Literature DB >> 11160401

Late oligodendrocyte progenitors coincide with the developmental window of vulnerability for human perinatal white matter injury.

S A Back1, N L Luo, N S Borenstein, J M Levine, J J Volpe, H C Kinney.   

Abstract

Hypoxic-ischemic injury to the periventricular cerebral white matter [periventricular leukomalacia (PVL)] results in cerebral palsy and is the leading cause of brain injury in premature infants. The principal feature of PVL is a chronic disturbance of myelination and suggests that oligodendrocyte (OL) lineage progression is disrupted by ischemic injury. We determined the OL lineage stages at risk for injury during the developmental window of vulnerability for PVL (23-32 weeks, postconceptional age). In 26 normal control autopsy human brains, OL lineage progression was defined in parietal white matter, a region of predilection for PVL. Three successive OL stages, the late OL progenitor, the immature OL, and the mature OL, were characterized between 18 and 41 weeks with anti-NG2 proteoglycan, O4, O1, and anti-myelin basic protein (anti-MBP) antibodies. NG2+O4+ late OL progenitors were the predominant stage throughout the latter half of gestation. Between 18 and 27 weeks, O4+O1+ immature OLs were a minor population (9.9 +/- 2.1% of total OLs; n = 9). Between 28 and 41 weeks, an increase in immature OLs to 30.9 +/- 2.1% of total OLs (n = 9) was accompanied by a progressive increase in MBP+ myelin sheaths that were restricted to the periventricular white matter. The developmental window of high risk for PVL thus precedes the onset of myelination and identifies the late OL progenitor as the major potential target. Moreover, the decline in incidence of PVL at approximately 32 weeks coincides with the onset of myelination in the periventricular white matter and suggests that the risk for PVL is related to the presence of late OL progenitors in the periventricular white matter.

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Year:  2001        PMID: 11160401      PMCID: PMC6762224     

Source DB:  PubMed          Journal:  J Neurosci        ISSN: 0270-6474            Impact factor:   6.167


  35 in total

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Authors:  A Nishiyama; A Chang; B D Trapp
Journal:  J Neuropathol Exp Neurol       Date:  1999-11       Impact factor: 3.685

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Review 3.  Dorsoventral patterning and oligodendroglial specification in the developing central nervous system.

Authors:  R J Hardy
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4.  Normal and reactive NG2+ glial cells are distinct from resting and activated microglia.

Authors:  A Nishiyama; M Yu; J A Drazba; V K Tuohy
Journal:  J Neurosci Res       Date:  1997-05-15       Impact factor: 4.164

5.  Identification, isolation, and promoter-defined separation of mitotic oligodendrocyte progenitor cells from the adult human subcortical white matter.

Authors:  N S Roy; S Wang; C Harrison-Restelli; A Benraiss; R A Fraser; M Gravel; P E Braun; S A Goldman
Journal:  J Neurosci       Date:  1999-11-15       Impact factor: 6.167

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Journal:  J Neurosci       Date:  1996-12-15       Impact factor: 6.167

7.  Multiple and novel specificities of monoclonal antibodies O1, O4, and R-mAb used in the analysis of oligodendrocyte development.

Authors:  R Bansal; A E Warrington; A L Gard; B Ranscht; S E Pfeiffer
Journal:  J Neurosci Res       Date:  1989-12       Impact factor: 4.164

8.  Immunocytochemical method to identify basic protein in myelin-forming oligodendrocytes of newborn rat C.N.S.

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Journal:  J Neurocytol       Date:  1978-04

9.  Maturation-dependent vulnerability of oligodendrocytes to oxidative stress-induced death caused by glutathione depletion.

Authors:  S A Back; X Gan; Y Li; P A Rosenberg; J J Volpe
Journal:  J Neurosci       Date:  1998-08-15       Impact factor: 6.167

Review 10.  Brain injury in the premature infant: overview of clinical aspects, neuropathology, and pathogenesis.

Authors:  J J Volpe
Journal:  Semin Pediatr Neurol       Date:  1998-09       Impact factor: 1.636

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8.  Differentiation of oligodendrocytes from mouse induced pluripotent stem cells without serum.

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9.  Rapid Infant Prefrontal Cortex Development and Sensitivity to Early Environmental Experience.

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