holds the exclusive worldwide license for adult multipotent stem cells derived from mononuclear cells of peripheral blood. The technology allows large quantities of monocyte derived stem cells to be produced efficiently for use in autologous therapy, thus circumventing the threat of rejection. The Company is in preclinical development for type 1 diabetes. For more information, visit the Opexa Therapeutics website at www.opexatherapeutics.com.

Contacts

Opexa Therapeutics, Inc.
Lynne Hohlfeld, 281-719-3421
lhohlfeld@opexatherapeutics.com
or
Investor Relations Contacts:
Lippert/Heilshorn & Associates
Kim Sutton Golodetz, 212-838-3777
kgolodetz@lhai.com
Bruce Voss, 310-691-7100
bvoss@lhai.com


http://home.businesswire.com/portal/site/google/index.jsp?ndmViewId=news_view&newsId=20061129005481&newsLang=en

The following are comments from patients or their families that are currently on Tysabri.

MS Patients For Choice
Beth

Infused October 25 and November 21, 2006

November 28, 2006

Both infusions came with ZERO side effects and a lessening of fatigue upon each infusion. As of November 28, 2006 I have noticed my left leg much stronger and again more strength all over. Left upper arm 'banding' feeling is now gone. Next infusion is scheduled for Dec 19, 2006 . I will then have to have my 3 month Neuro. exam. Thank you for the opportunity to 'blog' my progress.

Undisclosed

November 24, 2006

I have received 4 Tysabri infusions. I have noticed significant benefits since I’ve been on Tysabri. To me, one of the amazing benefits is that I have been able to do ½ hour step aerobics sessions, and my legs are fine afterwards. It’s amazing. I had been unable to do step aerobics for many years. It had been even longer that my legs had problems with walking after exercise. This medicine is amazing. I also have zero negative side effects after each infusion. I’m doing so well that my doctor has approved for 2 more treatments of Tysabri. My spasticity problems and balance problems are a ton better. They are significantly better.

Mike

Infused September 25, October 23 and November 20

November 2, 2006

I received two doses of Tysabri in early 2005. I am currently enrolled in the TOUCH prescription program for Tysabri therapy. I'm currently in week 6 after receiving my second dose last month. Current improvements noted are: substantial decrease in the chronic MS fatigue I have been burdened with for many years. It also seems I'm sleeping better at night and waking up feeling much more rested than before. My overall cognition seems to be improving. I am also napping much less than I had in the past. The improvements noted are very similar to the one's I experienced in 2005 after only 2 doses prior to the safety suspension. I was also recently suffering from occasional lower extremity/abdominal spasticity relapse and severe pain PRIOR to my 2 infusions in 2005 that never returned. I have noticed no adverse side effects at all and I was dosed without any Benadryl for both TOUCH infusions. I have been a long time sufferer of rheumatoid arthritis from previous sports injuries and knee surgeries. I have not been having any arthritic related pain in my knees or joints. The vision in my good eye has improved and I'm not experiencing any optic neuritis in that eye. My right eye is permanently damaged from severe optic neuritis (SON) I first experienced in 1985. I am totally blind in that eye. I don't expect my right eye to get much improvement because of the extent of damage and length of time since suffering the original exacerbation. Over all I'm very pleased at the progress I'm experiencing on Tysabri therapy. I was rated an EDSS 6 prior to initiation of TOUCH therapy. I am a previous interferon patient, Avonex (one month) and Betaseron user of almost ten years. In the previous 10 years of interferon therapy I never experienced what I'm welcoming now while on Tysabri therapy. This drug really works for me as I haven't had any problems or relapses since starting it in September. I am much less tired than I was before and also feeling much better after so many years with very little results, if any, with any of the older drugs.

Jan

Infused August 9, September 7, October 6 and November 2

November 6, 2006

My wife Janet has now received 4 infusions (since Tysabri was re-approved) and her response is very encouraging. Just prior to her first infusion she was at the lowest point in her disease progression. Her energy level was close to zero, her cognitive functions were at an all time low and her speech was very slurred. Her walking was to the point of not only using her walker but at times I would have to get on my knees and lift her feet for her and her legs were locked and she could not bend them to walk. Her vision was blurry, and her incontinence was very bad. With each infusion she has progressively improved to where her cognitive abilities are back to normal, her speech is normal, her incontinence problems have improved to the point that we can now travel to our son's home 2 !/2 hours away without any stops. Her vision has improved greatly, she is now bending her knees (not completely but much improved) and she began riding her exercise bike for short periods of time. Her hands were without feeling for about 3 to 5 years and the feeling is coming back. Her feet and legs were also without feeling and felt very heavy. As of yesterday she had some feeling back and they no longer felt heavy. Many of these improvements have come and then decreased only to return again in a few days. I would say that our feelings are all positive.

November 20, 2006

Jan continues to improve. The feeling has returned to her hands after over three years with no feeling. Now she is also having feeling return to her feet and legs after twelve years. Her walking improves from time to time so we believe that it is only a matter of more infusions before she gets that back also. She gets her fifth infusion on the afternoon of Dec. 1. Maybe that will be the one. Her speech has improved to the point where she was prior to her ever getting MS. We are both amazed at her constant improvement. It was sure great to hear that Heather's infusion went well and are hoping that improvement is not far behind.

Michele

Infused August 30, September 28 and October 31

November 10, 2006

It has been 3 months on Tysabri and my wife continues to do well. Has Tysabri eliminated her MS and all its damage? Unfortunately, no. But we never anticipated it would. However, her quality of life has greatly improved and we both feel she is on the most efficacious medicine to reduce relapses and slow the progression of additional disability.

So let's recap my wife's experiences over the last 6 months. Before Tysabri, and while on Avonex, she would receive an intramuscular injection every Tuesday evening. She could not work on Wednesdays. She could not drive on Wednesdays. All day would be spent at home with a constant headache and fatigue. She would attempt to sleep most of the day until the symptoms ended. 52 days per year, every year, were devoid of any meaningful activity. NONE of her MS symptoms improved on Avonex. The only reason she remained on Avonex was in hopes of reducing the frequency of relapses (30%) and the progression of disability (about 35%).

So how has her life changed after 3 months on Tysabri??

1. She receives her infusion early in the AM and experiences some fatigue until mid day. She has no headache, no flu-like symptoms and by the afternoon can function normally. So instead of 4.5 days / month lost (on Avonex) she loses .5 days/ month on Tysabri.

2. Her quality of life has greatly improved. While she still experiences some fatigue, she claims to have had a 70-80% improvement. There is no question regarding this improvement as I have the credit card bills from her shopping trips to back her claims. Her episodes of blurred vision have essentially ceased. This has removed many of her self imposed driving restrictions. She is more productive at work and fellow employees have stated that she appears less tired and that her eyes don't appear to close anymore. Neighbors have commented that she seems to be walking more confidently.

Lastly, and MOST important, is the fact that while on Tysabri the statistics indicate a 66% reduction in relapses and a 42% reduction in the progression of disability. There is no question in my mind that within the next 2-3 years Tysabri will emerge the dominant medicine in the treatment of MS.

There is only one factor that can stop Tysabri, PML!!! It's the wild card. We can all hope and try to convince ourselves that the risk is extremely rare. Unfortunately, no one can state with any degree of certainty (at this time) the actual risk of PML.

Lauren

Infused October 16 and November 16

Wheelchair bound, but after two infusions was able to stand briefly and take a step.

