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Development cell:神经干细胞如何决定增殖或分化 - 何时决定? [复制链接]

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楼主
发表于 2010-12-10 11:35 |只看该作者 |倒序浏览 |打印
本帖最后由 qingshui1985 于 2010-12-10 11:38 编辑
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2 L# E$ J5 v1 f2 X: M7 |. Y主题:Development cell:神经干细胞如何决定增殖或分化 - 何时决定?) j/ \  c: g% U/ E) Q1 ?3 j. L9 y
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说明:原文来源http://www.sciencedaily.com/releases/2010/11/101115122635.htm; M. O: h% c& z8 P3 t7 M  W" ~
由干细胞之家新闻小组成员qingshui1985翻译(转帖请注明)' l: f' z- N5 ^1 Q7 U
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新加坡国立大学研究生医学院的研究人员发现有一种新的精细控制大脑干细胞平衡的反馈机制。
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' [! Y3 e3 p3 T) `* vZif,是一种新发现的蛋白,参与调控神经干细胞是将自我更新还是将分化为各种专能的神经元(神经细胞)。8 \$ ]: l" Y/ e( P

7 v* s; {% `9 {# r4 a" r前期工作,研究人员发现 zif通过调控增殖因子aPKC(注:aPKC的过度表达诱发成神经细胞自我更新)使神经干细胞维持在适当水平。因而,它对抑制果蝇神经干细胞的增殖具有重要作用。
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/ R( V5 F6 K$ [1 t0 J' E/ W“人体内也具有一个 zif 相关蛋白,其功能有待进一步研究” 资深学者王红岩博士(音译)说:“我们的发现对于未来研究这一蛋白在一些疾病如胶质母细胞瘤(脑肿瘤中最严重的一种疾病)中的作用,铺平了道路”
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! {, ^/ I. g$ K+ z0 }* x她说未来有可能利用zif蛋白的功能来形成一种治疗脑肿瘤的新方法。这项研究结果发表在《Development cell》杂志11月16日上。
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& O+ w! g+ a1 N) V& e5 U2 \, b研究结果表明,缺乏zif蛋白的表达与果蝇神经干细胞过量密切相关。
4 f8 B* h. M% O" a% u3 o9 ?该机制形成了一个调控回路:zif是一种转录因子,可以抑制apkc的产生。但是zif也可以被apkc磷酸化,进而使zif离开细胞核导致zif的失活,此时神经干细胞反过来将要发生增殖。
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- M4 i5 F/ U& q“下一步,我们想研究神经干细胞在哺乳动物自我更新的机制,我们正在寻找相关的合作者”他说。“我们还将继续使用果蝇为模型,寻找果蝇中神经干细胞的自我更新的关键成员,这样我们可以了解更多的与这一调控相关的基因网络。* y; F/ H7 k4 G. s/ \5 H4 w

) J' I8 V3 `% w) ~& w* Y这项工作受到新加坡国立大学 神经科学与行为失调研究项目、新加坡卫生部教育部、新加坡国家基础研究项目、Temasek生命科学等基金资助。2 F/ C( O+ g7 _! C
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个人翻译,理解不准确的语句还望大家积极指出。
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沙发
发表于 2010-12-10 11:36 |只看该作者
英文稿件原文:
! z0 B. F; O* ?Researchers at Duke-NUS Graduate Medical School in Singapore have uncovered a novel feedback mechanism that controls the delicate balance of brain stem cells.7 |3 \/ B1 l% Z: W3 [5 {

