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神经内分泌激素的免疫和血液学效应。对DW/J侏儒小鼠的研究。

Immunologic and hematologic effects of neuroendocrine hormones. Studies on DW/J dwarf mice.

作者信息

Murphy W J, Durum S K, Anver M R, Longo D L

机构信息

Division of Cancer Treatment, Program Resources, Inc./DynCorp, National Cancer Institute-Frederick Cancer Research and Development Center, Frederick, MD 21702-1201.

出版信息

J Immunol. 1992 Jun 15;148(12):3799-805.

PMID:1602129
Abstract

DW/J dwarf mice lack acidophilic anterior pituitary cells and are deficient in growth hormone and other neuroendocrine mediators. These mice were examined to determine the effects of these deficiencies on hematopoietic and immune system development. Previous studies have suggested that these mice had immunologic defects primarily involving T cell development. However, we have found that these mice exhibit decreased peripheral blood cell counts affecting all lineages (erythrocytic, leukocytic, and platelets). Examination of lymphoid tissues of dwarf mice indicated that their spleens were hypoplastic. Treatment of these mice with recombinant human growth hormone resulted in a significant improvement of peripheral blood counts and spleen cell number. Analysis of the bone marrow indicated a profound deficiency of B cell progenitors in the dwarf mice. However, in untreated dwarf mice, mature B cells and T cells were observed in the spleens. Although treatment with recombinant human growth hormone could correct the hematopoietic deficiencies in these mice, it did not restore the B cell progenitor populations, suggesting that an absence of growth hormone is not solely responsible for this deficiency. Thus, these mice display significant myeloid and lymphoid deficiencies that have been previously undetected.

摘要

DW/J 侏儒小鼠缺乏嗜酸性垂体前叶细胞,生长激素及其他神经内分泌介质分泌不足。对这些小鼠进行检查,以确定这些缺陷对造血和免疫系统发育的影响。先前的研究表明,这些小鼠存在主要涉及 T 细胞发育的免疫缺陷。然而,我们发现这些小鼠外周血细胞计数下降,影响所有谱系(红细胞、白细胞和血小板)。对侏儒小鼠淋巴组织的检查表明,它们的脾脏发育不全。用重组人生长激素治疗这些小鼠可显著改善外周血细胞计数和脾细胞数量。对骨髓的分析表明,侏儒小鼠的 B 细胞祖细胞严重缺乏。然而,在未经治疗的侏儒小鼠脾脏中观察到了成熟的 B 细胞和 T 细胞。虽然用重组人生长激素治疗可以纠正这些小鼠的造血缺陷,但它并未恢复 B 细胞祖细胞群体,这表明生长激素的缺乏并非造成这种缺陷的唯一原因。因此,这些小鼠表现出先前未被发现的显著的髓系和淋巴系缺陷。

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