November 9, 2006

I totally freaked my caregiver out this am(lol), when he got up, and found me 1) out of bed (which I accomplished with a lot of difficulty on my part -- I won't try THAT again until after my 2nd infusion) and merrily sitting on the toilet with a fresh cup of coffee that I made for myself (while he was snoring away in his room at the other end of the house)! The first words out of his mouth were, " What the...How did you do that???" (I think I detected a slight "shrill" in his voice, and his unspoken chastisement of, "but what if you had fallen?"...ok ok).

Not much more improvement for me, other than what I've reported previously, but my small improvements have been sustained . . . for those, I am so very grateful . . .

November 19, 2006

I took my first step last night in over a year!!! Woooohoooooo! It was only one step with my right foot (with me hanging onto my caregiver, and my caregiver holding me around my waist-in the event I fell) and lifting my foot to take that step was like lifting a 25 lb weight with only one finger (it took all the strength and concentration I had, and it wasn't very graceful), but I did it! It's a good thing he had me by the waist as I collapsed afterwards (my stupid left foot was just plain frozen and would not move at all), but I started crying happy tears of joy. My hopes to walk again with Tysabri's help just went off the scale! Now I'm pushing my caregiver for more p.t. exercises, but I'm taking it slow, so no worries. Couldn't take that one step again yet to day, but maybe I can try again later tonight...

November 20, 2006

I could not take another step late last night, but I took a tiny one today with a lot of effort again on my part. However, I am not discouraged in the least, because I could stand today unassisted by my caregiver for up to 1 and 1/2 minutes while holding onto a grab-bar (he had a stopwatch -- lol), without my legs spasming and without my knees buckling under me during the time I was standing. Nice trade off if you ask me, considering I could only do this for a few seconds the day before my 2nd Tysabri infusion (11/16)! Come on December!

Midge

Infused September 21, October 19 and November 16

November 20, 2006

I had my third infusion of Tysabri on Thursday, November 16, 2006. To date, I have only experienced a slight headache the day after my first infusion. Subjectively, I am noticing a decrease in my fatigue, the ability to walk approximately 500 feet now without an assistive device (cane or scooter), and my ability to multi-task has improved.

Penny

Infused October 6 and November 3

November 4, 2006

Had my #2 infusion Friday. Everything went fine; I walked out of there with a bounce in my step, but I wasn’t dragging my left foot as much as I had been. It seems with each exacerbation my sides take turns being weak. Last time it was my left side’s turn. But ah ha I am fooling it. The big test will be when I go out to get my mail bare foot and if my left toes don’t come in scraped I will know there is progress. My fatigue seems to be held in bay. I felt so good last week I was thinking of either going back to work or going back to school and getting my doctorate – that is how positive I feel.

November 13, 2006

I walked around the mall today without a cane or walker. I’m beat but still typing.

November 13, 2006

I am tired. Did too much the last few days, and my legs feel it. I still have not felt one moment of fatigue, but my body is feeling my age. My next infusion is on December 1 st, and I am enthused and eager to get the next infusion

Chester

Infused August 18, September 15, October 13 and November 10

November 10, 2006

Now after my fourth infusion, my benefits from Tysabri have not changed from those I experienced almost immediately following my first infusion:

-- Somewhat Improved balance; and
-- Reduced side affects of minor increase in fatigue once every 4 weeks rather than Avonex flu-like side effects once per week.

The hope is that my disease is progressing at half the rate it previously was. Unfortunately, Tysabri has not affected my overall MS fatigue, nor the numbness and loss of strength on my left side causing me to limp.
© 2006 MSPATIENTSFORCHOICE

.ORG, All Rights Reserved | Disclaimer | Website by SPX Studios


http://mspatientsforchoice.org/progress.htm

Doctors Use Caution article

Your article Doctors Use Caution with Tysabri includes information from a previous Reuter's PR (about a month ago) based on a very poorly constructed and narrow survey.
As for doctor's willingness to prescribe Tysabri, I suggest you contact Dr Ted Phillips who is director of the Multiple Sclerosis Center at Texas Neurology in Dallas.
I would also suggest that you start posting some of the wonderful stories related to patients who are currently taking Tysabri.

Tuesday, November 28, 2006

ECTRIMS 2006 - New Advances in Clinical Trial Design and in the Treatment of Multiple Sclerosis CME

Disclosures

Barry A. Singer, MD

Introduction

Advances in clinical trial design and in the treatment of multiple sclerosis (MS) were presented during the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis (ECTRIMS), September 27-30, 2006, in Madrid, Spain. The highlights of new findings are reviewed, and implications for clinical practice are discussed.

Clinical Trial Design

Is it ethical to continue to have placebo arms in MS treatment clinical trials? Because therapies exist for relapsing-remitting and secondary progressive MS, randomizing patients to placebo for 2 years has become more controversial. The placebo arm has been critical in measuring the placebo effect. Relapse rates of the placebo group can be reduced by 30% to 50% as patients transition from prestudy to the active placebo phase. Without information of patients on placebo, treatment effects would be overestimated.[1]

Options to avoid a placebo trial include designs that employ add-on therapy, an external placebo group, and an active comparator. The Safety and Efficacy of Natalizumab in Combination with Avonex (interferon beta-1a) (SENTINEL) trial is an example of add-on therapy because natalizumab was added to interferon beta-1a intramuscularly in half of the trial patients. With an external placebo group, such as the Sylvia Lawry data set, all patients can also be on active treatment in a clinical trial. However, historical control groups can have very different outcomes with the same inclusion criteria. For example, patients in different secondary progressive trials of interferon beta-1b had very different disease progression results, although patients were selected with the same inclusion criteria. Active comparator trials are another option in which one treatment is compared with an existing treatment.[2] For example, the Betaferon Efficacy Yielding Outcomes of a New Dose (BEYOND) trial compares 2 doses of interferon beta-1b with glatiramer.

Criteria to ethically perform placebo trials in MS patients must start with informed consent, including the option of being randomized to not receive treatment. Patients should not have tolerated, failed, or refused current treatments. The trial design should be of short duration and have surrogate markers. Rules for patients to drop out of the trial for worsening disease should be clearly delineated. Equipoise is paramount in which the investigator is uncertain of the outcomes before placing patients on placebo.[1]

An important outcomes measure of the pivotal phase 3 MS trials has been confirmed progression of disability. Patients are considered to have confirmed progression with a documented Extended Disability Status Scale (EDSS) increase of greater than 1.0 point on 2 examinations 3-6 months apart. Butzkueven and colleagues[3] assessed whether the trial definition of "confirmed disability progression" equates with "long-term sustained" EDSS progression with the prospectively acquired global MSBase dataset. In their analysis of 4043 relapsing-remitting and secondary progressive patients from 33 contributing MS clinics, 981 had confirmed progression of disability on neurologic exams at least 3 months apart. After 2 years of confirmed disability progression in relapsing-remitting disease, 25% of patients' EDSS scores returned to baseline. After 5 years, 50% of relapsing-remitting patients with confirmed progression returned to baseline level of disability. Fifteen percent of patients with secondary progressive disease returned to baseline level of disability.

Early evaluation of new treatments frequently relies on MRI endpoints. Many trials, such as the 20-mg vs 40-mg glatiramer acetate phase 2 trial, have screened patients for enhancing lesions to assist in determining efficacy with fewer patients. Zhao and colleagues[4] examined the short-term changes in monthly gadolinium-enhancing lesion activity in patients with different initial activity levels. In the 65 placebo patients studied, 49% had no enhancing lesions at baseline. Of this group, 75% developed new lesions over 9 months. All patients with enhancing lesions at baseline had at least 2 more enhancing lesions over 9 months with monthly MRI scans.

