Per Soelberg Sørensen scite author profile

Accurate clinical course descriptions (phenotypes) of multiple sclerosis (MS) are important for communication, prognostication, design and recruitment of clinical trials, and treatment decision-making. Standardized descriptions published in 1996 based on a survey of international MS experts provided purely clinical phenotypes based on data and consensus at that time, but imaging and biological correlates were lacking. Increased understanding of MS and its pathology, coupled with general concern that the original descriptors may not adequately reflect more recently identified clinical aspects of the disease, prompted a re-examination of MS disease phenotypes by the International Advisory Committee on Clinical Trials of MS. While imaging and biological markers that might provide objective criteria for separating clinical phenotypes are lacking, we propose refined descriptors that include consideration of disease activity (based on clinical relapse rate and imaging findings) and disease progression. Strategies for future research to better define phenotypes are also outlined.

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A Placebo-Controlled Trial of Oral Cladribine for Relapsing Multiple Sclerosis

Giovannoni

Comi

Cook³

et al. 2010

N Engl J Med

804

962

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The changing demographic pattern of multiple sclerosis epidemiology

Koch‐Henriksen

Sørensen

2010

The Lancet Neurology

963

688

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Effect of early interferon treatment on conversion to definite multiple sclerosis: a randomised study

et al. 2001

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Acute Respiratory Tract Infections and Mannose-Binding Lectin Insufficiency During Early Childhood

Koch

Melbye²,

Sørensen³

et al. 2001

JAMA

389

312

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Factors influencing success of clinical genome sequencing across a broad spectrum of disorders

et al. 2015

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To assess factors influencing the success of whole genome sequencing for mainstream clinical diagnosis, we sequenced 217 individuals from 156 independent cases across a broad spectrum of disorders in whom prior screening had identified no pathogenic variants. We quantified the number of candidate variants identified using different strategies for variant calling, filtering, annotation and prioritisation. We found that jointly calling variants across samples, filtering against both local and external databases, deploying multiple annotation tools and using familial transmission above biological plausibility contributed to accuracy. Overall, we identified disease causing variants in 21% of cases, rising to 34% (23/68) for Mendelian disorders and 57% (8/14) in trios. We also discovered 32 potentially clinically actionable variants in 18 genes unrelated to the referral disorder, though only four were ultimately considered reportable. Our results demonstrate the value of genome sequencing for routine clinical diagnosis, but also highlight many outstanding challenges.Users may view, print, copy, and download text and data-mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use

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A systematic review of the incidence and prevalence of comorbidity in multiple sclerosis: Overview

et al. 2015

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Background:Comorbidity is an area of increasing interest in multiple sclerosis (MS).Objective:The objective of this review is to estimate the incidence and prevalence of comorbidity in people with MS and assess the quality of included studies.Methods:We searched the PubMed, SCOPUS, EMBASE and Web of Knowledge databases, conference proceedings, and reference lists of retrieved articles. Two reviewers independently screened abstracts. One reviewer abstracted data using a standardized form and the abstraction was verified by a second reviewer. We assessed study quality using a standardized approach. We quantitatively assessed population-based studies using the I2 statistic, and conducted random-effects meta-analyses.Results:We included 249 articles. Study designs were variable with respect to source populations, case definitions, methods of ascertainment and approaches to reporting findings. Prevalence was reported more frequently than incidence; estimates for prevalence and incidence varied substantially for all conditions. Heterogeneity was high.Conclusion:This review highlights substantial gaps in the epidemiological knowledge of comorbidity in MS worldwide. Little is known about comorbidity in Central or South America, Asia or Africa. Findings in North America and Europe are inconsistent. Future studies should report age-, sex- and ethnicity-specific estimates of incidence and prevalence, and standardize findings to a common population.

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Consistent high viral load of human papillomavirus 16 and risk of cervical carcinoma in situ: a nested case-control study

et al. 2000

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