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培养中的血红蛋白转换:存在一种体液因子的证据,该因子可诱导成人及新生儿而非胎儿红系细胞发生转换。

Hemoglobin switching in culture: evidence for a humoral factor that induces switching in adult and neonatal but not fetal erythroid cells.

作者信息

Papayannopoulou T, Kurachi S, Nakamoto B, Zanjani E D, Stamatoyannopoulos G

出版信息

Proc Natl Acad Sci U S A. 1982 Nov;79(21):6579-83. doi: 10.1073/pnas.79.21.6579.

Abstract

An erythropoietic activity that exerts a profound effect on fetal Hb synthesis is present in fetal sheep sera and it attains a peak concentration at the end of the second to the middle of the third trimester of fetal life. The activity consistently inhibits the increased synthesis of fetal Hb in cultures of burst-forming units (BFUes) from normal adults. In cultures of BFUes from homozygous beta+-thalassemias the activity produces a striking decline in gamma chain synthesis, a decline in G gamma/A gamma chain synthesis ratio, and an increase in delta/gamma and alpha/non-alpha ratios--i.e., findings suggesting a genuine gamma-to-beta switch. The activity accelerates Hb F-to-Hb A switching in neonatal BFUe cultures but it has no effect on fetal Hb synthesis in cultures of BFUe obtained from human fetuses. These findings provide direct evidence that (a) humoral factors play a role in the regulation of the switch from fetal to adult Hb formation, and (b) progenitor cells from various stages of ontogeny respond differently to these factors. The results are compatible with the hypothesis that Hb switching during development is mediated through a change in a developmental program which controls the responsiveness of progenitor cells to "switching" activities in their environment.

摘要

胎羊血清中存在一种对胎儿血红蛋白(Hb)合成有深远影响的促红细胞生成活性,该活性在胎儿期第二个月末至第三个月中期达到峰值浓度。这种活性持续抑制正常成年人爆式集落形成单位(BFUe)培养物中胎儿Hb合成的增加。在纯合β⁺地中海贫血患者的BFUe培养物中,该活性使γ链合成显著下降,Gγ/Aγ链合成比值下降,δ/γ和α/非α比值增加——即这些结果提示真正的γ向β转换。该活性加速新生儿BFUe培养物中Hb F向Hb A的转换,但对从人类胎儿获得的BFUe培养物中的胎儿Hb合成没有影响。这些发现提供了直接证据,即(a)体液因子在从胎儿Hb向成人Hb形成的转换调节中起作用,(b)个体发育不同阶段的祖细胞对这些因子的反应不同。这些结果与以下假设相符:发育过程中的Hb转换是通过发育程序的改变介导的,该程序控制祖细胞对其环境中“转换”活性的反应性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a2f1/347171/a1b8345acb8a/pnas00460-0174-a.jpg

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