New Therapies in Clinical Trials

Fingolimod

MRI results for oral fingolimod (FTY720) were presented from the placebo-controlled, phase II study with active drug extension.[5] At 6 months, the median cumulative number of new and persistent enhancing lesions was 5 for placebo, 1 for fingolimod 1.25 mg (P < .001 vs placebo), and 3 for fingolimod 5 mg (P = .006 vs placebo). The mean number of cumulative enhancing lesions was 14.8 with placebo, 8.4 with fingolimod 1.25 mg, and 5.7 with fingolimod 5 mg. A statistically significant effect on T2 lesions was seen early between months 1 and 2 (P < .003 for both doses). Crossover from placebo to active fingolimod treatment at month 6 resulted in a significant reduction in enhancing and T2 lesions at month 12 on both doses.

BG00012

Oral BG00012, a fumaric acid ester, was studied in 257 patients who were randomized into 4 arms by Kappos and colleagues.[6] The 240-mg thrice-daily dose resulted in a 69% reduction in the total number of enhancing MRI lesions at weeks 12-24 (P < .001). The number of new and enlarging T2-hyperintense lesions with treatment at week 24 was 4.2 ± 5.4 compared with 2.2 ± 5.4 with placebo (P < .001). The number of T1-hypointense lesions was also lower with oral fumarate therapy (1.7 ± 2.5 vs 0.8 ± 2.0; P = .014). A 32% reduction in relapse rate was a trend, but it was not statistically significant.

Cladribine

Oral cladribine is currently being investigated in a phase 3, multicenter international trial for MS. Although the results of this trial are pending, Martinez-Rodriguez and colleagues[7] used the intravenous form of cladribine in 6 patients with aggressive relapsing-remitting disease. These patients were treated with intravenous cladribine 0.07 mg/kg/day for 5 days monthly in 2-4 courses. The EDSS decreased from 5.5 to 7.0 at baseline to 1.5-5.0 at 12 months. The mean annualized relapse rate dropped to 0.71 ± 0.55 from 2.67 ± 0.75 at baseline. After 1 year, cladribine was infused again in 4 patients due to new severe relapses. No significant side effects were seen.

Teriflunomide

O'Connor and colleagues[8] reported on a 144-week open-label extension study of the phase 2, randomized, double-blind, placebo-controlled teriflunomide trial. Teriflunomide demonstrated more than a 61% reduction in the number of combined unique active lesions on MRI compared with placebo over 36 weeks of treatment. In the extension phase, the 55 placebo patients were randomized to receive either 7 mg or 14 mg teriflunomide a day, and a total of 147 patients entered this phase. The placebo patients who switched to 7 mg teriflunomide had a 65% reduction in the number of combined unique active lesions (P = .02). Those placebo patients who switched to 14 mg teriflunomide a day had an 85% reduction in the number of combined unique active lesions (P = .02). Annual relapses were similar between arms at approximately 0.4 relapses per year.

Alemtuzumab

Alemtuzumab is a humanized monoclonal antibody that targets the CD52 antigen and is administered intravenously over 3-5 days annually. In a multicenter, rater-blinded trial of 334 relapsing-remitting patients, patients on alemtuzumab had a 75% reduction in relapse rate (P < .003) and a 60% reduction in the risk for sustained accumulation of disability (P < .05) compared with patients on interferon beta-1a 44 micrograms (mcg) subcutaneously thrice weekly.[9] Four patients developed immune thrombocytopenic purpura from 1.5 to 14 months after their last infusion. One patient died from cerebral hemorrhage after 2 weeks of unrecognized symptoms of immune thrombocytopenic purpura. The other patients were successfully treated with steroids ± rituximab. Compston and colleagues[10] presented thyroid-related findings from the year 2 interim safety analysis. With 2.2 years of median follow-up, 11.1% of patients on alemtuzumab had a thyroid-related clinical adverse event compared with 1.9% of patients on interferon beta-1a. Both hyperthyroid and hypothyroid adverse events were reported, including the development of Graves' disease in 3 patients. Antithyroid-stimulating hormone receptor antibodies and antithyroid peroxidase antibodies without clinical thyroid adverse events were seen in 16.7% of alemtuzumab-treated patients and in 11.3% of interferon-treated patients.

Daclizumab

Daclizumab, a humanized monoclonal antibody, binds to the alpha chain of the interleukin (IL)-2 receptor. Rose and colleagues[11] described results from a phase 1/2 trial of daclizumab in patients with relapsing-remitting MS. Eight patients on interferon therapy were treated with the combination of daclizumab and interferon. One patient developed a severe relapse prior to daclizumab and only received 2 doses at baseline and in 2 weeks. The other 7 patients received daclizumab infusions at 1 mg/kg every 2 weeks for the first month and then monthly for 5.5 months. Five patients were found to have no contrast-enhancing lesions on MRI at 6 months, so interferon was discontinued, and daclizumab was continued at 1.5 mg/kg monthly for a total of 27.5 months of treatment. Two patients had contrast-enhancing lesions at 6 months, so interferon was continued with daclizumab at 1.5 mg/kg monthly. A significant reduction of total contrast-enhancing lesions (P < .05-.001) and new contrast-enhancing lesions (P < .001) was seen compared with pretreatment scans and subsequent scans in 3-month intervals. A significant reduction in relapses also occurred (P < .001).

Anti-CD154 Antibody

Blockage of CD154 prevents costimulation of CD4+ T cells, which disrupt T-cell activation. Kasper and colleagues[12] assessed clinical and MRI progression in subjects with relapsing MS following blockade of CD154. Four cohorts of 3 relapsing MS patients each received 1, 5, 10, or 15 mg/kg of fully humanized monoclonal anti-CD154 antibody every other week for 8 weeks. After 5 years of follow-up, no statistically significant change in disability was found on the EDSS (baseline 2.3 ± 0.5, and 5 years 2.5 ± 1.6; P = .622). Higher doses of anti-CD154 significantly correlated with less disability at 5 years (P < .05). The average annual relapse rate over 5 years was 0.125, whereas the pretreatment rate was 1.0.

Combination Therapy

To assess the benefit of add-on therapy with azathioprine and prednisone, a randomized, double-blind, placebo-controlled study of 181 relapsing patients on intramuscular weekly interferon beta-1a was conducted.[13] Over 2 years, the annualized relapse rate was 1.19 for patients only on interferon. The relapse rate was 1.06 for those on azathioprine 50 mg daily and interferon. Lastly, the relapse rate was 0.80 for patients on azathioprine, interferon, and prednisone 10 mg every other day. The differences in the relapse rate and in the cumulative proportion of patients with sustained disability progression at 2 years were not significant. Triple-combination therapy was superior to monotherapy with interferon on T2 lesion volume (P = .015). Combination therapy was safe and well tolerated with similar rates of infection among the groups. Perhaps greater efficacy would have been derived had the investigators used higher doses of azathioprine.