% J# t6 X8 |; J) g- u7 zZif, a newly discovered protein, controls whether brain stem cells renew themselves as stem cells or differentiate into a dedicated type of neuron (nerve cell).
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In preclinical studies, the researchers showed that Zif is important for inhibiting overgrowth of neural stem cells in fruit flies (genus Drosophila) by ensuring that a proliferation factor (known as aPKC) maintains appropriate levels in neural stem cells.$ q% R! {; H  x4 r; S6 c
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"There is a Zif-related protein in humans, and its function remains to be analyzed," said senior and corresponding author Hongyan Wang, Ph.D. "Our finding has paved the way for future study of this human protein in the context of diseases, including glioblastomas, the most severe form of brain tumors."
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She said it may be "possible to manipulate Zif function into a form of therapy against diseases, including cancer."
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The study was published in the Nov. 16 issue of Developmental Cell journal.
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# k) r( O/ i. V: b1 qThe findings suggest that a lack of Zif protein expression correlates with neural stem cell overpopulation in Drosophila.3 S( q5 S' P' D4 {8 L) F
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The mechanism is circular: Zif is a transcription factor that inhibits the manufacture of aPKC. But Zif can also be tagged with a phosphate by aPKC, which excludes Zif from the cell nucleus, and leads to Zif inactivation, which in turn means an overgrowth of stem cells.4 F7 a; m) H1 m: [
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"Next, we would like to investigate the mechanisms of neural stem cells' self-renewal in mammals, and we are looking for the right collaborators," Wang said. "We will also continue to use Drosophila as a powerful model system to uncover critical players in neural stem cell self-renewal so that we can understand the network involved in this regulation."0 E+ A7 e5 w. {9 x' r0 K

; k0 T. D, t" ROther authors on the paper included four co-lead authors, Kai Chen Chang and Gisela Garcia Alvarez of the Neuroscience and Behavioral Disorder Program at Duke-NUS Graduate Medical School; Gregory Somers of the Department of Genetics, La Trobe Institute for Molecular Science (LIMS), La Trobe University, in Australia; and Rita Sousa-Nunes of the National Institute for Medical Research, Mill Hill, in London. Fabrizio Rossi is from the Cell Division Group, IRB-Barcelona, PCB, in Barcelona, Swee Beng Soon is also with Duke-NUS Neuroscience and Behavioral Disorder Program, and Cayetano Gonzalez is with both the Cell Division Group, IRB-Barcelona, and the Institucio Catalana de Recera Estudis Advancats in Barcelona. William Chia and Kai Chen Chang are both with the Temasek Life Science Laboratory in Singapore.
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' J& V* p  E. z& p/ h* PThis work is supported by the Duke-NUS Neuroscience & Behavioral Disorders Signature Research Program funded by A*STAR and Ministry of Health, Ministry of Education in Singapore, and the Singapore National Research Foundation, as well as by Temasek Life Sciences funding.
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Journal Reference:
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1 o: ]  ~) K, e$ Q0 s9 v. i: {* P  SKai Chen Chang, Gisela Garcia-Alvarez, Gregory Somers, Rita Sousa-Nunes, Fabrizio Rossi, Ying Ying Lee, Swee Beng Soon, Cayetano Gonzalez, William Chia, Hongyan Wang. Interplay between the Transcription Factor Zif and aPKC Regulates Neuroblast Polarity and Self-Renewal. Developmental Cell, Volume 19, Issue 5, 778-785, 16 November 2010 DOI: 10.1016/j.devcel.2010.10.007
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藤椅
发表于 2010-12-12 10:40 |只看该作者
有原文么?

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板凳
发表于 2010-12-12 11:16 |只看该作者
干细胞之家微信公众号
回复 tjutiger 的帖子
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( i' l7 W+ D' b# y, e, Q% G& Q2 VKai Chen Chang, Gisela Garcia-Alvarez, Gregory Somers, Rita Sousa-Nunes, Fabrizio Rossi, Ying Ying Lee, Swee Beng Soon, Cayetano Gonzalez, William Chia, Hongyan Wang. Interplay between the Transcription Factor Zif and aPKC Regulates Neuroblast Polarity and Self-Renewal. Developmental Cell, Volume 19, Issue 5, 778-785, 16 November 2010 DOI: 10.1016/j.devcel.2010.10.007
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报纸
发表于 2010-12-16 21:18 |只看该作者
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地板
发表于 2010-12-24 11:06 |只看该作者
神经干细胞定向分化干预还是一个科学上的难题,可以学习一下作者的思路,继续寻求适合的方式,谢谢了
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发表于 2011-1-16 18:36 |只看该作者
我现在也在做分化感觉不好做
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