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小鼠造血系统的连续消耗与再生。对造血组织及细胞衰老研究的意义。

Serial depletion and regeneration of the murine hematopoietic system. Implications for hematopoietic organization and the study of cellular aging.

作者信息

Ross E A, Anderson N, Micklem H S

出版信息

J Exp Med. 1982 Feb 1;155(2):432-44. doi: 10.1084/jem.155.2.432.

Abstract

The mouse hematopoietic system was subjected to repeated depletion and regeneration either by serial transfer of bone marrow cells through lethally irradiated recipients or by repeated treatment with the cycle-active drug hydroxyurea (HU). The capacity of surviving stem cells to proliferate and self-renew was assayed at intervals by two methods: (a) the spleen colony method; and (b) competitive repopulation of irradiated recipients using chromosome markers, with normal bone marrow cells as an internal control. The progressive decline in stem cell function that occurred during serial transfer of bone marrow and that had already begun after a single transfer was not seen during HU treatment; up to 25 pairs of HU injections given over more than 1 yr had no discernible effect on the number of stem cells present 3 wk after the final injection or on their capacity to self-renew. Within 2 d after exposure to HU, the average self-renewal capacity of surviving stem cells was enhanced. This implies that the drug selectively eliminates poorly self-renewing stem cells and hence that these enter cycle more readily than stem cells with a high self-replicative potential. However, the fact of being in cycle at the time of injection did not of itself affect self-renewal. The results show that serial transfer of bone marrow is not a valid method for studying clonal aging phenomena because it does not fulfill the assumptions on which such studies are based. No evidence was obtained for any intrinsic limitation in the capacity of bone marrow populations for repeated regeneration after HU-induced depletion. However, this does not necessarily imply that individual hematopoietic clones are capable of indefinite expansion because hematopoiesis may (as suggested by the relative resistance of highly self-replicative stem cells to mitogenic signals) proceed on the basis of clonal succession.

摘要

通过将骨髓细胞连续移植到经致死剂量照射的受体中,或通过用细胞周期活性药物羟基脲(HU)反复处理,对小鼠造血系统进行反复的耗竭和再生。通过两种方法定期测定存活干细胞的增殖和自我更新能力:(a)脾集落法;(b)使用染色体标记物对经照射的受体进行竞争性再增殖,以正常骨髓细胞作为内部对照。在骨髓连续移植过程中发生的干细胞功能的逐渐下降,在单次移植后就已经开始,而在HU处理期间未观察到这种情况;在超过1年的时间内给予多达25对HU注射,对最后一次注射后3周时存在的干细胞数量或其自我更新能力没有明显影响。在接触HU后2天内,存活干细胞的平均自我更新能力增强。这意味着该药物选择性地消除了自我更新能力差的干细胞,因此这些干细胞比具有高自我复制潜力的干细胞更容易进入细胞周期。然而,注射时处于细胞周期这一事实本身并不影响自我更新。结果表明,骨髓连续移植不是研究克隆衰老现象的有效方法,因为它没有满足此类研究基于的假设。没有获得证据表明HU诱导的耗竭后骨髓群体反复再生的能力存在任何内在限制。然而,这不一定意味着单个造血克隆能够无限扩增,因为造血可能(如高度自我复制的干细胞对有丝分裂信号的相对抗性所表明的)基于克隆更替进行。

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本文引用的文献

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