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Tissue-engineered vascular grafts form neovessels that arise from regeneration of the adjacent blood vessel

机译:组织工程化的血管移植物形成新血管该新血管由邻近血管的再生产生

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摘要

We developed a tissue-engineered vascular graft composed of biodegradable scaffold seeded with autologous bone marrow-derived mononuclear cells (BMMCs) that is currently in clinical trial and developed analogous mouse models to study mechanisms of neovessel formation. We previously reported that seeded human BMMCs were rapidly lost after implantation into immunodeficient mice as host macrophages invaded the graft. As a consequence, the resulting neovessel was entirely of host cell origin. Here, we investigate the source of neotissue cells in syngeneic BMMC-seeded grafts, implanted into immunocompetent mouse recipients. We again find that seeded BMMCs are lost, declining to 0.02% at 14 d, concomitant with host macrophage invasion. In addition, we demonstrate using sex-mismatched chimeric hosts that bone marrow is not a significant source of endothelial or smooth muscle cells that comprise the neovessel. Furthermore, using composite grafts formed from seeded scaffold anastomosed to sex-mismatched natural vessel segments, we demonstrate that the adjacent vessel wall is the principal source of these endothelial and smooth muscle cells, forming 93% of proximal neotissue. These findings have important implications regarding fundamental mechanisms underlying neotissue formation; in this setting, the tissue-engineered construct functions by mobilizing the body's innate healing capabilities to “regenerate” neotissue from preexisting committed tissue cells.—Hibino, N., Villalona, G., Pietris, N., Duncan, D. R., Schoffner, A., Roh, J. D., Yi, T., Dobrucki, L. W., Mejias, D., Sawh-Martinez, R., Harrington, J. K., Sinusas, A., Krause, D. S., Kyriakides, T., Saltzman, W. M., Pober, J. S., Shin'oka, T., Breuer, C. K. Tissue-engineered vascular grafts form neovessels that arise from regeneration of the adjacent blood vessel.
机译:我们开发了一种组织工程化的血管移植物,该移植物由可生物降解的支架组成,该支架植入了自体骨髓来源的单核细胞(BMMC),目前正在临床试验中,并开发了类似的小鼠模型来研究新血管形成的机制。我们先前曾报道过,由于宿主巨噬细胞侵入移植物,植入人免疫缺陷小鼠后,播种的人BMMC迅速丢失。结果,所得的新血管完全来自宿主细胞。在这里,我们调查同种BMMC播种的移植物中的新组织细胞的来源,这些移植物被植入具有免疫能力的小鼠受体中。我们再次发现种子BMMC丢失,在14天下降至0.02%,并伴随宿主巨噬细胞入侵。此外,我们证明了使用性别不匹配的嵌合宿主,骨髓不是构成新生血管的内皮或平滑肌细胞的重要来源。此外,使用由植入的支架吻合到性别不匹配的天然血管片段的复合移植物,我们证明相邻的血管壁是这些内皮细胞和平滑肌细胞的主要来源,占近端新组织的93%。这些发现对新组织形成的基本机制具有重要意义。在这种情况下,组织工程化的构建体通过动员身体的先天治愈能力从先前存在的定型组织细胞中“再生”新组织而发挥作用。 A.,Roh,JD,Yi,T.,Dobrucki,LW,Mejias,D.,Sawh-Martinez,R.,Harrington,JK,Sinusas,A.,Krause,DS,Kyriakides,T.,Saltzman,WM, Pober,JS,Shin'oka,T.,Breuer,CK组织工程化的血管移植物形成新血管,这些血管是由邻近血管的再生产生的。

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