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神經(jīng)干細(xì)胞和蛋白質(zhì)組學(xué)

 GCTA 2022-06-11 發(fā)布于貴州


Neural Stem Cells (NSCs) and Proteomics.


|核心內(nèi)容:

神經(jīng)干細(xì)胞(NSCs)可以自我更新,形成中樞神經(jīng)系統(tǒng)的主要細(xì)胞類型,。

神經(jīng)干細(xì)胞的研究包括原代,、中樞神經(jīng)系統(tǒng)來(lái)源的細(xì)胞以及動(dòng)物和人類胚胎干細(xì)胞(ESC)來(lái)源和誘導(dǎo)多能干細(xì)胞(IPSC)來(lái)源的研究。

神經(jīng)干細(xì)胞為研究正常的神經(jīng)發(fā)育,、神經(jīng)退行性變和神經(jīng)系統(tǒng)疾病提供了一種手段,,也是受損和疾病的中樞神經(jīng)系統(tǒng)細(xì)胞修復(fù)的臨床相關(guān)來(lái)源。

對(duì)神經(jīng)干細(xì)胞的蛋白質(zhì)組學(xué)研究有可能描繪出對(duì)神經(jīng)干細(xì)胞生物學(xué)至關(guān)重要的分子和途徑,,以及神經(jīng)干細(xì)胞參與神經(jīng)修復(fù)的途徑,。

在這篇綜述中,我們提供了NSC生物學(xué)的背景知識(shí),,包括獲得NSC的方法和這些過(guò)程的注意事項(xiàng),。

然后,我們關(guān)注神經(jīng)干細(xì)胞蛋白質(zhì)組學(xué)研究的進(jìn)展,。這包括翻譯后修飾(PTM)的分析,;分析不同蛋白質(zhì)組間(如分泌組)的方法;以及分析蛋白質(zhì)組中的時(shí)間差異以闡明分化機(jī)制的方法,。

我們還討論了一些在神經(jīng)干細(xì)胞研究中無(wú)疑會(huì)有用但尚未應(yīng)用于該領(lǐng)域的方法,。

雖然許多對(duì)神經(jīng)干細(xì)胞的蛋白質(zhì)組學(xué)研究在很大程度上編目了特定細(xì)胞狀態(tài)的蛋白質(zhì)組或翻譯后修飾,但沒(méi)有深入研究特定的功能,,一些研究導(dǎo)致了對(duì)功能過(guò)程的理解或識(shí)別出無(wú)法通過(guò)其他手段識(shí)別的標(biāo)記,。

該領(lǐng)域仍然存在許多挑戰(zhàn),包括用于蛋白質(zhì)組分析的神經(jīng)干細(xì)胞的精確鑒定和標(biāo)準(zhǔn)化,,以及如何將基礎(chǔ)蛋白質(zhì)組學(xué)研究轉(zhuǎn)化為功能生物學(xué),。

下一層次的研究將需要跨學(xué)科的方法,將那些對(duì)蛋白質(zhì)組學(xué)生物化學(xué)感興趣的人的技能與那些對(duì)調(diào)節(jié)NSC功能感興趣的人的技能結(jié)合起來(lái),。


原文摘要:


Neural stem cells (NSCs) can self-renew and give rise to the major cell types of the CNS. Studies of NSCs include the investigation of primary, CNS-derived cells as well as animal and human embryonic stem cell (ESC)-derived and induced pluripotent stem cell (iPSC)-derived sources. NSCs provide a means with which to study normal neural development, neurodegeneration, and neurological disease and are clinically relevant sources for cellular repair to the damaged and diseased CNS. Proteomics studies of NSCs have the potential to delineate molecules and pathways critical for NSC biology and the means by which NSCs can participate in neural repair. In this review, we provide a background to NSC biology, including the means to obtain them and the caveats to these processes. We then focus on advances in the proteomic interrogation of NSCs. This includes the analysis of posttranslational modifications (PTMs); approaches to analyzing different proteomic compartments, such the secretome; as well as approaches to analyzing temporal differences in the proteome to elucidate mechanisms of differentiation. We also discuss some of the methods that will undoubtedly be useful in the investigation of NSCs but which have not yet been applied to the field. While many proteomics studies of NSCs have largely catalogued the proteome or posttranslational modifications of specific cellular states, without delving into specific functions, some have led to understandings of functional processes or identified markers that could not have been identified via other means. Many challenges remain in the field, including the precise identification and standardization of NSCs used for proteomic analyses, as well as how to translate fundamental proteomics studies to functional biology. The next level of investigation will require interdisciplinary approaches, combining the skills of those interested in the biochemistry of proteomics with those interested in modulating NSC function.




參考文獻(xiàn):https:///10.1074/mcp.O115.052704

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