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Hemopoietic precursor cell defects in nonanemic but stem cell-deficient W44/W44 mice.

作者信息

Barker J E, McFarland E C

机构信息

Jackson Laboratory, Bar Harbor, Maine 04609.

出版信息

J Cell Physiol. 1988 Jun;135(3):533-8. doi: 10.1002/jcp.1041350324.

DOI:10.1002/jcp.1041350324
PMID:3397389
Abstract

Hematopoietic stem cell deficiencies cause a severe macrocytic anemia in W/Wv mice. W44/W44 mice, on the other hand, are not anemic, but, since they accept marrow implants without prior total body irradiation, they have inherited a stem cell lesion. In an attempt to identify the aberrant stem cell(s), we have determined the concentration in W44/W44 marrow of hematopoietic precursors known to be deficient in W/Wv marrow. The in vitro erythroid burst-forming units (BFU-E), the in vivo spleen colony-forming units (CFU-S), and the cells that repopulate the erythroid compartment of stem cell-deficient mice were examined. The progenitors of 7-day bursts are dramatically reduced in W/Wv marrow but are present in normal concentrations in W44/W44 marrow. W44/W44 marrow CFU-S, unlike W/Wv, generate visible spleen colonies 10 days after injection into lethally irradiated recipients. The colonies are, however, smaller and at least 2 times less numerous than those produced from equivalent numbers of +/+ marrow. An additional defect was the inability of W44/W44 stem cells to compete with genetically marked +/+ cells during erythroid repopulation. An estimate of the number of W44/W44 stem cells needed to compete with +/+ cells was provided by enriching W44/W44 progenitors fivefold. Twice as many enriched W44/W44 marrow cells as unfractionated +/+ cells were required to replace competitor cells. This suggests that there are up to 10 times fewer stem cells somewhere in the W44/W44 erythrogenerative pathway. The data support the conclusion that an erythroid progenitor less mature than the BFU-E is one of the cells most severely affected by expression of the mutant gene.

摘要

相似文献

1
Hemopoietic precursor cell defects in nonanemic but stem cell-deficient W44/W44 mice.
J Cell Physiol. 1988 Jun;135(3):533-8. doi: 10.1002/jcp.1041350324.
2
Reconstitution of the W/Wv stem cell differentiation defect by infection with Rauscher leukemia virus.通过劳氏肉瘤病毒感染重建W/Wv干细胞分化缺陷。
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Analysis of the hematopoietic effects of new dominant spotting (W) mutations of the mouse. I. Influence upon hematopoietic stem cells.小鼠新的显性斑点(W)突变的造血作用分析。I. 对造血干细胞的影响。
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4
Studies of W mutant mice provide evidence for alternate mechanisms capable of activating hematopoietic stem cells.对W突变小鼠的研究为能够激活造血干细胞的替代机制提供了证据。
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Megakaryocytopoiesis and granulopoiesis in W/Wv mice: comparisons between bone marrow and spleen.W/Wv小鼠的巨核细胞生成和粒细胞生成:骨髓与脾脏的比较
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Aging and hematopoiesis. II. The ability of bone marrow cells from young and aged mice to cure and maintain cure in W/Wv.衰老与造血作用。II. 年轻和老年小鼠骨髓细胞治愈W/Wv小鼠并维持治愈状态的能力。
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Characterization of spleen colonies derived from mice with mutations at the W locus.
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B lymphocyte precursors in embryonic and adult W anemic mice.胚胎期和成年期患贫血症小鼠的B淋巴细胞前体。
J Immunol. 1984 Jun;132(6):2724-9.
10
Colony formation by bone marrow cells after incubation with neuraminidase. II. Sensitivity of erythroid progenitor cells for burst promoting activity and erythropoietin and restoration of reduced spleen colony formation in mice pretreated with desialated erythrocyte membrane fragments.用神经氨酸酶孵育后骨髓细胞的集落形成。II. 红系祖细胞对爆式促进活性和促红细胞生成素的敏感性以及用去唾液酸化红细胞膜片段预处理的小鼠脾脏集落形成减少的恢复情况。
Exp Hematol. 1981 Feb;9(2):156-67.

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