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一种自然杀伤性NKR-P1A+/CD56-/CD16-功能性不成熟人类自然杀伤细胞亚群的定义,该亚群在白细胞介素12存在的情况下可在体外分化。

Definition of a natural killer NKR-P1A+/CD56-/CD16- functionally immature human NK cell subset that differentiates in vitro in the presence of interleukin 12.

作者信息

Bennett I M, Zatsepina O, Zamai L, Azzoni L, Mikheeva T, Perussia B

机构信息

Kimmel Cancer Institute, Jefferson Medical College, Philadelphia, Pennsylvania 19107, USA.

出版信息

J Exp Med. 1996 Nov 1;184(5):1845-56. doi: 10.1084/jem.184.5.1845.

Abstract

Human natural killer (NK) cell differentiation from immature lineage negative (Lin-) umbilical cord blood cells was examined in vitro. Cells expressing differentiation antigens of mature NK cells (CD56, CD16, CD2, CD8, NKR-P1A) were generated from Lin- cells cultured with interleukin (IL)-2 and a murine bone marrow stromal cell line expressing the human membrane-bound form of stem cell factor. Two subsets of NK cells were identified in these cultures: one expressed both NKR-P1A and CD56 and, in variable proportions, all other NK cell differentiation antigens; the second subset expressed only NKR-P1A and, unlike the former, was not cytotoxic. Neither subset expressed interferon (IFN)-gamma mRNA even after stimulation with phorbol di-ester and Ca2+ ionophore, but both expressed tumor necrosis factor alpha mRNA and the cytotoxic granule-associated proteins TIA-1, perforin, and serine esterase-1. After 10-d culture with IL-2, IL-12, and irradiated B lymphoblastoid cells, approximately 45% of the NKR-P1A+/ CD56- cells became CD56+, and the same cultures contained cells capable of cytotoxicity and of IFN-gamma production. These results indicate that NKR-P1A expression in the absence of other NK cell markers defines an intermediate, functionally immature stage of NK cell differentiation, and that effector functions develop in these cells, concomitantly with CD56 expression, in the presence of IL-12. These cells likely represent the counterpart of a CD3-/NKR-P1A+/ CD56-/CD16- cell subset that, as shown here, is present both in adult and neonatal circulating lymphocytes.

摘要

我们在体外检测了人自然杀伤(NK)细胞从不成熟的谱系阴性(Lin-)脐带血细胞中的分化情况。在用白细胞介素(IL)-2和表达人膜结合形式干细胞因子的小鼠骨髓基质细胞系培养的Lin-细胞中,产生了表达成熟NK细胞分化抗原(CD56、CD16、CD2、CD8、NKR-P1A)的细胞。在这些培养物中鉴定出了两个NK细胞亚群:一个同时表达NKR-P1A和CD56,并以可变比例表达所有其他NK细胞分化抗原;第二个亚群仅表达NKR-P1A,与前者不同的是,它没有细胞毒性。即使在用佛波酯和Ca2+离子载体刺激后,这两个亚群均不表达干扰素(IFN)-γ mRNA,但两者均表达肿瘤坏死因子α mRNA以及细胞毒性颗粒相关蛋白TIA-1、穿孔素和丝氨酸酯酶-1。在用IL-2、IL-12和经辐照的B淋巴母细胞进行10天培养后,约45%的NKR-P1A+/CD56-细胞变成了CD56+,并且相同培养物中含有具有细胞毒性和能够产生IFN-γ的细胞。这些结果表明,在缺乏其他NK细胞标志物的情况下NKR-P1A的表达定义了NK细胞分化的一个中间的、功能上不成熟的阶段,并且在IL-12存在的情况下,效应功能在这些细胞中与CD56表达同时发展。这些细胞可能代表了CD3-/NKR-P1A+/CD56-/CD16-细胞亚群的对应物,如本文所示,该亚群存在于成人和新生儿循环淋巴细胞中。

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