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原位谱系追踪揭示了人前列腺上皮干细胞命运的一个共同克隆起源,即基底细胞和腔细胞。

In situ lineage tracking of human prostatic epithelial stem cell fate reveals a common clonal origin for basal and luminal cells.

机构信息

Mitochondrial Research Group, Institute for Ageing and Health, Newcastle University, Newcastle upon Tyne, UK.

出版信息

J Pathol. 2011 Oct;225(2):181-8. doi: 10.1002/path.2965.

DOI:10.1002/path.2965
PMID:21898876
Abstract

Stem cells accumulate mitochondrial DNA (mtDNA) mutations resulting in an observable respiratory chain defect in their progeny, allowing the mapping of stem cell fate. There is considerable uncertainty in prostate epithelial biology where both basal and luminal stem cells have been described, and in this study the clonal relationships within the human prostate epithelial cell layers were explored by tracing stem cell fate. Fresh-frozen and formalin-fixed histologically-benign prostate samples from 35 patients were studied using sequential cytochrome c oxidase (COX)/succinate dehydrogenase (SDH) enzyme histochemistry and COX subunit I immunofluorescence to identify areas of respiratory chain deficiency; mtDNA mutations were identified by whole mitochondrial genome sequencing of laser-captured areas. We demonstrated that cells with respiratory chain defects due to somatic mtDNA point mutations were present in prostate epithelia and clonally expand in acini. Lineage tracing revealed distinct patterning of stem cell fate with mtDNA mutations spreading throughout the whole acinus or, more commonly, present as mosaic acinar defects. This suggests that individual acini are typically generated from multiple stem cells, and the presence of whole COX-deficient acini suggests that a single stem cell can also generate an entire branching acinar subunit of the gland. Significantly, a common clonal origin for basal, luminal and neuroendocrine cells is demonstrated, helping to resolve a key area of debate in human prostate stem cell biology.

摘要

干细胞积累线粒体 DNA(mtDNA)突变,导致其后代出现可观察到的呼吸链缺陷,从而可以追踪干细胞的命运。前列腺上皮生物学存在很大的不确定性,其中已经描述了基底和腔干细胞,在这项研究中,通过追踪干细胞的命运来探索人前列腺上皮细胞层内的克隆关系。使用连续细胞色素 c 氧化酶(COX)/琥珀酸脱氢酶(SDH)酶组织化学和 COX 亚基 I 免疫荧光对 35 名患者的新鲜冷冻和福尔马林固定的组织学良性前列腺样本进行研究,以识别呼吸链缺陷区域;通过对激光捕获区域的整个线粒体基因组进行测序来鉴定 mtDNA 突变。我们证明,由于体细胞 mtDNA 点突变导致呼吸链缺陷的细胞存在于前列腺上皮中,并在腺泡中克隆性扩张。谱系追踪显示,干细胞命运具有明显的模式,mtDNA 突变遍布整个腺泡,或者更常见的是,呈现镶嵌性腺泡缺陷。这表明单个腺泡通常由多个干细胞产生,并且整个 COX 缺陷腺泡的存在表明单个干细胞也可以产生整个腺泡分支的腺单位。重要的是,证明了基底细胞、腔细胞和神经内分泌细胞具有共同的克隆起源,有助于解决人类前列腺干细胞生物学中一个关键的争论领域。

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In situ lineage tracking of human prostatic epithelial stem cell fate reveals a common clonal origin for basal and luminal cells.原位谱系追踪揭示了人前列腺上皮干细胞命运的一个共同克隆起源,即基底细胞和腔细胞。
J Pathol. 2011 Oct;225(2):181-8. doi: 10.1002/path.2965.
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Cell lineage tracing in human epithelial tissues using mitochondrial DNA mutations as clonal markers.利用线粒体DNA突变作为克隆标记对人类上皮组织进行细胞谱系追踪。
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