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一项简单的细胞增殖测定和炎症蛋白含量在年轻和老年受试者的人血浆中显示出显著差异。

A simple cell proliferation assay and the inflammatory protein content show significant differences in human plasmas from young and old subjects.

作者信息

Muraglia A, Utyro O, Nardini M, Santolini M, Ceresa D, Agostini V, Nencioni A, Filaci G, Cancedda R, Mastrogiacomo M

机构信息

Dipartimento di Medicina Interna e Specialità Mediche (DIMI), Università Degli Studi di Genova, Genova, Italy.

IRCCS Ospedale Policlinico San Martino, Genova, Italy.

出版信息

Front Bioeng Biotechnol. 2024 Sep 9;12:1408499. doi: 10.3389/fbioe.2024.1408499. eCollection 2024.

Abstract

Some studies showed a "rejuvenating" effect of exposing aging tissues to a young environment. In mouse heterochronic parabiosis experiments, in response to young organisms, old animals lived longer than isochrony old age-matched conjoint animals. Comparable "rejuvenating" effects were obtained by injecting young plasma in old mice. This raised great hopes of slowing down the senescence process in humans by the injection of young plasma, as well as to prevent or cure age-related diseases. Some clinical trials are currently being performed or were recently completed. However, these studies are small and of limited duration, and we still lack convincing evidence to support the effectiveness of young plasma injection. It is urgent to perform additional investigations, including the development of an assay to measure the cell proliferation induction capability of different human plasmas, before one can seriously think of a large-scale treatment of humans. We adopted a simple method to measure the potential of different plasmas in supporting cell line proliferation, regardless of the co-presence of a platelet lysate. By comparing plasmas from young and old subjects, we observed a decreased activity in plasmas from old individuals. The young plasma effect may be attributed to specific proteins and growth factors more abundant in younger individuals that could decrease with age. Alternatively, or at the same time, the reduced cell proliferation support could be due to inhibitors present in the old plasma. Studying the different protein content of young and old plasmas was out of the scope of this article. Such differences should be adequately investigated by proteomics using many samples. However, a preliminary study of the different protein content of young and old plasmas was part of the assay validation using a commercially available cytokine array for parallel determination of the relative levels of 105 selected human proteins. We could show the existence of specific differences between young and old plasmas and that plasmas from old individuals presented a higher concentration of "inflammatory" proteins.

摘要

一些研究表明,将衰老组织置于年轻环境中会产生“年轻化”效应。在小鼠异时联体共生实验中,与年轻生物体共生的老年动物比与年龄匹配的同龄联体动物寿命更长。给老年小鼠注射年轻血浆也能获得类似的“年轻化”效应。这让人们燃起了通过注射年轻血浆来减缓人类衰老过程以及预防或治疗与年龄相关疾病的巨大希望。目前正在进行一些临床试验,有些最近已经完成。然而,这些研究规模较小且持续时间有限,我们仍然缺乏令人信服的证据来支持注射年轻血浆的有效性。在认真考虑对人类进行大规模治疗之前,迫切需要进行更多的研究,包括开发一种检测方法来测量不同人类血浆诱导细胞增殖的能力。我们采用了一种简单的方法来测量不同血浆支持细胞系增殖的潜力,而不考虑血小板裂解物的共存情况。通过比较年轻和老年受试者的血浆,我们观察到老年个体血浆中的活性降低。年轻血浆的效应可能归因于年轻个体中更丰富的特定蛋白质和生长因子,这些物质可能会随着年龄增长而减少。或者,同时,细胞增殖支持能力的降低可能是由于老年血浆中存在的抑制剂。研究年轻和老年血浆中不同的蛋白质含量不在本文的讨论范围内。这种差异应该通过蛋白质组学对大量样本进行充分研究。然而,使用市售细胞因子阵列平行测定105种选定人类蛋白质的相对水平,对年轻和老年血浆中不同蛋白质含量的初步研究是检测方法验证的一部分。我们能够证明年轻和老年血浆之间存在特定差异,并且老年个体的血浆中“炎症”蛋白质的浓度更高。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b4fb/11440192/b167773da969/fbioe-12-1408499-g001.jpg

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