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人角质形成干细胞在短期原代离体培养中的生长动力学及调控。来自银屑病皮损T淋巴细胞的协同生长因子刺激银屑病非皮损区而非正常的角质形成干细胞增殖。

Kinetics and regulation of human keratinocyte stem cell growth in short-term primary ex vivo culture. Cooperative growth factors from psoriatic lesional T lymphocytes stimulate proliferation among psoriatic uninvolved, but not normal, stem keratinocytes.

作者信息

Bata-Csorgo Z, Hammerberg C, Voorhees J J, Cooper K D

机构信息

Immunodermatology Unit, University of Michigan, Ann Arbor 48109-0530.

出版信息

J Clin Invest. 1995 Jan;95(1):317-27. doi: 10.1172/JCI117659.

Abstract

Flow cytometric analysis of primary ex vivo keratinocyte cultures demonstrated that stem cells, (beta 1 integrin+, keratin 1/keratin 10 [K1/K10-], proliferating cell nuclear antigen [PCNA-] [Bata-Csorgo, Zs., C. Hammerberg, J. J. Voorhees, and K. D. Cooper. 1993. J. Exp. Med. 178:1271-1281]) establish such cultures. This methodology also enabled the quantitation of synchronized recruitment of these cells from G0 into G1 of the cell cycle (PCNA expression), which preceded bright beta 1 integrin expression. (beta 1 integrinbright expression has been shown to be a characteristic feature of keratinocyte stem cells in culture (Jones, P. H., and F. M. Watt. 1993. Cell. 73:713-724). Using the above assay, we determined whether lesional T lymphocytes in psoriasis could be directly responsible for the induction of the stem cell hyperproliferation that is characteristic of this disease. Indeed, CD4+ T lymphocytes, cloned from lesional psoriatic skin and stimulated by immobilized anti-CD3 plus fibronectin, promoted psoriatic uninvolved keratinocyte stem cell proliferation via soluble factors. This induction appeared to be through accelerated recruitment of stem cells from their quiescent state (G0) into cell cycle. By contrast, normal keratinocyte stem cells exhibited no such growth stimulation. Supernatants exhibiting growth induction all contained high levels of GM-CSF and gamma-IFN, low IL-3 and TNF-alpha, and variable IL-4. Only anti-gamma-IFN antibody was able to neutralize growth stimulatory activity of the supernatants on psoriatic uninvolved keratinocyte stem cells. However, because recombinant gamma-IFN alone inhibited growth in this assay, these data suggest that, in psoriasis, gamma-IFN acts cooperatively with other growth factors in the immune induction of cell cycle progression by the normally quiescent stem cell keratinocytes.

摘要

对原代离体角质形成细胞培养物进行的流式细胞术分析表明,干细胞(β1整合素阳性、角蛋白1/角蛋白10 [K1/K10-]、增殖细胞核抗原[PCNA-] [巴塔-乔尔戈,兹., C. 哈默贝格,J. J. 沃尔希斯,和K. D. 库珀。1993年。《实验医学杂志》178:1271 - 1281])建立了此类培养物。该方法还能够对这些细胞从G0期同步募集进入细胞周期的G1期(PCNA表达)进行定量,这先于β1整合素的明亮表达。(已表明β1整合素明亮表达是培养的角质形成细胞干细胞的一个特征 [琼斯,P. H., 和F. M. 瓦特。1993年。《细胞》73:713 - 724])。使用上述检测方法,我们确定了银屑病皮损中的T淋巴细胞是否可能直接导致了该疾病特有的干细胞过度增殖。实际上,从银屑病皮损皮肤克隆并经固定化抗CD3加纤连蛋白刺激的CD4 + T淋巴细胞,通过可溶性因子促进了银屑病非皮损角质形成细胞干细胞的增殖。这种诱导似乎是通过加速干细胞从静止状态(G0)进入细胞周期实现的。相比之下,正常角质形成细胞干细胞未表现出这种生长刺激。表现出生长诱导作用的上清液均含有高水平的GM - CSF和γ - IFN、低水平的IL - 3和TNF - α以及可变水平的IL - 4。只有抗γ - IFN抗体能够中和上清液对银屑病非皮损角质形成细胞干细胞的生长刺激活性。然而,由于单独的重组γ - IFN在该检测中抑制生长,这些数据表明,在银屑病中,γ - IFN与其他生长因子协同作用,在免疫诱导正常静止的干细胞角质形成细胞进入细胞周期过程中发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b23e/295434/143fd3cf241b/jcinvest00023-0339-a.jpg

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