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从成人胰腺组织中分离出的多能祖细胞。

Multipotent progenitor cells isolated from adult human pancreatic tissue.

作者信息

Todorov I, Nair I, Ferreri K, Rawson J, Kuroda A, Pascual M, Omori K, Valiente L, Orr C, Al-Abdullah I, Riggs A, Kandeel F, Mullen Y

机构信息

Southern California Islet Cell Resource Center, Department of Diabetes, Endocrinology and Metabolism, City of Hope National Medical Center, 1500 East Duarte Road, Duarte, CA 91010, USA.

出版信息

Transplant Proc. 2005 Oct;37(8):3420-1. doi: 10.1016/j.transproceed.2005.09.088.

Abstract

The supply of islet cells is a limiting factor for the widespread application of islet transplantation of type-1 diabetes. Islets constitute 1% to 2% of pancreatic tissue, leaving approximately 98% as discard after islet isolation and purification. In this report we present our data on the isolation of multipotent progenitor cells from discarded adult human pancreatic tissue. The collected cells from discarded nonislet fractions, after enzymatic digestion and gradient purification of islets, were dissociated for suspension culture in a serum-free medium. The cell clusters grown to a size of 100 to 150 mum contained cells staining for stage-specific embryonic antigens, but not insulin or C-peptide. To direct cell differentiation toward islets, clusters were recultured in a pancreatic differentiation medium. Insulin and C-peptide-positive cells by immunocytochemistry appeared within a week, reaching over 10% of the cell population. Glucagon and somatostatin-positive cells were also detected. The cell clusters were found to secrete insulin in response to glucose stimulation. Cells from the same clusters also had the capacity for differentiation into neural cells, as documented by staining for neural and glial cell markers when cultured as monolayers in media containing neurotrophic factors. These data suggest that multipotent pancreatic progenitor cells exist within the human pancreatic tissue that is typically discarded during islet isolation procedures. These adult progenitor cells can be successfully differentiated into insulin-producing cells, and thus they have the potential for treatment of type-1 diabetes mellitus.

摘要

胰岛细胞的供应是1型糖尿病胰岛移植广泛应用的一个限制因素。胰岛仅占胰腺组织的1%至2%,在胰岛分离和纯化后,约98%的胰腺组织被废弃。在本报告中,我们展示了从废弃的成人胰腺组织中分离多能祖细胞的数据。在对胰岛进行酶消化和梯度纯化后,从废弃的非胰岛部分收集细胞,将其解离后在无血清培养基中进行悬浮培养。生长到100至150微米大小的细胞团含有阶段特异性胚胎抗原染色的细胞,但不含有胰岛素或C肽。为了引导细胞向胰岛分化,将细胞团在胰腺分化培养基中重新培养。通过免疫细胞化学检测,胰岛素和C肽阳性细胞在一周内出现,占细胞总数的10%以上。还检测到了胰高血糖素和生长抑素阳性细胞。发现细胞团在葡萄糖刺激下分泌胰岛素。当在含有神经营养因子的培养基中单层培养时,来自同一细胞团的细胞也具有分化为神经细胞的能力,这通过神经和神经胶质细胞标志物的染色得以证明。这些数据表明,在胰岛分离过程中通常被废弃的人类胰腺组织中存在多能胰腺祖细胞。这些成年祖细胞可以成功分化为胰岛素产生细胞,因此它们具有治疗1型糖尿病的潜力。

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