Literature DB >> 17182551

Genetic manipulation of CD74 in mouse strains of different backgrounds can result in opposite responses to central nervous system injury.

Hadas Schori1, Ravid Shechter, Idit Shachar, Michal Schwartz.   

Abstract

The ability to recover from CNS injuries is strain dependent. Transgenic mice that weakly express the p41 CD74 isoform (an integral membrane protein functioning as a MHC class II chaperone) on an I-A(b) genetic background have normal CD4(+) T cell populations and normal surface expression of MHC class II, but their B cell development is arrested while the cells are still immature. After a CNS injury, these mice recover better than their matched wild-type controls. We generated p41-transgenic mice on an I-A(d) background (p41-I-A(d) mice), and found that their recovery from CNS injuries was worse than that of controls. A correlative inverse effect was seen with respect to the kinetics of T cell and B cell recruitment to the injured CNS and the expression of insulin-like growth factor at the lesion site. These results, besides verifying previous findings that B cells function in the damaged CNS, demonstrate that the outcome of a particular genetic manipulation may be strain dependent.

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Year:  2007        PMID: 17182551     DOI: 10.4049/jimmunol.178.1.163

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  5 in total

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4.  Lack of macrophage migration inhibitory factor in mice does not affect hallmarks of the inflammatory/immune response during the first week after stroke.

Authors:  Ana R Inácio; Richard Bucala; Tomas Deierborg
Journal:  J Neuroinflammation       Date:  2011-06-29       Impact factor: 8.322

5.  Traumatic brain injury causes selective, CD74-dependent peripheral lymphocyte activation that exacerbates neurodegeneration.

Authors:  Richard P Tobin; Sanjib Mukherjee; Jessica M Kain; Susannah K Rogers; Stephanie K Henderson; Heather L Motal; M Karen Newell Rogers; Lee A Shapiro
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  5 in total

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