A phase III study evaluating the efficacy and safety of MBP8298 in secondary progressive MS.

OBJECTIVE: To evaluate the efficacy and safety of MBP8298 in subjects with secondary progressive multiple sclerosis (SPMS) who express human leukocyte antigen (HLA) haplotype DR2 or DR4 (DR2(+) or DR4(+)). METHODS: This multicenter randomized 2-year, double-blind, placebo-controlled study included 612 subjects with a diagnosis of SPMS and an Expanded Disability Status Scale (EDSS) score of 3.5-6.5, stratified according to baseline EDSS score (3.5-5.0, or 5.5-6.5) and HLA haplotype (DR2(+) or DR4(+), or DR2(-)/DR4(-)). Upon entry of 100 DR2(-)/DR4(-) subjects, further study enrollment was limited to DR2(+) or DR4(+) subjects. Subjects were randomly assigned to either 500 mg MBP8298 or placebo, given by IV injection once every 6 months for 2 years. The primary outcome measure was time to progression by ≥1.0 EDSS point (or 0.5 point if baseline EDSS was 5.5 or higher), confirmed 6 months later. Secondary outcomes included mean change in EDSS, mean change in Multiple Sclerosis Functional Composite, MRI changes, annualized relapse rate, and quality of life. RESULTS: There were no significant differences between treatment groups in either the primary or secondary endpoints. MBP8298 was well tolerated in all treated subjects with no safety issues identified. CONCLUSION: In the population studied, treatment with MBP8298 did not provide a clinical benefit compared to placebo. CLASSIFICATION OF EVIDENCE: This study provides Class 1 evidence that MBP8298 is not effective in patients with SPMS who are HLA DR2(+) or DR4(+).

Intravenous synthetic peptide MBP8298 delayed disease progression in an HLA Class II-defined cohort of patients with progressive multiple sclerosis: results of a 24-month double-blind placebo-controlled clinical trial and 5 years of follow-up treatment.

MBP8298 is a synthetic peptide with a sequence corresponding to amino acid residues 82-98 of human myelin basic protein (DENPVVHFFKNIVTPRT). It represents the immunodominant target for both B cells and T cells in multiple sclerosis (MS) patients with HLA haplotype DR2. Its administration in accordance with the principle of high dose tolerance results in long-term suppression of anti-myelin basic protein (MBP) autoantibody levels in the cerebrospinal fluid (CSF) of a large fraction of progressive MS patients. MBP8298 was evaluated in a 24-month placebo-controlled double-blinded Phase II clinical trial in 32 patients with progressive MS. The objective was to assess the clinical efficacy of 500 mg of MBP8298 administered intravenously every 6 months, as measured by changes in Expanded Disability Status Scale (EDSS) scores. Contingency analysis for all patients at 24 months showed no significant difference between MBP8298 and placebo-treatments (n = 32, P = 0.29). Contingency analysis in an HLA Class II defined subgroup showed a statistically significant benefit of MBP8298 treatment compared with placebo in patients with HLA haplotypes DR2 and/or DR4 (n = 20, P = 0.01). Long-term follow-up treatment and assessment of patients in this responder group showed a median time to progression of 78 months for MBP8298 treated patients compared with 18 months for placebo-treatment (Kaplan-Meier analysis, P = 0.004; relative rate of progression = 0.23). Anti-MBP autoantibody levels in the CSF of most MBP8298 treated patients were suppressed, but antibody suppression was not predictive of clinical benefit. Anti-MBP autoantibodies that reappeared in the CSF of one patient at 36 months, whilst under treatment with MBP8298, were not reactive with the MBP8298 peptide in vitro. The identification of a responder subgroup (62.5% of the patients in this study) enables a more efficient design of a large confirmatory clinical trial of MBP8298. The probability that patients with other less common HLA-DR haplotypes will respond to this treatment should not be ignored.

Geographic areas with extremely high mortality correlations for cancers in the province of Alberta, Canada.

Age-adjusted mortality rates, calculated by the direct method and based on the 1971 census-population of Alberta, for 24 male and 26 female cancer sites, from 29 census sub-divisions of the province of Alberta, collected over the period 1961 through 1981, were employed in this study. A total of 50,374 cases of cancer mortality were utilized. Correlations between pairs of cancer sites across census sub-divisions were calculated and cancer sites noted that varied little in mortality rates over Alberta's geographic areas. Significant correlations of mortalities (p less than 0.01) were observed between 5 pairs of male cancer and 18 pairs of female cancer sites. Risk factors common to correlating pairs are discussed. Similarities of our results with other studies are pointed out. The geographical distribution of extreme mortality correlations is analyzed and possible risk factors are discussed.

Factors influencing the survival of patients with cancer of the stomach.

During the period 1969 through 1973, 332 male and 135 female patients diagnosed with stomach cancer were registered with the Cross Cancer Institute in Edmonton, Alberta. These patients were followed up to December 31, 1981. Therefore, we were able to observe eight year survival times for all patients. Rates for one to eight years of survival were calculated using the Kaplan-Meier method. The results showed poor survival experience for male and female patients, similar to survival reported in other countries. Stomach cancer in Alberta belongs to the ten most common cancers and a search for factors influencing survival is therefore important. A large number of environmental factors and factors pertaining to the patients' lifestyle, as well as clinical factors related to stage of disease and treatment were examined using Cox's proportional hazard model. Surgical treatment and the presence of metastases were found to be important determinants of survival for both sexes. In males, increased age and British ethnicity were associated with poor survival prospects. Relative hazards of dying are presented for various combinations of factors.