中文摘要:
產(chǎn)生血小板的巨核細胞 (MKs) 主要存在于骨髓中���,它們在每個(gè)細胞周期中復制其 DNA 含量�,從而產(chǎn)生具有復雜分界膜系統的多倍體細胞�����。雖然已經(jīng)確定了血小板形成過(guò)程中細胞骨架重組的關(guān)鍵要素���,但是什么開(kāi)始血小板釋放到血管竇中�����,在很大程度上仍然難以捉摸����。使用細胞周期指標����,我們觀(guān)察到一種現象��,在此期間���,MKs 中擴增的中心體在有絲分裂后發(fā)生聚集��,緊接著(zhù)是血小板形成�,這僅發(fā)生在間期的 G1 中�。G1 中的強制細胞周期停滯不僅增加了體外前血小板的形成�,而且在小鼠短期饑餓后也增加了體內前血小板的形成��。我們發(fā)現����,中心體蛋白驅動(dòng)蛋白家族成員 C1 (KIFC1) 的抑制損害了聚集和隨后的血小板形成�,而 KIFC1 缺陷小鼠表現出血小板計數降低���?����?傊?����,我們發(fā)現 KIFC1 和細胞周期介導的中心體聚集是 MKs 前血小板形成的重要起始因子����。
英文摘要:
Platelet-producing megakaryocytes (MKs) primarily reside in the bone marrow, where they duplicate their DNA content with each cell cycle resulting in polyploid cells with an intricate demarcation membrane system. While key elements of the cytoskeletal reorganizations during proplatelet formation have been identified, what initiates the release of platelets into vessel sinusoids remains largely elusive. Using a cell cycle indicator, we observed a unique phenomenon, during which amplified centrosomes in MKs underwent clustering following mitosis, closely followed by proplatelet formation, which exclusively occurred in G1 of interphase. Forced cell cycle arrest in G1 increased proplatelet formation not only in vitro but also in vivo following short-term starvation of mice. We identified that inhibition of the centrosomal protein kinesin family member C1 (KIFC1) impaired clustering and subsequent proplatelet formation, while KIFC1-deficient mice exhibited reduced platelet counts. In summary, we identified KIFC1- and cell cycle–mediated centrosome clustering as an important initiator of proplatelet formation from MKs.
論文信息:
論文題目:Cell cycle–dependent centrosome clustering precedes proplatelet formation
期刊名稱(chēng):SCIENCE ADVANCES
時(shí)間期卷: Vol 10, Issue 25
在線(xiàn)時(shí)間:2024年6月19日
DOI: 10.1126/sciadv.adl6153
Emfret血小板清除抗體R300檢測圖:
Emfret血小板清除抗體R300引用截圖:
血小板來(lái)源于主要存在于骨髓 (BM) 內的大型祖細胞巨核細胞 (MK) ����。在從造血干細胞發(fā)育過(guò)程中���,MK 會(huì )增加 mRNA 和蛋白質(zhì)合成�����,積累專(zhuān)門(mén)的顆粒�,并形成血小板生成所需的內陷膜儲庫 [分界膜系統 (DMS)] ����。然后���,MK 將稱(chēng)為血小板前體的長(cháng)突起(每個(gè)突起由血小板大小的腫脹組成)擠出到血管竇中�����,在那里它們發(fā)生額外的形態(tài)變化以產(chǎn)生循環(huán)血小板 �����。MK 表達 β1-微管蛋白的譜系特異性同工型��,該同工型經(jīng)翻譯后修飾以介導前血小板形成 ��。在血小板產(chǎn)生之前�����,微管分布在整個(gè) MK 細胞質(zhì)中�。然而��,一旦血小板形成���,微管就會(huì )排列在細胞皮層中����,其中動(dòng)力蛋白依賴(lài)性微管滑動(dòng)力會(huì )促進(jìn)伸長(cháng)�����。迄今為止�,尚未研究微管的這種重新分布是如何發(fā)生的��。此外�,雖然近年來(lái)已經(jīng)確定了血小板制備和釋放的重要分子介質(zhì) ���,但直接誘導 MK 釋放前血小板的原因仍然未知����。
