首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Three human elastase-like genes coordinately expressed in the myelomonocyte lineage are organized as a single genetic locus on 19pter.
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Three human elastase-like genes coordinately expressed in the myelomonocyte lineage are organized as a single genetic locus on 19pter.

机译:在19pter上三个在骨髓单细胞谱系中协调表达的人类弹性蛋白酶样基因被组织为单个遗传基因座。

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摘要

The human neutrophil and monocyte-derived serine protease homologues neutrophil elastase (NE), proteinase 3 (PR3), and azurocidin (AZU) are involved in a variety of immune defense reactions. NE and PR3 assist in the destruction of phagocytosed microorganisms, cleave the important connective-tissue protein elastin, and generate chemotactic activities by forming alpha 1-proteinase inhibitor complexes and elastin peptides. AZU is cytotoxic to certain microorganisms and chemotactic for monocytes. All three proteins are produced and packaged into azurophil granules in large quantities during neutrophil differentiation. We have isolated several cosmid clones each of which contains the functional genes for AZU, PR3, and NE in this order. The PR3 gene is separated by 8 kilobases from the 3' end of the AZU gene and by 3 kilobases from the 5' end of the NE gene. We report a physical map of the gene cluster, its location on chromosome 19pter, and the exon-intron organization of the AZU and PR3 genes. Our fluorescence in situ hybridization studies disprove the previous chromosomal assignment of the human NE gene to 11q14. The five exons of AZU and PR3 are organized like those of NE and other granule-associated serine proteases of hematopoietic cells. NE, PR3, and AZU are coordinately downregulated in the premonocytic cell line U937 during induced terminal differentiation. The cluster-like physical organization of these genes and concerted regulation during hematopoietic differentiation suggests that they are located in a developmentally activated chromatin domain promoting high-level, cell-specific expression in the monocyte-myelocyte lineage.
机译:人嗜中性粒细胞和单核细胞衍生的丝氨酸蛋白酶同源物嗜中性粒细胞弹性蛋白酶(NE),蛋白酶3(PR3)和天青霉素(AZU)参与多种免疫防御反应。 NE和PR3有助于破坏吞噬微生物,裂解重要的结缔组织蛋白弹性蛋白,并通过形成α1-蛋白酶抑制剂复合物和弹性蛋白肽来产生趋化活性。 AZU对某些微生物具有细胞毒性,对单核细胞具有趋化作用。在嗜中性粒细胞分化过程中,所有这三种蛋白质均被大量生产并包装成嗜蓝粒颗粒。我们已经分离了几个粘粒克隆,每个粘粒克隆都包含AZU,PR3和NE的功能基因。 PR3基因与AZU基因的3'末端相距8碱基,与NE基因的5'末端相距3碱基。我们报告了该基因簇的物理图谱,其在19pter染色体上的位置,以及AZU和PR3基因的外显子-内含子组织。我们的荧光原位杂交研究证明了人类NE基因先前对11q14的染色体分配。 AZU和PR3的五个外显子的结构类似于NE和造血细胞的其他颗粒相关丝氨酸蛋白酶。在诱导的终末分化过程中,前单核细胞系U937中的NE,PR3和AZU协同下调。这些基因的簇状物理组织和造血分化过程中的一致调控表明它们位于发育活化的染色质结构域中,可促进单核细胞-骨髓细胞谱系中高水平的细胞特异性表达。

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