Induction with mitoxantrone prior to glatiramer therapy was investigated in a randomized trial of 40 relapsing-remitting patients with at least 1 gadolinium-enhancing lesion at baseline.[14] The patients received either daily glatiramer acetate 20 mg subcutaneously for 15 months or monthly intravenous mitoxantrone for 3 months and then glatiramer acetate for 12 months. Mitoxantrone induction produced an 89% greater reduction in enhancing lesions at 9 months (P = .0001) than glatiramer alone. Patients who received glatiramer alone had a 47% reduction in enhancing lesion frequency at 9 months and an 87% reduction at 15 months. The relapse rate over 15 months was 0.16 for the mitoxantrone induction group and 0.32 for the glatiramer-only group. The relapse rates over 24 months were 0.24 for patients who received glatiramer acetate after mitoxantrone induction and 0.62 for patients who received glatiramer acetate alone. The reduction in relapse rate was a trend in favor of the combination therapy, but the trial design does not allow one to determine whether this result is superior to that observed by administering mitoxantrone alone.

Updates on Current Therapies

New Interferon beta-1a Formulation

A new formulation of subcutaneous interferon beta-1a without human serum albumin was studied in 260 patients in a single-arm, open-label, multicenter trial.[15] At 48 weeks, neutralizing antibodies greater then 20 neutralizing units/mL were detected in 13.9% of patients compared with 24.4% in the Evidence for Interferon Dose Response: European-North American Comparative Efficacy (EVIDENCE) trial. Persistently positive antibody incidence at 48 weeks was 2.5% compared with 14.3% in the EVIDENCE trial. The incidence of injection site reactions was 29.6% with the new formulation compared with 83.3% in the EVIDENCE trial. Flulike symptoms were higher at 70.8% compared with 48.1% in the EVIDENCE trial. Only 38% of patients who received the new formulation were taking anti-inflammatory medications or anilides at study day 1, which likely contributed to the higher incidence of flu symptoms. The lower incidence of neutralizing antibodies may be potentially clinically beneficial. The study is ongoing to assess the persistently positive neutralizing antibody incidence at 96 weeks because these antibodies generally form over the first 18 months of therapy.

Glatiramer Acetate

Double-dose (40 mg) glatiramer acetate was compared with the standard 20-mg dose by Cohen and colleagues[16] in a randomized, double-blind trial. Of the 229 patients screened, only 90 had 1-15 enhancing MRI lesions at baseline and were randomized to receive 20 or 40 mg of daily subcutaneous glatiramer acetate. The higher dose resulted in a 38% reduction of total enhancing lesions over months 7-9, but this primary endpoint was not statistically significant (P = .09). Seventy-six percent of patients on the 40-mg dose and 52% on the 20-mg dose were relapse-free, which was a significant benefit. There was a trend in favor of the higher dose in the relapse rate; the rate was 0.43 with 40 mg and 0.57 with 20 mg (P = .12). The rates of immediate postinjection reactions were 22.7% with 20 mg and 32.6% with 40 mg. Further study of higher dose glatiramer is being pursued in a phase 3 clinical trial.

Interferon beta-1b

Goodin and colleagues[17] examined the rates of neutralizing antibody-positive titers in 2 cohorts of patients with a poor clinical response to interferon beta-1b therapy and 1 cohort of patients unselected for response to therapy. This analysis of 6698 patients was conducted to gain an understanding of the clinical impact of these antibodies. Out of the 1998 patients in the North American cohort, 94% had neutralizing antibody testing for disease worsening. Sixty-seven percent had disease progression for at least 6 months, and 34% had at least 3 exacerbations that required steroids and/or hospitalizations per year. Of interest, only 21.3% of patients in the North American cohort were neutralizing antibody-positive with a mean duration of interferon treatment of 3.32 years. Compulsory testing was performed in the Australian cohort of 2271 patients regardless of their clinical response. If neutralizing antibody-positive status was a principal cause for worsening disease, the incidence of positive neutralizing antibodies would be expected to be lower in the Australian cohort with routine testing than in the North American cohort with testing for worsening disease. However, in the Australian cohort, 37% of patients had at least 20 neutralizing units/mL of neutralizing antibodies. Therefore, these results suggest that antibody positivity does not appear to be the major etiology for worsening MS.

Natalizumab

O'Connor and colleagues[18] presented the pivotal trial extension results after natalizumab dosing was suspended. The annualized relapse rate for 1866 patients increased monthly after treatment cessation and peaked at 0.64 at 7 months. Data from 341 patients who had MRI results greater than 60 days after natalizumab discontinuation also experienced a rise in enhancing lesions over 6 months. No new cases of progressive multifocal leukoencephalopathy were reported.

Mitoxantrone

Le Page and colleagues[19] presented the long-term safety data for mitoxantrone in a French cohort of 802 patients. All patients had at least 5 years of follow-up. One patient developed acute congestive heart failure. Thirty-nine patients (4.9%) developed an asymptomatic reduction of their left ventricular ejection fraction below 50%, but it was only transitory in 26 patients. Two patients (0.25%) developed therapy-related acute myeloblastic leukemia 20 and 22 months after the initiation of treatment. One of the 2 patients died regardless of receiving specific chemotherapy. Persistent amenorrhea occurred in 5.4% of women less than 35 and in 31% of women 35 and older. With up to 15 years of follow-up, 51 patients had died but only the leukemia patient's death was considered treatment-related. Thirty-three patients' deaths were considered complications of severe MS.

Therapeutic Development in Experimental Models

IL-17

IL-17, a proinflammatory cytokine, can be blocked with a monoclonal antibody. Smith and colleagues[20] tested the hypothesis that IL-17 was responsible for driving relapses in the spontaneous chronic-relapsing experimental allergic encephalomyelitis model in the mouse, with an antimouse IL-17 monoclonal immunoglobulin antibody. Ten milligrams per kilogram of anti-IL-17 antibody were administered weekly subcutaneously during remission. The anti-IL-17 antibody significantly reduced the relapse incidence and the inhibited neurologic deficit formation. Treatment with the antibody prior to the acute phase delayed disease, but failed to reduce the clinical score. Because IL-17 may be playing an important role in driving relapses, anti-IL-17 therapies may prove to be effective treatment options for relapsing-remitting disease.

c-Jun N-terminal Kinase Inhibition

The c-Jun N-terminal kinase (JNK) pathway, which can be induced in activated T cells, affects gene expression, cellular survival, and cellular proliferation in response to cytokines. These events are associated with the pathogenesis of autoimmune diseases, such as MS. Ferrandi and colleagues[21] investigated the potential role of the JNK pathway in MS. The JNK2 isoform was upregulated in peripheral blood mononuclear cells of patients with relapsing-remitting disease. In vitro administration of a JNK inhibitor resulted in a significant reduction in cell proliferation with triggering of T-cell apoptosis and c-Jun dephosphorylation. The JNK inhibitor, given in daily oral doses, reduced the severity of pathology and delayed the onset of disease in experimental allergic encephalomyelitis. These results support the hypothesis that the inhibition of the JNK pathway could have a role in the treatment of relapsing-remitting MS.

Tyrosine Kinase Inhibition

C-1311 (Symadex), a tyrosine kinase inhibitor, disrupts trafficking of autoreactive cells and concomitant angiogenic processes. Karlik and Ajami[22] presented results showing that treatment initiated in the chronic phase of guinea pig experimental allergic encephalomyelitis showed reversal of clinical and pathologic signs. Treatment with C-1311 was associated with remyelination and modulation of vascular changes.

