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I. Embryonal vasculature formation recapitulated in transgenic mammary tumor spheroids implanted pseudo-orthotopicly into mouse dorsal skin fold: the organoblasts concept

机译:一在假正位植入小鼠背部皮肤褶皱的转基因乳腺肿瘤球体中概述了胚胎脉管系统的形成:成胚细胞概念

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摘要

Inadequate understanding of cancer biology is a problem. This work focused on cellular mechanisms of tumor vascularization. According to earlier studies, the tumor vasculature derives from host endothelial cells (angiogenesis) or their precursors of bone marrow origin circulating in the blood (neo-vasculogenesis) unlike in embryos. In this study, we observed the neo-vasculature form in multiple ways from local precursor cells. Recapitulation of primitive as well as advanced embryonal stages of vasculature formation followed co-implantation of avascular ( in vitro cultured) N202 breast tumor spheroids and homologous tissue grafts into mouse dorsal skin chambers. Ultrastructural and immunocytochemical analysis of tissue sections exposed the interactions between the tumor and the graft tissue stem cells. It revealed details of vasculature morphogenesis not seen before in either tumors or embryos. A gradual increase in complexity of the vascular morphogenesis at the tumor site reflected a range of steps in ontogenic evolution of the differentiating cells. Malignant- and surgical injury repair-related tissue growth prompted local cells to initiate extramedullar erythropoiesis and vascular patterning. The new findings included: interdependence between the extramedullar hematopoiesis and assembly of new vessels (both from the locally differentiating precursors); nucleo-cytoplasmic conversion (karyolysis) as the mechanism of erythroblast enucleation; the role of megakaryocytes and platelets in vascular pattern formation before emergence of endothelial cells; lineage relationships between hematopoietic and endothelial cells; the role of extracellular calmyrin in tissue morphogenesis; and calmyrite, a new ultrastructural entity associated with anaerobic energy metabolism. The central role of the extramedullar erythropoiesis in the formation of new vasculature (blood and vessels) emerged here as part of the tissue building process including the lymphatic system and nerves, and suggests a cellular mechanism for instigating variable properties of endothelial surfaces in different organs. Those findings are consistent with the organoblasts concept, previously discussed in a study on childhood tumors, and have implications for tissue definition.
机译:对癌症生物学的了解不足是一个问题。这项工作集中于肿瘤血管形成的细胞机制。根据较早的研究,与胚胎不同,肿瘤脉管系统源自血液中循环的宿主内皮细胞(血管生成)或其骨髓起源的前体(新血管生成)。在这项研究中,我们从本地前体细胞以多种方式观察了新脉管系统形式。在将无血管的(体外培养的)N202乳腺肿瘤球体和同源组织移植物共同植入小鼠背部皮肤腔室之后,概述了脉管系统形成的原始以及晚期胚胎阶段。组织切片的超微结构和免疫细胞化学分析揭示了肿瘤与移植组织干细胞之间的相互作用。它揭示了在肿瘤或胚胎中从未见过的脉管形态发生的细节。在肿瘤部位的血管形态发生的复杂性的逐渐增加反映了分化细胞的本体进化的一系列步骤。恶性和外科损伤修复相关的组织生长促使局部细胞启动髓外红细胞生成和血管形成。新发现包括:髓外造血与新血管组装之间的相互依赖性(均来自局部分化的前体);核细胞质转化(核解)是成红细胞去核的机制;巨核细胞和血小板在内皮细胞出现之前在血管模式形成中的作用;造血和内皮细胞之间的谱系关系;细胞外钙调蛋白在组织形态发生中的作用;钙锰矿,一种与厌氧能量代谢有关的新的超微结构实体。髓外红细胞生成在新的脉管系统(血液和血管)形成中的核心作用是作为包括淋巴系统和神经在内的组织构建过程的一部分出现的,并暗示了一种促进不同器官中内皮表面可变特性的细胞机制。这些发现与先前在有关儿童肿瘤的研究中讨论的成细胞细胞概念相符,并且对组织的定义有影响。

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