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X连锁重症联合免疫缺陷症携带者自然杀伤细胞中的非随机X染色体失活

Nonrandom X chromosome inactivation in natural killer cells from obligate carriers of X-linked severe combined immunodeficiency.

作者信息

Wengler G S, Allen R C, Parolini O, Smith H, Conley M E

机构信息

Department of Pediatrics, University of Tennessee, Memphis.

出版信息

J Immunol. 1993 Jan 15;150(2):700-4.

PMID:8093460
Abstract

X-linked severe combined immunodeficiency (XSCID) is characterized by hypogammaglobulinemia, markedly reduced numbers of T cells, absent mitogen responses, decreased numbers of NK cells, and normal or elevated numbers of B cells. The abnormalities in the NK cell and B cell lineages could be attributed to dependence of these cell lineages on T cells or T cell-derived factors, or to expression of the XSCID gene defect in these cell lineages. In past experiments, we have examined X chromosome inactivation patterns in T cells and cultured B cells from female obligate carriers of XSCID and have found that both cell lineages demonstrate nonrandom X chromosome inactivation. This indicates that the gene defect is intrinsic to both of these cell lineages. In the present experiments, a polymerase chain reaction technique was used to evaluate X chromosome inactivation patterns in highly purified populations of freshly isolated NK cells, B cells, CD4+ cells, and CD8+ cells from three obligate carriers of XSCID. All four lymphoid cell populations from these three women exhibited exclusive use of a single X as the active X. In contrast, both X chromosomes were used as the active X in neutrophils and monocytes. These findings indicate that the XSCID gene is expressed in the NK cell lineage as well as in T cells and B cells. This observation makes it highly unlikely that the XSCID gene is involved in Ag receptor gene rearrangements.

摘要

X连锁重症联合免疫缺陷(XSCID)的特征为低丙种球蛋白血症、T细胞数量显著减少、无丝裂原反应、NK细胞数量减少以及B细胞数量正常或升高。NK细胞和B细胞谱系的异常可能归因于这些细胞谱系对T细胞或T细胞衍生因子的依赖,或者归因于XSCID基因缺陷在这些细胞谱系中的表达。在过去的实验中,我们检测了XSCID女性义务携带者的T细胞和培养的B细胞中的X染色体失活模式,发现这两种细胞谱系均表现出非随机的X染色体失活。这表明基因缺陷在这两种细胞谱系中都是内在的。在本实验中,采用聚合酶链反应技术评估了来自三名XSCID义务携带者的新鲜分离的NK细胞、B细胞、CD4 +细胞和CD8 +细胞的高度纯化群体中的X染色体失活模式。这三名女性的所有四个淋巴细胞群体均仅使用一条X染色体作为活性X染色体。相比之下,中性粒细胞和单核细胞中两条X染色体均被用作活性X染色体。这些发现表明XSCID基因在NK细胞谱系以及T细胞和B细胞中均有表达。这一观察结果使得XSCID基因参与抗原受体基因重排的可能性极小。

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