Arundic Acid

Arundic acid (ONO-2506) is a compound that modulates the function of astrocytes. Studies are examining its use in stroke, Parkinson's disease, and Alzheimer's disease. Arundic acid may enhance the uptake of the neurotransmitter glutamate by activation of astrocytic glutamate transporter receptors in ischemia models. With less extracellular glutamate, neurons are more protected from glutamate influx and cell death. Arundic acid was studied by Takizawa and colleagues[23] in chronic progressive and relapsing-remitting experimental allergic encephalomyelitis. Treatment resulted in milder neurologic symptoms and fewer demyelinating lesions in the brain and spinal cord.

Sphingosine-1-phosphate Receptors and Extracellular Receptor Regulated Kinase Phosphorylation

FTY-720 (fingolimod) also may modulate astrocyte function, which could be beneficial in MS. FTY-720 can activate subtypes 1 and 3 of sphingosine-1-phosphate (S1P) receptors on astrocytes. Osinde and Dev[24] determined which receptor subtype is involved in extracellular receptor regulated kinase (ERK) phosphorylation in astrocytes. Activation of these receptors was measured with downstream signaling via adenylyl cyclase, phospholipase C, and ERK. The study authors found that the S1P receptor subtype-1 mediates ERK phosphorylation in astrocytes. Potential astrocytic functions that are beneficial in MS are those that promote neuronal survival and remyelination and strengthen the contact sites between endothelial cells at the blood-brain barrier.

Understanding Axonal and Myelin Injury and New Opportunities for Treatment

Obtaining a deeper understanding of mechanisms of axonal and myelin injury in MS is leading to opportunities for targeted treatment. Matute[25] presented current knowledge about the mechanisms leading to oligodendrocyte cell death and demyelination as a consequence of alterations in glutamate signaling, and the clinical relevance to MS. Glutamate excitotoxicity can cause injury to neurons, myelin, and oligodendrocytes. The mechanisms of action are either from sustained activation of glutamate receptors or independent influx of glutamate. Treatments directed at glutamate receptor types, such as NMDA, AMPA, or kainate, may prevent downstream events that lead to cell death from DNA fragmentation. Clinically, plasma glutamate levels of MS patients are higher than control patient levels, especially in relapse. The P2X7 receptor is expressed on oligodendrocytes, and in vitro activation leads to oligodendrocyte cell death. P2X7 receptor expression is higher in the white matter of MS brains that appears normal on MRI than the white matter of controls. BBG, a P2X7 antagonist, has been shown to ameliorate disease in chronic experimental allergic encephalomyelitis.

Smith[26] discussed partial blockade of sodium channels and axonal protection. At sites of inflammation, sodium influx occurs along the axon via sodium channels. The calcium/sodium exchanger fails, resulting in further sodium accumulation plus calcium influx. The resultant high intracellular concentration of sodium and calcium leads to axonal injury. In experimental allergic encephalomyelitis, sodium channel blockers, such as flecainide and lamotrigine, can block this influx and reduce disease severity. Furby and colleagues[27] are recruiting patients for a phase 2 trial of lamotrigine in secondary progressive disease. In total, 120 patients are being randomized to receive either lamotrigine or placebo. The primary outcome of this trial will be brain atrophy.

A critical question in MS is whether early treatment of inflammation prevents axonal degeneration. A partial answer comes from the results of a pathologic brain study of 5 MS patients who died after autologous stem cell transplantation.[28] The patients had died 20 days to 1.5 years after transplantation. Of the 53 total white matter lesions examined, 41 had demyelinating features and 20 had remyelinating features. Sixteen lesions demonstrated chronic active features with macrophages at the edge or rim of the lesions. Inflammation of T cells, B cells, and plasma cells was profoundly suppressed. However, microglia and macrophage activation were ongoing. In addition, axonal degeneration and demyelination continued regardless of the transplant. These results parallel those from the phase 1/2 clinical studies,[29] which showed continued disease progression in patients with high Expanded Disability Status Scale (EDSS) scores despite autologous stem cell transplantation.

Comi[30] described progress in MS research in Europe, including research on disease injury. Early inflammatory changes in MS may lead to axonal injury and/or oligodendrocyte cell death. An alternative hypothesis is that the inflammation is actually secondary to axonal loss and/or oligodendrocyte cell death. Possible triggers for oligodendrocyte apoptosis are nitrous oxide, excitotoxicity, and hypoxia. Noninflammatory oligodendrocyte injury (pattern III lesions) may precede inflammatory pathologic changes (pattern II lesions). Radiologic evidence for this alternative hypothesis is increased diffusion restriction and decreased magnetic transfer ratios prior to lesion formation on MRI. Therefore, focal inflammation may be a reaction to axonal damage.

Mesenchymal stem cells are a subset of adult stem cells that may have the potential to repair damage in the central nervous system in MS. Derived from the bone marrow stroma, mesenchymal stem cells can differentiate into 3 germ cell layers. In addition, these cells can directly inhibit T cells and B cells. Intravenous injection of mesenchymal stem cells into a tail vein can ameliorate both relapsing-remitting (proteolipid protein-induced) and chronic progressive (myelin-oligodendrocyte-glycoprotein-induced) experimental allergic encephalomyelitis. Reduction in disease occurs when the mesenchymal stem cells are added either before or after disease onset. Gerdoni and colleagues[31] showed that intravenously injected mesenchymal stem cells can ameliorate relapsing-remitting and chronic progressive experimental autoimmune encephalomyelitis before and after disease onset. Injection with mesenchymal stem cells led to reduced inflammatory infiltrates, demyelination, and axonal loss within the central nervous system. Neurons, astrocytes, and oligodendrocytes were spared, which could suggest a neuroprotective role of the stem cells. The mesenchymal stem cells had migrated to the central nervous system in 30 days, but no differentiation to neural cells was seen.

Neurofascin, a cell-surface glycoprotein, may be a target for antibody-mediated axonal injury in MS. Mathey and colleagues[32] performed a proteomics-based analysis of autoantibody specificities in patients with MS and controls that identified a prominent disease associated antibody response to neurofascin, a cell-surface glycoprotein that exists in 2 isoforms. The study authors found that neurofascin-specific monoclonal antibodies rapidly exacerbated disease severity in experimental allergic encephalomyelitis. Marked acute axonal injury was seen in the absence of demyelination and any significant local inflammatory response. Confocal microscopy demonstrated that the antineurofascin monoclonal antibody colocalizes with voltage-gated sodium channels at the nodes of Ranvier. These results suggest that blocking this autoantibody may prevent axonal injury.

Baker[33] investigated the protection of axonal damage by cannabinoids in experimental autoimmune encephalomyelitis. Cannabinoids in cannabis and synthetic cannabinoid receptor agonists can help spare axonal damage in experimental allergic encephalomyelitis. Cannabinoids can inhibit mononuclear cells from invading the central nervous system. Stimulation of the cannabinoid CB1 receptor in the brain in experimental allergic encephalomyelitis caused the release of immunosuppressive molecules that downregulate proinflammatory TH1 responses. However, cannabinoids may also protect axons via a direct neuroprotective role in the central nervous system. Animals deficient in cannabinoid receptors exhibit exaggerated nerve loss to autoimmune attacks and increased neurodegeneration in experimental allergic encephalomyelitis. Cannabinoid receptor stimulation slowed neurodegeneration in a manner independent of inhibition of autoimmunity in animal models of MS, uveitis, and amyotrophic lateral sclerosis. These results suggest that the cannabinoid system may be able to slow progression of disease by preventing nerve loss in addition to symptom control.

