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α-酮戊二酸加速啟動的人多能干細(xì)胞的初始分化

 GCTA 2022-06-11 發(fā)布于貴州


α-Ketoglutarate Accelerates the Initial Differentiation of Primed Human Pluripotent Stem Cell


|核心內(nèi)容:

多能干細(xì)胞(PSCs)可以從特定培養(yǎng)條件下建立的原始或更多分化、啟動、多潛能狀態(tài)自我更新或分化。

細(xì)胞內(nèi)α-酮戊二酸(α-KG)濃度的增加有利于幼鼠胚胎干細(xì)胞(MESCs)的自我更新。

αKG或αKG/琥珀酸水平對人PSCs和小鼠上皮干細(xì)胞分化的影響尚不清楚。

我們檢測了啟動的hPSCs和EpiSCs,發(fā)現(xiàn)αKG或αKG/琥珀酸比值的增加加速,而琥珀酸水平的升高延遲了啟動的PSC的分化

αKG已被證明可以抑制線粒體ATP合成酶,并調(diào)節(jié)表觀基因組修飾的雙加氧酶。

線粒體解偶聯(lián)不妨礙αKG加速啟動的PSC分化。

取而代之的是,αKG誘導(dǎo)和琥珀酸化受損的PSCs的整體組蛋白和脫氧核糖核酸去甲基化。

這些數(shù)據(jù)支持αKG促進(jìn)自我更新或分化,取決于多能性狀態(tài)。
原文摘要:


Pluripotent stem cells (PSCs) can self-renew or differentiate from naive or more differentiated, primed, pluripotent states established by specific culture conditions. Increased intracellular α-ketoglutarate (αKG) was shown to favor self-renewal in naive mouse embryonic stem cells (mESCs). The effect of αKG or αKG/succinate levels on differentiation from primed human PSCs (hPSCs) or mouse epiblast stem cells (EpiSCs) remains unknown. We examined primed hPSCs and EpiSCs and show that increased αKG or αKG-to-succinate ratios accelerate, and elevated succinate levels delay, primed PSC differentiation. αKG has been shown to inhibit the mitochondrial ATP synthase and to regulate epigenome-modifying dioxygenase enzymes. Mitochondrial uncoupling did not impede αKG-accelerated primed PSC differentiation. Instead, αKG induced, and succinate impaired, global histone and DNA demethylation in primed PSCs. The data support αKG promotion of self-renewal or differentiation depending on the pluripotent state.


#αKG就像一個催化加速劑,naive細(xì)胞就像在原地轉(zhuǎn)圈圈,αKG只能讓細(xì)胞原地轉(zhuǎn)得更快,可以鞏固保持原地不動的狀態(tài)。但是primed細(xì)胞已經(jīng)做出命運(yùn)決定,αKG當(dāng)然會加速該決定。

參考文獻(xiàn):http:///backend/ptpmcrender.fcgi?accid=PMC5023506&blobtype=pdf

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