Inflammation in white matter: Clinical and pathophysiological aspects

  1. David Pleasure1,*,
  2. Athena Soulika1,
  3. Sunit K. Singh1,
  4. Vittorio Gallo2,
  5. Peter Bannerman3

Article first published online: 28 JUN 2006

DOI: 10.1002/mrdd.20100

Issue

Mental Retardation and Developmental Disabilities Research Reviews

Mental Retardation and Developmental Disabilities Research Reviews

Special Issue: White Matter Disorders

Volume 12, Issue 2, pages 141–146, 2006

Additional Information

How to Cite

Pleasure, D., Soulika, A., Singh, S. K., Gallo, V. and Bannerman, P. (2006), Inflammation in white matter: Clinical and pathophysiological aspects. Mental Retardation and Developmental Disabilities Research Reviews, 12: 141–146. doi: 10.1002/mrdd.20100

Author Information

  1. 1

    Deparment of Neurology, UC Davis School of Medicine, and Shriners Hospitals for Children Northern California, Sacramento, California 95817

  2. 2

    Chidren's National Medical Center, Washington, District of Columbia 20010

  3. 3

    Children's Hospital of Philadelphia, Philadelphia, Pennsylvania 19104

*Department of Neurology, UC Davis School of Medicine, c/o Shriners Hospital for Children, Northern California, 2425 Stockton Blvd., Sacramento CA 95817, USA

Publication History

  1. Issue published online: 28 JUN 2006
  2. Article first published online: 28 JUN 2006
  3. Manuscript Accepted: 5 MAR 2006
  4. Manuscript Received: 3 MAR 2006

Funded by

  • NINDS. Grant Number: NS25044
  • National MS Society. Grant Number: RG3523
  • Shriners Hospitals for Children

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Keywords:

  • axonal disruption;
  • inflammation;
  • multiple sclerosis;
  • oligodendroglia;
  • periventricular leukomalacia

Abstract

While the central nervous system (CNS) is generally thought of as an immunopriviledged site, immune-mediated CNS white matter damage can occur in both the perinatal period and in adults, and can result in severe and persistent neurological deficits. Periventricular leukomalacia (PVL) is an inflammatory white matter disease of premature infants that frequently results in cerebral palsy (CP). Clinical and experimental studies show that both hypoxic/ischemic and innate immune mechanisms contribute to the destruction of immature oligodendroglia and of axons in the deep cerebral white matter in PVL. No data are yet available as to whether there is any genetic predisposition to PVL or to its neurological sequelae. Multiple sclerosis (MS) is an inflammatory white matter disease that often begins in young adulthood, causes multifocal destruction of mature oligodendroglia and of axons, and eventually leads to substantial cumulative neurological disability. Certain genetic polymorphisms contribute to susceptibility to MS, and adaptive immune responses to myelin-associated self antigens, or to exogenous antigens that mimic these self antigens, play a central role in the pathophysiology of this disease. MRDD Research Reviews 2006;12:141–146. © 2006 Wiley-Liss, Inc.

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