Conclusion

Placebo-controlled trials can still be ethically performed if patients have not tolerated, failed, or refused current treatments. Such trials should have informed consent, be of short duration, and allow dropping out of the trial for worsening disease. Potential new treatments being studied are oral agents (BG00012, cladribine, fingolimod, and teriflunomide) and monoclonal therapies (alemtuzumab, daclizumab, and anti-CD154 antibody). Additional advances in treatment include a new formulation of interferon beta-1a that produces fewer neutralizing antibodies and the use of double-dose glatiramer acetate. Ongoing research may yield further discovery, leading to targeted treatments to prevent axonal and myelin injury.

References

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  12. Kasper L, Fadul C, Ryan K, et al. Short-term blockade of CD154 potentiates long term clinical and MRI remission of RRMS: a five-year follow up. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Poster 390.
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  14. Vollmer T, Panitch H, Freedman MS, et al. Short-term induction with mitoxantrone preceding treatment with glatiramer acetate offers early and pronounced effects on MRI-disease activity in patients with relapsing forms of multiple sclerosis. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Abstract 62.
  15. Giovannoni G, Barbarash OL, Jaber A, et al; on behalf of the RNF Study Group. Reduced immunogenicity with a new formulation of interferon-beta-1a (Rebif): 24-week results of a phase IIIb study. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Poster 675.
  16. Cohen J, Rovaris M, Goodman A, Wynn D, Ladkani D, Filippi M; for the 9006 Study Group. Randomised, double-blind, parallel-group, dose-comparison study of glatiramer acetate in relapsing-remitting multiple sclerosis. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Abstract 100.
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  23. Takizawa K, Tomioka R, Kinoshita S, et al. Arundic acid (ONO-2506) prevents chronic progressive and relapsing-remitting EAE. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Poster 233.
  24. Osinde M, Dev KK. The sphingosine-1-phosphate receptor subtype-1 stimulates ERK phosphorylation in astrocytes. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Poster 792.
  25. Matute C. Glutamate toxicity and experimental myelin injury. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Abstract 39.
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  32. Mathey E, Derfuss T, Storch M, et al. Neurofascin: a novel target for antibody mediated axonal injury in multiple sclerosis. Program and abstracts of the 22nd Congress of the European Committee for Treatment and Research in Multiple Sclerosis; September 27-30, 2006; Madrid, Spain. Abstract 102.
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http://www.medscape.com/viewarticle/548063

Study Shows Pregabalin Effective in Difficult-to-Treat Nerve Pain

Study Shows Pregabalin Effective in Difficult-to-Treat Nerve Pain
RedNova Tue, 28 Nov 2006 6:18 AM PST
SYDNEY, Australia, November 28 /PRNewswire/ --

PharmaLive: Novartis Highlights Strong R&D Pipeline, Plans for Multiple New Product Launches and Novel Projects Moving Into Late-stage Trials

FTY720 (fingolimod), seeking to become the first oral disease-modifying treatment for patients with relapsing multiple sclerosis (MS), is being studied in a Phase III program underway with the goal of enrolling more than 3,000 patients worldwide. A two-year placebo-controlled program (FREEDOMS) is measuring reductions in the frequency of relapses and disability progression in MS patients. A one-year trial (TRANFORMS) started in May 2006 comparing FTY720 with interferon beta-1a (Avonex®). Two-year data from the extension of a Phase II trial showed sustained benefits, indicating that FTY720 could provide an important new option for the estimated 2.5 million people worldwide suffering from this disabling neurological disease. Submission remains on track for 2009.
http://www.medadnews.com/News/index.cfm?articleid=394765

Multiple Sclerosis Foundation Internet Newsletter

We value your opinions!
Please let us know what you think of the MSFYi, this month's features, or send ideas for future issues.

NOVEMBER 2006 - MSFYi

Happy Thanksgiving from all your friends at the MSF!

""Happy is the house that shelters a friend." ~ Ralph Waldo Emerson

In This Issue
* DOCTORS USE CAUTION WITH TYSABRI®
* ESTRIOL FOR TREATMENT OF MS
* T'AI CHI IMPROVES FITNESS IN ELDERLY WOMEN
* THE EFFECTS OF VEGETABLES ON COGNITION
* LAST CHANCE FOR "FOCUS ON YOUR FEELINGS" HOLIDAY GIVEAWAY!
* MS LINKED TO ABNORMAL LIVER TEST RESULTS
* LAST CALL FOR ADAPTIVE SKIING SCHOLARSHIPS
* MEN CAN GET OSTEOPOROSIS, TOO
* A WINTER'S WISH TO BENEFIT MS RESEARCH
* BETASERON APPROVED FOR CIS

MSF News
* MSF HOSTS 3RD ANNUAL NURSE SYMPOSIA
* NATIONAL MS EDUCATION & AWARENESS MONTH™
* 2007 MSF CRUISE FOR A CAUSE TO ALASKA



DOCTORS USE CAUTION WITH TYSABRI®
Doctors are proving more cautious than expected about prescribing Tysabri, which was re-launched in July after being suspended due to safety concerns.

A Reuters Primary Research survey of 63 neurologists indicates that Tysabri will be used in less than 1 percent of MS patients during 2006.

Since July, only 47 of more than 8,500 patients treated by physicians surveyed had used Tysabri, despite the fact that more than 700 patients had discussed using it.

The survey also showed that more than 75 percent of the patients who had used Tysabri prior to its suspension have decided not to use it since its reintroduction.

"At our center, we recommend Tysabri cautiously," confirms Dr. Roger Williams, Medical Director of the Northern Rockies MS Center in Billings, Montana. "Initially, we may have considered Tysabri as first-line therapy for relapsing-remitting MS. Now, we use it for patients with breakthrough disease after one or two of the C-R-A-B drugs. Hence, it now competes with Novantrone and Cytoxan as a potentially more aggressive and effective therapy, but one that is risky, riskier than the C-R-A-B drugs but comparable to chemotherapy. We have enrolled eight patients for Tysabri. All patients have been pre-approved by third party payers. However it may take three to four months to work out the glitches of reimbursement."

"I am also being cautious with Tysabri," adds Dr. Ben Thrower, Medical Director of the MS Center at Shepherd Center in Atlanta, Georgia. "I use it in individuals who have failed the A-B-C-R drugs and who have aggressive enough disease to warrant the risk. The problem is that we really don't know what the true, long-term risk of PML will be. We work with a little over 2,000 people with MS, but only consider about 17 of them to be Tysabri candidates."

Another issue may be the 'Touch' Program, a special training required for physicians prescribing and personnel administering Tysabri. "I have yet to be 'touched' by Biogen-Idec so I cannot prescribe Tysabri yet," says Dr. Greg Zarelli, Staff Physician in the Department of Neurology at Kaiser-Permanente NW in Clackamas, Oregon.



ESTRIOL FOR TREATMENT OF MS
The first large-scale trial of the female hormone estriol for the treatment of MS is about to begin. UCLA neurologist Dr. Rhonda Voskuhl is leading a team of investigators to conduct a two-year, controlled clinical trial of estriol involving 130 women with early relapsing-remitting MS.

Estriol levels rise significantly during pregnancy, when most women's MS disease activity declines. Consequently, some researchers suspect that estriol may play a role in the reduction of symptoms during pregnancy. Preliminary research has indicated that estriol may help protect against the immune attacks associated with MS.

In the near future, newly diagnosed women with relapsing-remitting MS will be recruited for this two-year study at seven medical centers across the country (Los Angeles, CA; St. Louis, MO; New Brunswick, NJ; Columbus, OH; Chicago, IL; Salt Lake City, UT; and Detroit, MI).

