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利用单细胞组学技术解析人类脂肪组织异质性。

Dissecting human adipose tissue heterogeneity using single-cell omics technologies.

机构信息

Unit of Cellular Networks and Molecular Therapeutic Targets, IRCCS Regina Elena National Cancer Institute, 00144, Rome, Italy.

Fondazione Policlinico Universitario Agostino Gemelli IRCCS, 00168, Rome, Italy.

出版信息

Stem Cell Res Ther. 2024 Sep 27;15(1):322. doi: 10.1186/s13287-024-03931-w.

Abstract

Single-cell omics technologies that profile genes (genomic and epigenomic) and determine the abundance of mRNA (transcriptomic), protein (proteomic and secretomic), lipids (lipidomic), and extracellular matrix (matrisomic) support the dissection of adipose tissue heterogeneity at unprecedented resolution in a temporally and spatially defined manner. In particular, cell omics technologies may provide innovative biomarkers for the identification of rare specific progenitor cell subpopulations, assess transcriptional and proteomic changes affecting cell proliferation and immunomodulatory potential, and accurately define the lineage hierarchy and differentiation status of progenitor cells. Unraveling adipose tissue complexity may also provide for the precise assessment of a dysfunctional state, which has been associated with cancer, as cancer-associated adipocytes play an important role in shaping the tumor microenvironment supporting tumor progression and metastasis, obesity, metabolic syndrome, and type 2 diabetes mellitus. The information collected by single-cell omics has relevant implications for regenerative medicine because adipose tissue is an accessible source of multipotent cells; alternative cell-free approaches, including the use of adipose tissue stromal cell-conditioned medium, extracellular vesicles, or decellularized extracellular matrix, are clinically valid options. Subcutaneous white adipose tissue, which is generally harvested via liposuction, is highly heterogeneous because of intrinsic biological variability and extrinsic inconsistencies in the harvesting and processing procedures. The current limited understanding of adipose tissue heterogeneity impinges on the definition of quality standards appropriate for clinical translation, which requires consistency and uniformity of the administered product. We review the methods used for dissecting adipose tissue heterogeneity and provide an overview of advances in omics technology that may contribute to the exploration of heterogeneity and dynamics of adipose tissue at the single-cell level.

摘要

单细胞组学技术可以分析基因(基因组和表观基因组),并确定 mRNA(转录组)、蛋白质(蛋白质组和分泌组)、脂质(脂质组)和细胞外基质(基质组)的丰度,以支持以空前的分辨率在时间和空间上定义的方式剖析脂肪组织的异质性。特别是,细胞组学技术可以为鉴定罕见的特定祖细胞亚群提供创新的生物标志物,评估影响细胞增殖和免疫调节潜力的转录和蛋白质变化,并准确定义祖细胞的谱系层次结构和分化状态。揭示脂肪组织的复杂性还可以为功能失调状态提供精确评估,这种状态与癌症有关,因为癌症相关脂肪细胞在塑造支持肿瘤进展和转移的肿瘤微环境方面起着重要作用,与肥胖、代谢综合征和 2 型糖尿病有关。单细胞组学收集的信息对再生医学具有重要意义,因为脂肪组织是多能细胞的可及来源;替代无细胞方法,包括使用脂肪组织基质细胞条件培养基、细胞外囊泡或脱细胞细胞外基质,是临床有效的选择。通常通过吸脂术采集的皮下白色脂肪组织由于内在生物学变异性和采集及处理过程中的外在不一致性而高度异质。目前对脂肪组织异质性的有限理解影响了适合临床转化的质量标准的定义,这需要所给予产品的一致性和均一性。我们回顾了剖析脂肪组织异质性的方法,并概述了组学技术的进展,这些进展可能有助于探索脂肪组织在单细胞水平上的异质性和动态。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b28/11437900/700552943ae4/13287_2024_3931_Fig1_HTML.jpg

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