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淋巴组织中 Asrij 扰动的蛋白质组学分析,以鉴定造血新调控因子。

Proteomics of Asrij Perturbation in Lymph Glands for Identification of New Regulators of Hematopoiesis.

机构信息

From the ‡Jawaharlal Nehru Centre for Advanced Scientific Research, Jakkur, Bangalore 560064, India.

§Institute of Bioinformatics, International Technology Park, Bangalore 560066, India.

出版信息

Mol Cell Proteomics. 2019 Jun;18(6):1171-1182. doi: 10.1074/mcp.RA119.001299. Epub 2019 Mar 28.

Abstract

Hematopoiesis is the process of differentiation of precursor blood cells into mature blood cells that is controlled by a complex set of molecular interactions. Understanding hematopoiesis is important for the study of hematological disorders. However, a comprehensive understanding of how physiological and genetic mechanisms regulate blood cell precursor maintenance and differentiation is lacking. Owing to simplicity and ease of genetic analysis, the lymph gland (LG) is an excellent model to study hematopoiesis. Here, we quantitatively analyzed the LG proteome under genetic conditions that either maintain precursors or promote their differentiation , by perturbing expression of Asrij, a conserved endosomal regulator of hematopoiesis. Using iTRAQ-based quantitative proteomics, we determined the relative expression levels of proteins in Asrij-knockout and overexpressing LGs from 1500 larval dissections compared with wild type. Our data showed that at least 6.5% of the proteome is expressed in wild type LGs. Of the 2133 proteins identified, 780 and 208 proteins were common to previously reported cardiac tube and hemolymph proteomes, respectively, resulting in the identification of 1238 proteins exclusive to the LG. Perturbation of Asrij levels led to differential expression of 619 proteins, of which 27% have human homologs implicated in various diseases. Proteins regulating metabolism, immune system, signal transduction and vesicle-mediated transport were significantly enriched. Immunostaining of representative candidates from the enriched categories and previous reports confirmed 73% of our results, indicating the validity of our LG proteome. Our study provides, for the first time, an proteomics resource for identifying novel regulators of hematopoiesis that will also be applicable to understanding vertebrate blood cell development.

摘要

造血是指前体细胞分化为成熟血细胞的过程,该过程受一系列复杂的分子相互作用的控制。了解造血对于研究血液疾病非常重要。然而,人们对于生理和遗传机制如何调节血细胞前体的维持和分化还缺乏全面的认识。由于淋巴腺(LG)具有简单的遗传分析特性,因此是研究造血的极佳模型。在这里,我们通过扰乱内体中造血保守调节因子 Asrij 的表达,在维持前体细胞或促进其分化的遗传条件下,定量分析了 LG 的蛋白质组。通过 iTRAQ 基于定量蛋白质组学,我们将与野生型相比,从 1500 个幼虫解剖中确定了 Asrij 敲除和过表达 LG 中的蛋白质的相对表达水平。我们的数据表明,至少有 6.5%的蛋白质组在野生型 LG 中表达。在鉴定的 2133 种蛋白质中,有 780 种和 208 种蛋白质分别与先前报道的心脏管和血淋巴蛋白质组共有,从而鉴定出 1238 种仅存在于 LG 的蛋白质。Asrij 水平的波动导致 619 种蛋白质的差异表达,其中 27%的蛋白质具有与人相关的同源物,这些同源物与各种疾病有关。调节代谢,免疫系统,信号转导和囊泡介导的运输的蛋白质明显富集。对来自富集类别的代表性候选蛋白进行免疫染色,以及对先前报道的验证,证实了我们的 73%的结果,这表明了我们的 LG 蛋白质组的有效性。我们的研究首次提供了一种蛋白质组学资源,用于鉴定新的造血调节因子,这也将适用于理解脊椎动物血细胞的发育。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/834b/6553936/ad245fb6bce8/zjw0061959360007.jpg

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