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处于红细胞生成刺激和抑制状态下的小鼠中的红细胞生成前体细胞。

Erythropoietic precursors in mice under erythropoietic stimulation and suppression.

作者信息

Hara H, Ogawa M

出版信息

Exp Hematol. 1977 Mar;5(2):141-8.

PMID:844518
Abstract

Using a methylcellulose clonal cell culture technique, we examined serial changes in erythropoietic precursors in the femur, spleen, and blood of mice prepared with bleeding, erythropoietin injections, or hypertransfusion with packed red blood cells. Significant changes were observed for all hemopoietic organs in the number of erythropoietic burst-forming units (BFU-E) and erythrocytic colony-forming units (CFU-E). In mice prepared with bleeding or erythropoietin injections, the serial changes of BFU-E and CFU-E were similar to but less striking than those seen in mice with phenylhydrazine-induced anemia. The transient decline in the femoral BFU-E coincided with the temporary increase in the splenic and blood BFU-E. A more pronounced increase in CFU-E was noted in the femur and spleen of these mice. In hypertransfused mice, the direction of the changers in the erythropoietic precursors was opposite. While femoral BFU-E increased mildly, a significant drop was noted in the splenic and blood BFU-E. Both femoral and splenic CFU-E declined and remained low while erythrocytosis presisted. Next, we examined the proliferative state of the erythropoietic precursors in the marrow and spleen using short-term incubation with high specific tritiated thymidine. In the marrow and spleen of normal mice, the BFU-E and CFU-E in the DNA synthetic phase was about 36 and 74%, respectively. Neither induction of anemia with phenylhydrazine hydrochloride nor polycythemia with hypertransfusion caused changes in the proliferative state of the precursors. These results indicate that the serial changes in the number of BFU-E represent migration of BFU-E from marrow to spleen rather than BFU-E proliferation. Marrow CFU-E increased in anemic mice and decreased in polycythemic mice without changes in their proliferative state. It is possible that the target of erythropoietic stimulation in mice may be cells at maturational stages intermediate between BFU-E and CFU-E.

摘要

我们采用甲基纤维素克隆细胞培养技术,研究了通过放血、注射促红细胞生成素或输注浓缩红细胞制备的小鼠股骨、脾脏和血液中红细胞生成前体细胞的系列变化。在所有造血器官中,促红细胞生成爆式集落形成单位(BFU-E)和红细胞集落形成单位(CFU-E)的数量均出现了显著变化。在放血或注射促红细胞生成素制备的小鼠中,BFU-E和CFU-E的系列变化与苯肼诱导贫血小鼠相似,但程度较轻。股骨中BFU-E的短暂下降与脾脏和血液中BFU-E的暂时增加同时出现。这些小鼠的股骨和脾脏中CFU-E有更明显的增加。在输注浓缩红细胞的小鼠中,红细胞生成前体细胞变化的方向相反。股骨中BFU-E轻度增加,而脾脏和血液中BFU-E显著下降。在红细胞增多症持续期间,股骨和脾脏中的CFU-E均下降并维持在低水平。接下来,我们通过用高比活度的氚标记胸腺嘧啶进行短期孵育,研究了骨髓和脾脏中红细胞生成前体细胞的增殖状态。在正常小鼠的骨髓和脾脏中,处于DNA合成期的BFU-E和CFU-E分别约为36%和74%。盐酸苯肼诱导贫血或输注浓缩红细胞导致红细胞增多均未引起前体细胞增殖状态的改变。这些结果表明,BFU-E数量的系列变化代表BFU-E从骨髓向脾脏的迁移,而非BFU-E的增殖。贫血小鼠的骨髓CFU-E增加,红细胞增多小鼠的骨髓CFU-E减少,但其增殖状态未发生变化。小鼠红细胞生成刺激的靶点可能是处于BFU-E和CFU-E之间成熟阶段的细胞。

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