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永生化的小鼠附睾头部上皮细胞系(mECap18)再现了体内环境。

Immortalized mouse caput epididymal epithelial (mECap18) cell line recapitulates the in-vivo environment.

机构信息

Priority Research Centre for Reproductive Science, School of Environmental and Life Sciences, College of Engineering, Science and Environment, The University of Newcastle, Callaghan, New South Wales, Australia.

Infertility and Reproduction Research Program, Hunter Medical Research Institute, New Lambton, New South Wales, Australia.

出版信息

Proteomics. 2024 Apr;24(7):e2300253. doi: 10.1002/pmic.202300253. Epub 2023 Sep 27.

Abstract

Residing between the testes and the vas deferens, the epididymis is a highly convoluted tubule whose unique luminal microenvironment is crucial for the functional maturation of spermatozoa. This microenvironment is created by the combined secretory and resorptive activity of the lining epididymal epithelium, including the release of extracellular vesicles (epididymosomes), which encapsulate fertility modulating proteins and a myriad of small non-coding RNAs (sncRNAs) that are destined for delivery to recipient sperm cells. To enable investigation of this intercellular communication nexus, we have previously developed an immortalized mouse caput epididymal epithelial cell line (mECap18). Here, we describe the application of label-free mass spectrometry to characterize the mECap18 cell proteome and compare this to the proteome of native mouse caput epididymal epithelial cells. We report the identification of 5,313 mECap18 proteins, as many as 75.8% of which were also identified in caput epithelial cells wherein they mapped to broadly similar protein classification groupings. Furthermore, key pathways associated with protein synthesis (e.g., EIF2 signaling) and cellular protection in the male reproductive tract (e.g., sirtuin signaling) were enriched in both proteomes. This comparison supports the utility of the mECap18 cell line as a tractable in-vitro model for studying caput epididymal epithelial cell function.

摘要

附睾位于睾丸和输精管之间,是一个高度卷曲的管状结构,其独特的管腔微环境对于精子的功能成熟至关重要。这种微环境是由附睾上皮的分泌和吸收活动共同创造的,包括释放细胞外囊泡(附睾小体),其中包含调节生育能力的蛋白质和大量旨在递送给受体细胞的小非编码 RNA(sncRNA)。为了能够研究这种细胞间通讯的枢纽,我们之前开发了一种永生化的小鼠附睾头部上皮细胞系(mECap18)。在这里,我们描述了使用无标记质谱法来描述 mECap18 细胞蛋白质组,并将其与天然小鼠附睾头部上皮细胞的蛋白质组进行比较。我们报告了 5313 种 mECap18 蛋白的鉴定,多达 75.8%的蛋白也在附睾上皮细胞中被鉴定出来,它们映射到广泛相似的蛋白质分类分组中。此外,与蛋白质合成(例如 EIF2 信号转导)和男性生殖道细胞保护(例如 Sirtuin 信号转导)相关的关键途径在两个蛋白质组中都得到了富集。这种比较支持了 mECap18 细胞系作为研究附睾头部上皮细胞功能的可行体外模型的实用性。

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