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克隆性扩增的CD28-CD8+ T细胞中端粒缩短,这意味着其复制历史与CD28+CD8+对应细胞不同。

Shortened telomeres in clonally expanded CD28-CD8+ T cells imply a replicative history that is distinct from their CD28+CD8+ counterparts.

作者信息

Monteiro J, Batliwalla F, Ostrer H, Gregersen P K

机构信息

Department of Medicine, North Shore University Hospital/Cornell University Medical College, Manhasset, NY 11030, USA.

出版信息

J Immunol. 1996 May 15;156(10):3587-90.

PMID:8621891
Abstract

Long term in vitro culture of clonally expanded CD8+T cells, generally found within the CD57+ or CD28-subset, has generally been unsuccessful, suggesting that these cells may have a limited replicative potential. Telomeric shortening may reflect the action of a "mitotic clock" regulating the number of divisions a cell can undergo. In this study, we have compared the telomeric lengths of CD28-CD8+ and CD28+CD8+ T cells in 10 normal individuals to assess their replicative history. Overall, the telomeric lengths were found to be significantly shorter in the CD28-CD8+ T cell subset compared with the CD28+CD8+ subset. Furthermore, clonally expanded TCRBV11+CD8+ T cells from an individual exhibited telomeric lengths that were 2.9 kb shorter than those found in the polyclonal CD28+CD8+ T cell subset. These findings indicate that clonally expanded CD28-CD8+ T cells have undergone many more rounds of replication than CD28+CD8+ T cells, and consistent with the loss of CD28 expression, they may have reached a state of replicative senescence.

摘要

克隆扩增的CD8 + T细胞通常存在于CD57 +或CD28 -亚群中,其长期体外培养一般不成功,这表明这些细胞可能具有有限的复制潜力。端粒缩短可能反映了调节细胞可经历分裂次数的“有丝分裂时钟”的作用。在本研究中,我们比较了10名正常个体中CD28 - CD8 +和CD28 + CD8 + T细胞的端粒长度,以评估它们的复制历史。总体而言,发现CD28 - CD8 + T细胞亚群的端粒长度明显短于CD28 + CD8 +亚群。此外,来自一名个体的克隆扩增的TCRBV11 + CD8 + T细胞的端粒长度比多克隆CD28 + CD8 + T细胞亚群中的端粒长度短2.9 kb。这些发现表明,克隆扩增的CD28 - CD8 + T细胞比CD28 + CD8 + T细胞经历了更多轮的复制,并且与CD28表达的丧失一致,它们可能已达到复制衰老状态。

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