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模拟微重力对有无支持细胞共培养的新生猪细胞团形态和功能的影响。

Effects of simulated microgravity on the morphology and function of neonatal porcine cell clusters cultured with and without Sertoli cells.

作者信息

Luca G, Calvitti M, Nastruzzi C, Macchiarulo G, Becchetti E, Neri L M, Capitani S, Basta G, Brunetti P, Calafiore R, Cameron D F

机构信息

Department of Internal Medicine and Endocrine and Metabolic Sciences, University of Perugia, Perugia, Italy.

出版信息

Cell Transplant. 2006;15(1):55-65. doi: 10.3727/000000006783982223.

Abstract

Human islet allografts are well known to induce full and sustained remission of hyperglycemia, with complete normalization of key metabolic parameters. Nevertheless, acquiring human islets, even from cadaveric human donor pancreases, remains a significant impediment to successful transplantation therapy for diabetes. To overcome this difficulty, neonatal porcine cell clusters (NPCCs) have been considered for human islet substitutes because they are easily obtained by collagenase digestion of the neonatal piglet pancreas. Currently, the major hurdle in using NPCCs for xenograft is the delay (time lag) in achieving the posttransplant normalization of blood glucose levels in animal diabetic recipients. The present work is the first attempt to evaluate whether incubation of NPCCs in simulated microgravity, in the presence or absence of Sertoli cells (SC), may reduce the maturation time lag of beta-cells by differentiation acceleration in vitro, thereby expediting production, viability, and acquisition of functional competence of pretransplantation beta-cell-enriched islets. Following a 3-day incubation period, NPCCs maintained in conventional culture, NPCCs incubated in simulated microgravity in the HARV biochamber, and NPCCs plus co-incubated SC in simulated microgravity were examined for viability, morphology, and insulin secretion. Results show that NPCCs grown alone in the HARV biochamber are superior in quality, both in terms of viability and functional competence, when compared to other culture pretreatment protocols. This finding strongly suggests that NPCC pretreatment in simulated microgravity may enhance the transplantation success of NPCCs in the diabetic recipient.

摘要

众所周知,人胰岛同种异体移植可诱导高血糖完全且持续缓解,关键代谢参数完全恢复正常。然而,获取人胰岛,即使是从尸体供体胰腺获取,仍然是糖尿病成功移植治疗的重大障碍。为克服这一困难,新生猪细胞团(NPCCs)已被考虑用作人胰岛替代物,因为它们可通过对新生仔猪胰腺进行胶原酶消化轻易获得。目前,将NPCCs用于异种移植的主要障碍是动物糖尿病受体移植后血糖水平恢复正常存在延迟(时间滞后)。本研究首次尝试评估在有或没有支持细胞(SC)存在的情况下,将NPCCs置于模拟微重力环境中培养,是否可通过体外加速分化来减少β细胞的成熟时间滞后,从而加快移植前富含β细胞的胰岛的产生、活力及功能能力的获得。在3天的培养期后,对常规培养的NPCCs、在HARV生物舱模拟微重力环境中培养的NPCCs以及在模拟微重力环境中与SC共同培养的NPCCs进行活力、形态及胰岛素分泌检测。结果表明,与其他培养预处理方案相比,单独在HARV生物舱中培养的NPCCs在活力和功能能力方面质量更优。这一发现有力地表明,模拟微重力环境下的NPCCs预处理可能会提高NPCCs在糖尿病受体中的移植成功率。

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