Literature DB >> 8100269

CD4+ T cells that express high levels of CD45RB induce wasting disease when transferred into congenic severe combined immunodeficient mice. Disease development is prevented by cotransfer of purified CD4+ T cells.

P J Morrissey1, K Charrier, S Braddy, D Liggitt, J D Watson.   

Abstract

Purified CD4+ lymph node T cells were sorted into two populations on the basis of their expression of CD45RB (CD45RBhi and CD45RBlo) and injected into congenic severe combined immunodeficient (SCID) mice. After a period of time that was dependent on the number of cells injected, the SCID mice that received CD45RBhi/CD4+ T cells developed a wasting disease that was not seen in SCID mice that received the CD4+/CD45RBlo cells or whole lymph node cells. At death, SCID mice that received the CD4+/CD45RBhi cells had increased spleen and lymph node cellularity compared with normal SCID mice and SCID mice that received the CD4+/CD45RBlo T cells. The spleen and lymph node contained CD4+ cells and neither CD8+ nor surface immunoglobulin M-positive cells, plus a population of cells that did not express any of those markers. At necropsy, the SCID mice that received the CD4+/CD45RBhi cells had significant hyperplasia of the intestinal mucosa with significant lymphoid cell accumulation in the lamina propria. Interestingly, mice that received mixtures of whole lymph node or purified CD4+ cells with CD4+/CD45RBhi cells did not develop weight loss, indicating that the unseparated CD4+ population contained cells that were capable of regulating the reactivity of the CD4+/CD45RBhi cells.

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Year:  1993        PMID: 8100269      PMCID: PMC2191069          DOI: 10.1084/jem.178.1.237

Source DB:  PubMed          Journal:  J Exp Med        ISSN: 0022-1007            Impact factor:   14.307


  31 in total

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Review 2.  A functional dichotomy in CD4+ T lymphocytes.

Authors:  K Bottomly
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Authors:  U McKeever; J P Mordes; D L Greiner; M C Appel; J Rozing; E S Handler; A A Rossini
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Authors:  M L Birkeland; J Metlay; V M Sanders; R Fernandez-Botran; E S Vitetta; R M Steinman; E Puré
Journal:  J Mol Cell Immunol       Date:  1988

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Authors:  K Haskins; M McDuffie
Journal:  Science       Date:  1990-09-21       Impact factor: 47.728

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Authors:  K Croitoru; R H Stead; J Bienenstock; G Fulop; D G Harnish; L D Shultz; P K Jeffery; P B Ernst
Journal:  Eur J Immunol       Date:  1990-03       Impact factor: 5.532

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Authors:  A Bandeira; T Mota-Santos; S Itohara; S Degermann; C Heusser; S Tonegawa; A Coutinho
Journal:  J Exp Med       Date:  1990-07-01       Impact factor: 14.307

8.  Functional and ontogenetic analysis of murine CD45Rhi and CD45Rlo CD4+ T cells.

Authors:  W T Lee; X M Yin; E S Vitetta
Journal:  J Immunol       Date:  1990-05-01       Impact factor: 5.422

9.  The transfer of autoimmune diabetes in NOD mice can be inhibited or accelerated by distinct cell populations present in normal splenocytes taken from young males.

Authors:  P R Hutchings; A Cooke
Journal:  J Autoimmun       Date:  1990-04       Impact factor: 7.094

10.  OX-22high CD4+ T cells induce wasting disease with multiple organ pathology: prevention by the OX-22low subset.

Authors:  F Powrie; D Mason
Journal:  J Exp Med       Date:  1990-12-01       Impact factor: 14.307

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  137 in total

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7.  Characterisation of the T cell and dendritic cell repertoire in a murine model of mucopolysaccharidosis I (MPS I).

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8.  Emergent autoimmunity in graft-versus-host disease.

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Journal:  Blood       Date:  2005-03-03       Impact factor: 22.113

9.  Elimination of local macrophages in intestine prevents chronic colitis in interleukin-10-deficient mice.

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Review 10.  Probiotics and medical nutrition therapy.

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