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血细胞激肽是一种调节B淋巴细胞生成的造血特异性速激肽。

Hemokinin is a hematopoietic-specific tachykinin that regulates B lymphopoiesis.

作者信息

Zhang Y, Lu L, Furlonger C, Wu G E, Paige C J

机构信息

Ontario Cancer Institute, Princess Margaret Hospital, University Health Network and Department of Medical Biophysics and Immunology, University of Toronto, Toronto, Ontario, Canada, M5G 2M9.

出版信息

Nat Immunol. 2000 Nov;1(5):392-7. doi: 10.1038/80826.

Abstract

We report here the molecular cloning of a newly identified preprotachykinin gene, Pptc, which specifies the sequence for a new preprotachykinin protein and bioactive peptide designated hemokinin 1 (HK-1). PPT-C mRNA was detected primarily in hematopoietic cells in contrast to the previously described Ppta and Pptb genes, which are predominantly expressed in neuronal tissues. HK-1 has several biological activities that are similar to the most studied tachykinin, substance P, such as induction of plasma extravasation and mast cell degranulation. However, HK-1 also has properties that are indicative of a critical role in mouse B cell development. HK-1 stimulated the proliferation of interleukin 7-expanded B cell precursors, whereas substance P had no effect. HK-1, but not substance P, promoted the survival of freshly isolated bone marrow B lineage cells or cultured, lipopolysaccharide-stimulated pre-B cells. N-acetyl-L-trytophan-3,5-bistrifluromethyl benzyl ester, a tachykinin receptor antagonist, increased apoptosis of these cells and in vivo administration of this antagonist led to specific reductions of the B220lowCD43 population (the pre-B cell compartment) in the bone marrow and the IgMhighIgDlow population (the newly generated B cells) in the spleen. Thus, HK-1 may be an autocrine factor that is important for the survival of B cell precursors at a critical phase of development.

摘要

我们在此报告一个新鉴定的前速激肽原基因Pptc的分子克隆,该基因确定了一种新的前速激肽原蛋白和名为血激肽1(HK-1)的生物活性肽的序列。与先前描述的主要在神经组织中表达的Ppta和Pptb基因不同,PPT-C mRNA主要在造血细胞中检测到。HK-1具有几种与研究最多的速激肽P物质相似的生物学活性,如诱导血浆外渗和肥大细胞脱颗粒。然而,HK-1还具有在小鼠B细胞发育中起关键作用的特性。HK-1刺激白细胞介素7扩增的B细胞前体的增殖,而P物质则无作用。HK-1而非P物质促进新鲜分离的骨髓B系细胞或培养的、脂多糖刺激的前B细胞的存活。速激肽受体拮抗剂N-乙酰-L-色氨酸-3,5-双三氟甲基苄酯增加了这些细胞的凋亡,并且在体内给予该拮抗剂导致骨髓中B220lowCD43群体(前B细胞区室)和脾脏中IgMhighIgDlow群体(新产生的B细胞)的特异性减少。因此,HK-1可能是一种自分泌因子,对B细胞前体在发育关键阶段的存活很重要。

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