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首页> 外文期刊>Developmental Immunology: Journal of Immunology Research >TCR Vα- and V?-Gene Segment Use in T-CellSubcultures Derived from a Type-III Bare LymphocyteSyndrome Patient Deficient in MHC Class-II Expression
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TCR Vα- and V?-Gene Segment Use in T-CellSubcultures Derived from a Type-III Bare LymphocyteSyndrome Patient Deficient in MHC Class-II Expression

机译:来自MHC II类表达不足的III型裸淋巴细胞综合征患者的T细胞亚培养中的TCRVα和Vα基因片段使用

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摘要

Previously, we and others have shown that MHC class-II deficient humans have greatlyreduced numbers of CD4+CD8– peripheral T cells. These type-III Bare LymphocyteSyndrome patients lack MHC class-II and have an impaired MHC class-I antigenexpression. In this study, we analyzed the impact of the MHC class-II deficientenvironment on the TCR V-gene segment usage in this reduced CD4+CD8– T-cellsubset. For these studies, we employed TcR V-region-specific monoclonal antibodies(mAbs) and a semiquantitative PCR technique with Vαand V?amplimers, specific foreach of the most known Vα- and V?;-gene region families. The results of our studiesdemonstrate that some of the Vα-gene segments are used less frequent in theCD4+CD8– T-cell subset of the patient, whereas the majority of the TCR Vα- andV?-gene segments investigated were used with similar frequencies in both subsets in thetype-III Bare Lymphocyte Syndrome patient compared to healthy control familymembers. Interestingly, the frequency of TcR Vα12 transcripts was greatly diminishedin the patient, both in the CD4+CD8– as well as in the CD4–CD8+ compartment,whereas this gene segment could easily be detected in the healthy family controls. Onthe basis of the results obtained in this study, it is concluded that within the reducedCD4+CD8– T-cell subset of this patient, most of the TCR V-gene segments tested for areemployed. However, a skewing in the usage frequency of some of the Vα-gene segmentstoward the CD4–CD8+ T-cell subset was noticeable in the MHC class-II deficient patientthat differed from those observed in the healthy family controls.
机译:以前,我们和其他人已经证明,缺乏MHC II类的人类已经大大减少了CD4 + CD8-外周血T细胞的数量。这些III型裸淋巴细胞综合征患者缺乏II类MHC,并且MHC I类抗原表达受损。在这项研究中,我们分析了MHC II类缺陷环境对这种减少的CD4 + CD8-T细胞亚群中TCR V基因片段使用的影响。在这些研究中,我们采用了TcR V区特异性单克隆抗体(mAbs),并使用了Vα和VΔamplimer的半定量PCR技术,这些技术分别针对最知名的Vα-和Vα-基因家族。我们的研究结果表明,在患者的CD4 + CD8–T细胞亚群中,某些Vα基因片段的使用频率较低,而大多数TCRVα和Vβ基因片段的使用频率相似。与健康对照家庭成员相比,III型裸淋巴细胞综合征患者的两个亚组。有趣的是,无论是在CD4 + CD8–区,还是在CD4–CD8 +区室,患者的TcRVα12转录物的频率都大大降低了,而在健康的家庭对照中很容易检测到该基因片段。根据这项研究获得的结果,可以得出结论,在该患者的CD4 + CD8–T细胞减少的亚群中,使用了大多数测试的TCR V基因片段。但是,在MHC II类缺陷患者中,一些Vα基因片段的使用频率向CD4-CD8 + T细胞亚群的倾斜是明显的,这与健康家庭对照中观察到的有所不同。

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