According to Dr. Voskuhl, the oral estriol study will aim to simulate some of the disease protection offered by pregnancy. Investigators will administer estriol in pill form in combination with Copaxone. The team will evaluate effects of the treatment combination on relapse rates and several clinical and magnetic resonance imaging measures of disease progression.

The consensus in the U.S. is that all patients with relapsing-remitting MS should be on an injectable disease-modifying medication as they have been proven to reduce relapses by a third, according to Dr. Voskuhl.

"Therefore, it is no longer ethical to have an arm of a trial that receives only placebo if it goes on for longer than four to six months. Thus, ours has to be an 'add on' study."



T'AI CHI IMPROVES FITNESS IN ELDERLY WOMEN
In older women, a short style of t'ai chi may promote physical fitness better than brisk walking, according to a small study. In 19 women, both activities were compared for their effects on aerobic capacity, heart rate variability, strength, flexibility, balance, psychological status, and quality of life.

Participants in this study were sedentary, with an average age of 71. Another group of similar elderly women from the same population served as an inactive comparison group. Fitness was measured at baseline and after the study period for all study parameters. The two exercise groups performed the activities (either walking or t'ai chi) for 1 hour, 3 days per week, for a period of 12 weeks. The control group remained inactive.

At the end of the study, the t'ai chi group had significantly better improvements than the walking group in lower-extremity strength, balance and flexibility. In addition, the practice generally improved the other fitness measures.

T'ai chi is an ancient Chinese system of slow, flowing, meditative motion derived from the martial arts, and prior to that, the natural movements of birds and animals. Literally translated, tai means big or great and chi means ultimate energy.

T'ai chi can be practiced and enjoyed, regardless of physical capacity. It can even be practiced while sitting in a chair or reclining on the bed or floor.

Visit the MSF Lending Library and view our t'ai chi materials. Click http://www.msfocus.org/publication_lending.php?id=3.



THE EFFECTS OF VEGETABLES ON COGNITION
Eating three or more servings of vegetables daily may slow your mental decline by about 40 percent compared with someone who consumes few vegetables, according to a six-year study of about 3,000 Chicago residents age 65 or older. The study was conducted by Rush University Medical Center. Results were published in the in October 24 issue of Neurology.

When compared to people who ate less than one serving of vegetables daily, people who ate 2.8 or more serving of vegetables daily demonstrated a rate of cognitive decline equivalent to people five years younger. One serving of a vegetable is equal to about a cup.

The study also revealed that older people who started eating more than two servings of vegetables a day still showed a significant delay in mental decline, suggesting that it's likely never too late to reap the benefits of vegetable consumption.

The new findings follow two earlier studies, also conducted by Rush University Medical Center, indicating that the foods people eat may significantly affect their mental agility. Four years ago, Martha Clare Morris, chief of Rush University's Center for Healthy Aging, reported that eating foods high in vitamin E appeared to reduce the risk of Alzheimer's disease and last year, she found that eating fish had a similar effect.

Vegetables, especially those in the green, leafy category, are rich in antioxidant compounds like vitamin E, flavonoids and carotenoids.

Eating vegetables with olive oil, vegetable oil or some other type of poly- or mono-unsaturated fats, enhances the body's absorption of antioxidants, which help destroy cell-damaging free radicals, she added.

"When we controlled for all of those healthy lifestyle variables - physical exercise, age, sex, race, education, cognitive activity, participation - the effects of vegetables on cognition actually became stronger," Morris said.

Consuming lots of fruit did not appear to offer the same mental protection, although fruit has been associated with a wide variety of other health benefits.



LAST CHANCE FOR "FOCUS ON YOUR FEELINGS" HOLIDAY GIVEAWAY!
MSF and Hunter House Publications have teamed up to host a special "Focus On Your Feelings" Holiday Giveaway. Ten winners will receive a complimentary, autographed copy of MS & Your Feelings (Hunter House 2006) and also have their winning entries published on the MSF website, http://www.msfocus.org and the Hunter House website, http://www.hunterhouse.com.

MS and Your Feelings is written by Allison Shadday, a woman who lives with MS and who has counseled hundreds of people with the disease, Her book explores denial and acceptance, guilt and depression, psychological numbing, loneliness, and much more.

To enter our "Focus On Your Feelings" Holiday Giveaway, in 200 words or less, tell us about the emotional impact MS has had on your life. Whether you're finally moving from denial to acceptance, finding a way to manage depression, surviving a bitter breakup, or experiencing the loneliness and isolation that sometimes accompanies MS, we want to know! You may write in any style you wish, be it first-person essay, poetry or prose.

Entries must be submitted via email by December 1st. Those that exceed the 200-word limit will automatically be disqualified. Please include your name, age, city, state, telephone number or email address and the date of your MS diagnosis. Ten winning entries will be selected and contacted by December 15th. Send entries to editor@msfocus.org. Please type "Focus On Your Feelings" Holiday Giveaway in the subject line.



MS LINKED TO ABNORMAL LIVER TEST RESULTS
MS has been linked to abnormal liver test results, according to research findings from the MS Society of Canada. The study was published in the October 10 edition of Neurology.

These findings indicate that people with MS need to take extra care when using medications that might affect their liver and be alert to any possible symptoms of liver disease, according to Dr. Helen Tremlett, assistant professor at the University of British Columbia and lead researcher of the study.

"I would recommend people with MS have their liver tested as a routine part of their care when being treated with drugs known to affect the liver," Dr. Tremlett says. "In addition, people need to inform their doctor immediately if there is any presentation of liver disease symptoms."

Symptoms of liver disease include jaundice, or yellowing of the skin or yellowing of the whites of the eyes, itchy skin and unexpected fatigue.

The liver is an organ located on the right side of the body, under the lower ribcage. It stores and metabolizes energy, regulates fat storage and blood clotting, breaks down drugs and alcohol, aids in digestion, produces essential immune system factors, and more. Diseases of the liver include hepatitis and cirrhosis.

Researchers used data from the Sylvia Lawry Centre for MS Research in Germany, the largest database of MS clinical trial information in the world. Medical information from 813 people with MS, enrolled in various clinical trials from North America, Australia and Europe, was analyzed.

Over a two-year period, there was an over three-fold increased risk of a person with MS having an elevated liver test result compared to expectations, i.e., within a "normal range." An elevated test result indicates that liver enzymes have leaked out of their cells. This leakage into the blood stream may be an indicator of liver cell damage.

Over-the-counter medicines like acetaminophen or herbal remedies may cause elevated levels of liver enzymes in the blood. So, it is important that people with MS keep their doctor and pharmacist fully informed of all medicines being taken so that symptoms and test results are not misinterpreted.

An earlier study, also led by Dr. Tremlett, showed that the beta interferons - Avonex, Betaseron and Rebif - can increase the risk of liver problems. However, the current study examined those who were not on beta interferon treatment.

"Although beta interferons do further increase the risk of an elevated test, we know now that abnormal liver tests can result independent of this treatment," says Dr. Tremlett. "The next step is to determine why this is and hopefully add another piece to the complex puzzle that is MS."



LAST CALL FOR ADAPTIVE SKIING SCHOLARSHIPS
The Adaptive Sports Association (ASA), a non-profit, year-round sports and recreational organization dedicated to enhancing the well-being of people with disabilities, is offering the New Dimensions Scholarship for a snow-skiing program in Durango, Colorado. The deadline for applications is December 15th.

