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细胞介导免疫的适应性独立于 repertoire 多样性。 (注:这里“repertoire”在医学免疫等领域可能有特定含义,比如免疫细胞受体库等,但仅按要求翻译字面意思)

Fitness of cell-mediated immunity independent of repertoire diversity.

作者信息

AbuAttieh Mouhammed, Rebrovich Michelle, Wettstein Peter J, Vuk-Pavlovic Zvezdana, Limper Andrew H, Platt Jeffrey L, Cascalho Marilia

机构信息

Transplantation Biology Program, Mayo Clinic College of Medicine, 200 First Street SW, Rochester, MN 55905, USA.

出版信息

J Immunol. 2007 Mar 1;178(5):2950-60. doi: 10.4049/jimmunol.178.5.2950.

Abstract

Fitness of cell-mediated immunity is thought to depend on TCR diversity; however, this concept has not been tested formally. We tested the concept using JH(-/-) mice that lack B cells and have TCR Vbeta diversity <1% that of wild-type mice and quasimonoclonal (QM) mice with oligoclonal B cells and TCR Vbeta diversity 7% that of wild-type mice. Despite having a TCR repertoire contracted >99% and defective lymphoid organogenesis, JH(-/-) mice rejected H-Y-incompatible skin grafts as rapidly as wild-type mice. JH(-/-) mice exhibited T cell priming by peptide and delayed-type hypersensitivity, although these responses were less than normal owing either to TCR repertoire contraction or defective lymphoid organogenesis. QM mice with TCR diversity contracted >90%, and normal lymphoid organs rejected H-Y incompatible skin grafts as rapidly as wild type mice and exhibited normal T cell priming and normal delayed-type hypersensitivity reactions. QM mice also resisted Pneumocystis murina like wild-type mice. Thus, cell-mediated immunity can function normally despite contractions of TCR diversity >90% and possibly >99%.

摘要

细胞介导免疫的适应性被认为取决于TCR多样性;然而,这一概念尚未得到正式验证。我们使用JH(-/-)小鼠(缺乏B细胞,TCR Vβ多样性低于野生型小鼠的1%)和准单克隆(QM)小鼠(具有寡克隆B细胞且TCR Vβ多样性为野生型小鼠的7%)来验证这一概念。尽管JH(-/-)小鼠的TCR库收缩超过99%且淋巴器官发生存在缺陷,但它们排斥H-Y不相容皮肤移植物的速度与野生型小鼠一样快。JH(-/-)小鼠表现出肽诱导的T细胞致敏和迟发型超敏反应,尽管由于TCR库收缩或淋巴器官发生缺陷,这些反应低于正常水平。TCR多样性收缩超过90%且淋巴器官正常的QM小鼠排斥H-Y不相容皮肤移植物的速度与野生型小鼠一样快,并表现出正常的T细胞致敏和正常的迟发型超敏反应。QM小鼠也像野生型小鼠一样抵抗鼠肺孢子菌。因此,尽管TCR多样性收缩超过90%甚至可能超过99%,细胞介导免疫仍能正常发挥功能。

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