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与成人骨髓相比,胎儿肝脏进行长期再增殖的效率几乎是短期再增殖的五倍。

Relative to adult marrow, fetal liver repopulates nearly five times more effectively long-term than short-term.

作者信息

Harrison D E, Zhong R K, Jordan C T, Lemischka I R, Astle C M

机构信息

Jackson Laboratory, Bar Harbor, ME 04609-0800, USA.

出版信息

Exp Hematol. 1997 Apr;25(4):293-7.

PMID:9131003
Abstract

Multilineage precursor cells from 14-day B6 (C57B1/6J) mouse fetal liver and adult bone marrow that repopulate both the lymphoid and myeloid systems were compared by competitive repopulation. Cells were assayed in normally functioning populations, and enrichment, tissue culture, and induced marking were avoided since these manipulations might affect cell function. Fetal or adult donor cells were mixed with marked adult competitor cells and transplanted into irradiated recipients whose blood was tested at short (25-33-day) or long (105-245-day) time periods after transplantation. Proportions of lymphocytes, granulocytes, and platelets descended from donor precursors were measured by GPI (glucosephosphate isomerase) isozyme genetic markers in congenic mice, and represent the repopulating abilities of these precursors relative to the standard competitor. For short-term repopulation 25-33 days after transplantation, fetal and adult donor cells were similar; in three studies, fetal liver contributed 0.8, 1.1, and 1.4 times as much as adult marrow per 10(5) cells transplanted. However, when long-term (105-245-day) repopulation was tested in the same recipients, fetal liver contributed 3.5, 5.0, and 7.1 times as much as adult marrow. Ratios of long-term/short-term repopulating abilities in fetal liver relative to standard adult marrow competitors were 2.5, 8.9, and 4.7, while in marrow controls, these ratios remained approximately one (1.14 and 0.80). Thus, 14-day fetal liver contains several times more long-term repopulating cells relative to short-term repopulating cells than does adult marrow. Ratios of long-term/short-term fetal cells were unchanged by precursor enrichment. The AA4.1+, Ly-6A/E+, lineage low fraction had a ratio of 4.4, although it repopulated 276 times better than unenriched fetal cells whose ratio was 4.7. There are two hypotheses that explain these data most simply: 1) There may be only a single multilineage precursor, but after transplantation cells seed in different microenvironments that support either long-term or short-term function. 2) Conversely, the difference may be at the stem cell level rather than the microenvironmental level, so that there are tow types of stem cells with multilineage differentiating ability, but only one functions over the long-term. The current report defines new conditions required by each hypothesis. If functional life spans are defined by seeding sites, as in hypothesis 1, fetal cells seed much higher proportions of long-term sites than adult cells. If different types of stem cells function short-term and long-term, as in hypothesis 2, they are not distinguished by markers allowing a 276-fold enrichment to 1367 times the repopulating ability of fresh marrow.

摘要

通过竞争性再增殖实验比较了来自14天龄B6(C57B1/6J)小鼠胎肝和成年骨髓的多谱系前体细胞,这些细胞能够重新填充淋巴系统和髓系系统。细胞在正常功能的群体中进行检测,避免进行富集、组织培养和诱导标记,因为这些操作可能会影响细胞功能。将胎儿或成年供体细胞与标记的成年竞争细胞混合,然后移植到经辐射的受体中,并在移植后的短时间(25 - 33天)或长时间(105 - 245天)对受体血液进行检测。通过同基因小鼠中的GPI(葡萄糖磷酸异构酶)同工酶遗传标记来测量源自供体前体细胞的淋巴细胞、粒细胞和血小板的比例,这些比例代表了这些前体细胞相对于标准竞争细胞的再增殖能力。对于移植后25 - 33天的短期再增殖,胎儿和成年供体细胞相似;在三项研究中,每移植10⁵个细胞,胎肝的贡献是成年骨髓的0.8倍、1.1倍和1.4倍。然而,当在相同受体中检测长期(105 - 245天)再增殖时,胎肝的贡献是成年骨髓的3.5倍、5.0倍和7.1倍。相对于标准成年骨髓竞争细胞,胎肝中长期/短期再增殖能力的比率分别为2.5、8.9和4.7,而在骨髓对照中,这些比率约为1(1.14和0.80)。因此,相对于短期再增殖细胞,14天龄的胎肝中含有的长期再增殖细胞数量是成年骨髓的数倍。前体细胞富集并未改变胎儿细胞长期/短期的比率。AA4.1⁺、Ly - 6A/E⁺、谱系低表达部分的比率为4.4,尽管它的再增殖能力比未富集的胎儿细胞(比率为4.7)高276倍。有两种假设能最简洁地解释这些数据:1)可能只有单一的多谱系前体细胞,但移植后细胞在支持长期或短期功能的不同微环境中定植。2)相反,差异可能存在于干细胞水平而非微环境水平,即存在两种具有多谱系分化能力的干细胞,但只有一种能长期发挥作用。本报告确定了每种假设所需的新条件。如果功能寿命由定植位点定义,如假设1所述,胎儿细胞在长期位点的定植比例比成年细胞高得多。如果不同类型的干细胞分别发挥短期和长期功能,如假设2所述,它们无法通过标记区分,标记允许富集276倍至新鲜骨髓再增殖能力的1367倍。

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