Nishino T, Hisha H, Nishino N, Adachi M, Ikehara S
Cellular Technology Institute, Otsuka Pharmaceutical Co, Ltd, Tokushima, Japan.
Blood. 1995 Jun 1;85(11):3093-100.
Hepatocyte growth factor (HGF) was originally isolated as a mitogen for adult hepatocytes, but this cytokine is now regarded as a multi-functional factor. In the present study, we show that the mouse liver in the middle and/or late stage of the fetal life expresses both HGF and c-met (its receptor) messages. HGF and c-met mRNA are coexpressed not only in the adherent layers of fetal liver long-term cultures (FL-LTCs) and adult bone marrow long-term cultures (BM-LTCs), but also in the stromal cell lines MS-5 and PA-6. Addition of human HGF (2 and 20 ng/mL) to the LTCs enhances (1) nonadherent cell counts (ninefold in FL-LTCs and sixfold in BM-LTCs), (2) nonadherent colony-forming unit-in culture (CFU-C) counts (eightfold in FL-LTCs and fivefold in BM-LTC), and (3) cobblestone colony counts. However, HGF slightly inhibits the proliferation of stromal cells. No direct effect of HGF on freshly isolated BM and/or FL cells is found in the CFU-C assay. However, an approximately 1.5-fold synergistic increase in CFU-C counts is noted when the BM or FL cells are cocultured with HGF in the presence of interleukin-3. These findings strongly suggest that HGF plays a crucial role as a hematopoietic regulator in the proliferation and differentiation of hematopoietic progenitors.
肝细胞生长因子(HGF)最初是作为成年肝细胞的促有丝分裂原被分离出来的,但这种细胞因子现在被认为是一种多功能因子。在本研究中,我们发现小鼠胎儿期中期和/或后期的肝脏表达HGF和c-met(其受体)信息。HGF和c-met mRNA不仅在胎儿肝脏长期培养物(FL-LTCs)和成年骨髓长期培养物(BM-LTCs)的贴壁层中共同表达,而且在基质细胞系MS-5和PA-6中也共同表达。向长期培养物中添加人HGF(2和20 ng/mL)可增强:(1)非贴壁细胞计数(FL-LTCs中增加9倍,BM-LTCs中增加6倍);(2)非贴壁培养集落形成单位(CFU-C)计数(FL-LTCs中增加8倍,BM-LTC中增加5倍);以及(3)鹅卵石样集落计数。然而,HGF会轻微抑制基质细胞的增殖。在CFU-C试验中未发现HGF对新鲜分离的骨髓和/或胎儿肝脏细胞有直接作用。然而,当骨髓或胎儿肝脏细胞在白细胞介素-3存在的情况下与HGF共培养时,CFU-C计数会有大约1.5倍的协同增加。这些发现有力地表明,HGF在造血祖细胞的增殖和分化中作为一种造血调节因子发挥着关键作用。
