Functional analysis of a conditionally transformed pancreatic β-cell line

被引:78
作者
Fleischer, N
Chen, C
Surana, M
Leiser, M
Rossetti, L
Pralong, W
Efrat, S
机构
[1] Yeshiva Univ Albert Einstein Coll Med, Ctr Diabet Res & Training, Dept Med, Bronx, NY 10461 USA
[2] Yeshiva Univ Albert Einstein Coll Med, Ctr Diabet Res & Training, Dept Mol Pharmacol, Bronx, NY 10461 USA
[3] Modex Therapeut, Lausanne, Switzerland
[4] Tel Aviv Univ, Sackler Sch Med, Dept Human Genet, Tel Aviv, Israel
来源
DIABETES | 1998年 / 47卷 / 09期
关键词
D O I
10.2337/diabetes.47.9.1419
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Development of beta-cell lines for cell therapy of diabetes is hindered by functional deviations of the replicating cells from the normal beta-cell phenotype. In a recently developed cell line, denoted beta TC-tet, derived from transgenic mice expressing the SV40 T antigen (Tag) under control of the tetracycline (Tc) gene regulatory system, growth arrest can be induced by shutting off Tag expression in the presence of Tc. Here, we compared differentiated cell functions in dividing and growth-arrested beta TC-tet cells, both in culture and in vivo. Proliferating cells stably maintained normal glucose responsiveness for >60 passages in culture. Growth-arrested cells survived for months in culture and in vivo and maintained normal insulin production and secretion. After growth arrest, the cells gradually increased their insulin content three- to fourfold. This occurred without significant changes in insulin biosynthetic rates. At high passage numbers, proliferating beta TC-tet cells exhibited an abnormal increase in hexokinase expression. However, the upregulation of hexokinase was reversible upon growth arrest. Growth-arrested cells transplanted intraperitoneally into syngeneic recipients responded to hyperglycemia by a significant increase in insulin secretion. These findings demonstrate that transformed beta-cells maintain function during long periods of growth arrest, suggesting that conditional transformation of beta-cells may be a useful approach for developing cell therapy for diabetes.
引用
收藏
页码:1419 / 1425
页数:7
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