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小鼠肝细胞系促进干细胞前体来源的自然杀伤细胞的扩增和分化。

Murine hepatocyte cell lines promote expansion and differentiation of NK cells from stem cell precursors.

作者信息

Bordoni Veronica, Alonzi Tonino, Agrati Chiara, Poccia Fabrizio, Borsellino Giovanna, Mancino Giorgio, Fimia Gian Maria, Piacentini Mauro, Fantoni Antonio, Tripodi Marco

机构信息

National Institute for Infectious Diseases L. Spallanzani, IRCCS, Rome, Italy.

出版信息

Hepatology. 2004 Jun;39(6):1508-16. doi: 10.1002/hep.20234.

Abstract

While fetal liver is a major hematopoietic organ, normal adult liver provides a suitable microenvironment for a variety of immune cells and, in several pathological conditions, may become a site of extramedullary hematopoiesis. The direct influence of hepatocytes on hematopoietic cell differentiation is poorly understood. We have previously reported that the Met murine hepatocyte (MMH) untransformed hepatocytic lines retain several morphological and functional features of hepatocytes in vivo and are able to support the survival, self-renewal, and differentiation of hematopoietic precursors in a cell-cell contact system. Here we report the effects of soluble factors released by MMH lines on bone marrow-derived cells. Lymphohematopoietic cells were cultured in two different cell contact-free systems: transwell inserts on MMH feeder layers, and MMH conditioned medium (MMH-CM). Both culture systems were able to promote a substantial expansion of bone marrow-derived cells and their differentiation to natural killer (NK) cells that express the NK1.1 and U5A2-13 markers. Purified hematopoietic stem cells (Sca-1+Lin-), either plated as a bulk population or as single cells, were also able to differentiate into NK cells, when cultured in MMH-CM; thus, soluble factors secreted by MMH lines promote the expansion and differentiation of NK precursor cells. MMH-CM-derived NK cells are functionally active; stimulation by interleukin (IL)-12 together with IL-18 was required to induce interferon-gamma (IFNgamma) expression and to enhance their cytotoxic activity. In conclusion, our findings may imply a direct role of hepatocytes in NK cell development, and the system we have used may provide a tool for studying the molecular mechanisms of NK cell differentiation.

摘要

虽然胎儿肝脏是主要的造血器官,但正常成人肝脏为多种免疫细胞提供了适宜的微环境,并且在几种病理状态下,可能成为髓外造血的场所。肝细胞对造血细胞分化的直接影响尚不清楚。我们之前报道过,Met小鼠肝细胞(MMH)未转化的肝细胞系保留了体内肝细胞的一些形态和功能特征,并且能够在细胞 - 细胞接触系统中支持造血前体细胞的存活、自我更新和分化。在此我们报道MMH系释放的可溶性因子对骨髓来源细胞的影响。淋巴细胞造血细胞在两种不同的无细胞接触系统中培养:MMH饲养层上的Transwell小室,以及MMH条件培养基(MMH - CM)。两种培养系统都能够促进骨髓来源细胞的大量扩增及其向表达NK1.1和U5A2 - 13标志物的自然杀伤(NK)细胞的分化。纯化的造血干细胞(Sca - 1 + Lin -),无论是作为群体接种还是单细胞接种,在MMH - CM中培养时也能够分化为NK细胞;因此,MMH系分泌的可溶性因子促进NK前体细胞的扩增和分化。MMH - CM来源的NK细胞具有功能活性;需要白细胞介素(IL) - 12与IL - 18共同刺激才能诱导干扰素 - γ(IFNγ)表达并增强其细胞毒性活性。总之,我们的发现可能意味着肝细胞在NK细胞发育中具有直接作用,并且我们所使用的系统可能为研究NK细胞分化的分子机制提供一种工具。

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