Scholarship winners will receive a trip to Durango to learn to snow ski! Round-trip transportation, five-nights lodging with Durango area host homes, most meals, accessible ground transportation, four days of adaptive ski instruction, lift tickets, equipment and private instruction are included!

For more information or to apply for a New Dimensions Scholarship, please call the ASA at 970-259-0374. Or visit http://www.asadurango.org/scholarships.html#newdimensions.



MEN CAN GET OSTEOPOROSIS, TOO
When people hear the word "osteoporosis," they generally think of calcium, broken bones, and women. But osteoporosis, a disease that reduces bone density and strength, making bones more vulnerable to fracture, affects men, too.

According to the National Osteoporosis Foundation, of the 10 million Americans estimated to have osteoporosis, eight million are women and two million - that's 20% - are men. Still, osteoporosis in men is under-recognized and under-treated.

Usually, osteoporosis is diagnosed after a person has broken a bone or taken a bone density test. But men are less likely than women to get this test - even after they've suffered a fracture or broken bone.

Risk factors associated with osteoporosis in men include:
· Prolonged exposure to certain medications that can affect bone density, particularly steroids or treatments for prostate cancer
· A fracture after the age of 50
· Having a first-degree relative who has osteoporosis or has suffered a fragility fracture
· Being underweight
· Low intake of calcium or a deficiency of vitamin D
· Excessive intake of caffeine
· Certain conditions, including endocrine disorders, gastrointestinal diseases, kidney disorders and low testosterone production
· A sedentary lifestyle
· Smoking and excessive alcohol consumption

The good news is that osteoporosis can be prevented. To reduce your risk, eat a balanced diet rich in calcium and vitamin D. Participate in weight-bearing exercises, such as walking, yoga or bike riding. Strive to stop smoking and drink alcohol in moderation. It's also important for men to discuss their bone health with their physicians.

To learn more about osteoporosis, visit the National Osteoporosis Foundation http://www.nof.org or the International Osteoporosis Foundation at http://www.iofbonehealth.org.



A WINTER'S WISH TO BENEFIT MS RESEARCH
This Christmas, help others with MS and get a beautiful holiday CD, perfect for gift-giving or as an addition to your own collection.

"A Winter's Wish," which can be purchased as a CD or full album download, includes 12 Christmas songs, including So This Is Christmas, recorded by Paul Nicholas, who joined us on our 5th Annual Cruise for a Cause!

Others songs, recorded by a variety of artists, include Do You Hear What I Hear, Jingle Bell Rock, O Holy Night, and many more.

Proceeds will go to the programs and services provided by the MSF, toward finding a cure for MS through the Montel Williams MS Foundation and a preventive vaccine for AIDS through the International AIDS Vaccine Initiative.

To learn more or to purchase "A Winter's Wish," go to http://www.airgomusic.com.



BETASERON APPROVED FOR CIS
The FDA has approved expanding the indication of Betaseron® (interferon beta-1b) to include individuals who have experienced a clinically isolated syndrome (CIS) consistent with MS.

CIS refers to a single clinical event indicative of demyelination, such as inflammation of the optic nerve or an episode of numbness, along with MRI findings consistent with MS.

This is the second therapy approved for treatment for those with CIS. In 2003, the FDA expanded the labeling of Avonex® (interferon beta-1a) to include this indication.

"Most MS centers look at the CIS patient and try to determine their future risk of developing MS," clarifies MSF Medical Advisor, Dr. Ben Thrower. "If the patient has brain MRI abnormalities or CSF oligoclonal bands (a pattern of banding seen in MS), we know they have a high risk of having more attacks in the future. If we decide to treat that person, we are doing so because we think they have early MS. I would argue that we did not really need studies to show that the interferon drugs work in such people. I would also argue that you should treat them with whatever you think is appropriate for early relapsing-remitting MS. With that said, I usually do not treat a CIS patient. I would discuss their MS risk with them and then encourage them to get a follow-up MRI in about three months. If the patient has a new lesion on MRI or a second relapse, then they have definite MS, not CIS with a risk of MS. I think that is an important distinction down the road when patients start wond!
ering if they really need to inje
themselves with medication."



MSF NEWS

MSF HOSTS 3RD ANNUAL NURSE SYMPOSIA
All MS nurses are cordially invited to join us for a Voyage to a Better Understanding of MS Care - a four-day Western Caribbean Cruise! This educational program will be held aboard Carnival Cruise Line's Imagination. We'll set sail from Miami on Thursday, March 8 and return on Monday, March 12th, 2007. Ports of call include Key West, Florida and Calica, Mexico.

This program will provide up to 13.2 contact hours through the Texas Nurses Association, an accredited approver of continuing nursing education by the American Nurses Credentialing Center's Commission on Accreditation.

Presented by MS nurses from across the country, the educational curriculum will provide updated and pertinent information needed by nurses who provide care for patients with MS, including symptom management and other topics of relevance to the MS patient. The educational program will also prepare the nurse for the International Organization of Multiple Sclerosis Nurses (IOMSN) certification board examination and may also be applied to re-certification credits.

Space for this program is limited and passports are required. For more information call Fun Cruise & Travel toll-free at 888-826-9660, or visit http://www.funcruiseandtravel.com/msf2.htm.



NATIONAL MS EDUCATION & AWARENESS MONTH™
National MS Education & Awareness Month is rapidly approaching. There are so many ways that you, your friends, family members, and MS support groups can participate! Our theme this year is Lights, Camera, Action!

We have three international teleconferences and two webchats planned for the month, along with several regional events. Empower yourself by joining us for these unbiased educational programs. We will provide specific details soon.

MS Awareness Kits, filled with educational literature created for those with MS as well as their families and care partners, are free upon request. Simply send an email to awareness@msfocus.org.

We encourage you to take action during the month by planning a fundraiser, special event, or educational program in your community. If you need help getting started, call our Community Relations Department at 800-225-6495 or send an email to awareness@msfocus.org. If you have a website, newsletter, e-newsletter or blog, help us get the word out about National MS Education and Awareness Month. Do it for yourself. Or, do it for someone you know who is newly diagnosed. Whatever you do, play a part in Lights! Camera! Action!



2007 MSF CRUISE FOR A CAUSE TO ALASKA
The MSF Cruise for a Cause offers innovative, educational programs at sea for individuals with MS. This fun-filled adventure provides an opportunity to learn from renowned MS specialists, forge friendships with others with MS, and enjoy an infinite number of amenities, all aboard a luxury cruise ship!
This year, we will follow the Inside Passage from Seattle, Washington to Skagway, Alaska - 500 miles of crisp, clean air and unparalleled natural wonders!

Don't miss this seven-night adventure, from June 8th through the 15th, aboard Royal Caribbean's Vision of the Seas. Ports of call include Juneau, Skagway, Tracy Arm Fjord, Prince Rupert, British Columbia, and Seattle, Washington!

Passports required! For more information call Fun Cruise & Travel toll-free at 888-826-9660, or visit http://www.funcruiseandtravel.com/msf2.htm.

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**Editor's Note: The intent of this newsletter is to provide information on various medical conditions, medications, treatments, and procedures for your personal knowledge and to keep you informed of current health-related issues. It is not intended to be complete or exhaustive, nor is it a substitute for the advice of your physician. Should you or your family members have any specific medical problem, seek medical care promptly.


For questions regarding this publication, email editor@msfocus.org. For support services, email support@msfocus.org. Please do not reply to this email address for correspondence.

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