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不同白细胞亚群中 MHC Ⅰ类分子的差异表达。

Differential MHC class I expression in distinct leukocyte subsets.

机构信息

Department of Pathology and Laboratory Medicine, University of Wisconsin-Madison, Madison, 53706 Wisconsin, USA.

出版信息

BMC Immunol. 2011 Jul 15;12:39. doi: 10.1186/1471-2172-12-39.

Abstract

BACKGROUND

MHC class I proteins are partly responsible for shaping the magnitude and focus of the adaptive cellular immune response. In humans, conventional wisdom suggests that the HLA-A, -B, and -C alleles are equally expressed on the majority of cell types. While we currently have a thorough understanding of how total MHC class I expression varies in different tissues, it has been difficult to examine expression of single MHC class I alleles due to the homogeneity of MHC class I sequences. It is unclear how cDNA species are expressed in distinct cell subsets in humans and particularly in macaques which transcribe upwards of 20 distinct MHC class I alleles at variable levels.

RESULTS

We examined MHC gene expression in human and macaque leukocyte subsets. In humans, while we detected overall differences in locus transcription, we found that transcription of MHC class I genes was consistent across the leukocyte subsets we studied with only small differences detected. In contrast, transcription of certain MHC cDNA species in macaques varied dramatically by up to 45% between different subsets. Although the Mafa-B134:02 RNA is virtually undetectable in CD4+ T cells, it represents over 45% of class I transcripts in CD14+ monocytes. We observed parallel MHC transcription differences in rhesus macaques. Finally, we analyzed expression of select MHC proteins at the cell surface using fluorescent peptides. This technique confirmed results from the transcriptional analysis and demonstrated that other MHC proteins, known to restrict SIV-specific responses, are also differentially expressed among distinct leukocyte subsets.

CONCLUSIONS

We assessed MHC class I transcription and expression in human and macaque leukocyte subsets. Until now, it has been difficult to examine MHC class I allele expression due to the similarity of MHC class I sequences. Using two novel techniques we showed that expression varies among distinct leukocyte subsets of macaques but does not vary dramatically in the human cell subsets we examined. These findings suggest pathogen tropism may have a profound impact on the shape and focus of the MHC class I restricted CD8+ T cell response in macaques.

摘要

背景

MHC Ⅰ类蛋白部分负责塑造适应性细胞免疫反应的幅度和焦点。在人类中,传统观点认为 HLA-A、-B 和 -C 等位基因在大多数细胞类型上的表达水平相当。虽然我们目前对不同组织中总 MHC Ⅰ类表达的变化有了全面的了解,但由于 MHC Ⅰ类序列的同质性,很难检查单个 MHC Ⅰ类等位基因的表达。目前尚不清楚 cDNA 物种在人类不同细胞亚群中的表达情况,特别是在猕猴中,其转录的 20 多种不同的 MHC Ⅰ类等位基因的表达水平各不相同。

结果

我们检查了人类和猕猴白细胞亚群中的 MHC 基因表达。在人类中,虽然我们检测到了基因转录的总体差异,但我们发现我们研究的白细胞亚群中 MHC Ⅰ类基因的转录是一致的,只有很小的差异。相比之下,猕猴中某些 MHC cDNA 物种的转录差异高达 45%,不同亚群之间差异显著。尽管 Mafa-B134:02 RNA 在 CD4+T 细胞中几乎无法检测到,但它在 CD14+单核细胞中代表了超过 45%的 I 类转录本。我们在恒河猴中观察到了类似的 MHC 转录差异。最后,我们使用荧光肽在细胞表面分析了选择 MHC 蛋白的表达。这项技术证实了转录分析的结果,并表明其他已知限制 SIV 特异性反应的 MHC 蛋白在不同的白细胞亚群中也存在差异表达。

结论

我们评估了人类和猕猴白细胞亚群中的 MHC Ⅰ类转录和表达。到目前为止,由于 MHC Ⅰ类序列的相似性,检查 MHC Ⅰ类等位基因的表达一直很困难。使用两种新的技术,我们表明在猕猴的不同白细胞亚群中表达存在差异,但在我们检查的人类细胞亚群中没有显著变化。这些发现表明,病原体嗜性可能对猕猴 MHC Ⅰ类限制性 CD8+T 细胞反应的形态和焦点产生深远影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/18e8/3155488/39ef99bf1784/1471-2172-12-39-1.jpg

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