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自然杀伤细胞存活依赖白细胞介素15的体内证据。

In vivo evidence for a dependence on interleukin 15 for survival of natural killer cells.

作者信息

Cooper Megan A, Bush Jennifer E, Fehniger Todd A, VanDeusen Jeffrey B, Waite Ross E, Liu Yang, Aguila Hector L, Caligiuri Michael A

机构信息

Department of Internal Medicine, Division of Hematology/Oncology, The James Cancer Hospital and Comprehensive Cancer Center, The Ohio State University, Columbus 43210, USA.

出版信息

Blood. 2002 Nov 15;100(10):3633-8. doi: 10.1182/blood-2001-12-0293. Epub 2002 Jul 5.

Abstract

Cellular homeostasis requires a balance between cell production, cell survival, and cell death. Production of natural killer (NK) cells from bone marrow precursor cells requires interleukin 15 (IL-15); however, very little is known about the factors controlling survival of mature NK cells in vivo. Because mice deficient in IL-15 (IL-15(-/-) mice) fail to develop NK cells, it is not known whether mature NK cells can survive in an environment lacking IL-15. We hypothesized that IL-15 might indeed be required for survival of mature NK cells in vivo. Freshly isolated NK cells labeled with 5-(and-6)-carboxyfluorescein diacetate, succinimidyl ester (CFSE) were adoptively transferred into IL-15(-/-) mice and littermate control (IL-15(+/-)) mice. Within 36 hours after transfer, NK cells were detected in both IL-15(-/-) and IL-15(+/-) mice; however, significantly more (P <.003) CFSE-positive (CFSE(+)) NK cells were found in control mice than in IL-15(-/-) mice. By 5 days, similar numbers of CFSE(+) NK cells were still easily detected in IL-15(+/-) mice, whereas no CFSE(+) NK cells survived in IL-15(-/-) mice. Furthermore, mice with severe combined immunodeficiency treated with the Fab fragment of a blocking antibody recognizing a signaling subunit of the IL-15 receptor, IL-2/15Rbeta, had a significant ( approximately 90%) loss of NK cells compared with control mice. Finally, NK cells from Bcl-2 transgenic mice that were adoptively transferred into IL-15(-/-) mice did survive. These results show conclusively that IL-15 is required for mature NK cell survival in vivo and suggest that IL-15 mediates its effect on NK cell survival by means of Bcl-2.

摘要

细胞内环境稳定需要细胞生成、细胞存活和细胞死亡之间保持平衡。骨髓前体细胞生成自然杀伤(NK)细胞需要白细胞介素15(IL-15);然而,对于体内控制成熟NK细胞存活的因素却知之甚少。由于缺乏IL-15的小鼠(IL-15(-/-)小鼠)无法发育出NK细胞,所以尚不清楚成熟NK细胞在缺乏IL-15的环境中是否能够存活。我们推测IL-15实际上可能是体内成熟NK细胞存活所必需的。将用5-(和-6)-羧基荧光素二乙酸琥珀酰亚胺酯(CFSE)标记的新鲜分离的NK细胞过继转移到IL-15(-/-)小鼠和同窝对照(IL-15(+/-))小鼠体内。转移后36小时内,在IL-15(-/-)和IL-15(+/-)小鼠体内均检测到NK细胞;然而,对照小鼠中发现的CFSE阳性(CFSE(+))NK细胞明显多于IL-15(-/-)小鼠(P <.003)。到第5天时,在IL-15(+/-)小鼠中仍能轻易检测到数量相似的CFSE(+) NK细胞,而在IL-15(-/-)小鼠中没有CFSE(+) NK细胞存活。此外,与对照小鼠相比,用识别IL-15受体信号亚基IL-2/15Rβ的阻断抗体的Fab片段处理的严重联合免疫缺陷小鼠,NK细胞显著减少(约90%)。最后,过继转移到IL-15(-/-)小鼠体内的Bcl-2转基因小鼠的NK细胞确实存活了下来。这些结果确凿地表明,IL-15是体内成熟NK细胞存活所必需的,并提示IL-15通过Bcl-2介导其对NK细胞存活的作用。

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