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利用透明质酸纳米涂层细胞移植构建1型糖尿病雌性动物模型:改进及对未来方案的思考

Towards the Development of a Female Animal Model of T1DM Using Hyaluronic Acid Nanocoated Cell Transplantation: Refinements and Considerations for Future Protocols.

作者信息

Zamboni Fernanda, Cengiz Ibrahim F, Barbosa Ana M, Castro Antonio G, Reis Rui L, Oliveira Joaquim M, Collins Maurice N

机构信息

Stokes Laboratories, School of Engineering, Bernal Institute, University of Limerick, Limerick V94 T9PX, Ireland.

Health Research Institute, University of Limerick, Limerick V94 T9PX, Ireland.

出版信息

Pharmaceutics. 2021 Nov 13;13(11):1925. doi: 10.3390/pharmaceutics13111925.

Abstract

Female mice (Black 6 strain) (C57BL/6) aged 6 weeks were subject to low dose streptozotocin (STZ) treatment for five consecutive days to mimic type 1 diabetes mellitus (T1DM) with insulitis. At two weeks after STZ injections, evaluation of the elevated glucose levels was used to confirm diabetes. The diabetic mice were then subject to the transplantation of pancreatic β-cells (MIN-6 line). Four groups of mice were studied. The first group was injected with saline-only acting as the placebo surgery control, also known as SHAM group, the second and third groups were injected with MIN-6 single cells and polyethylene glycol-modified dipalmitoyl-glycerol-phosphatidyl ethanolamine (PEG-DPPE) modified MIN-6 single cells (500 µg per 1.10 cells), respectively, while the fourth group was injected with hyaluronic acid (HA)-coated MIN-6 single cells (5 bilayers). At seven- and fourteen-days following transplantation, the mice were euthanised. The renal and pancreatic tissues were then collected and histologically analysed. The induction of diabetes in female mice, through five-consecutive daily STZ injections resulted in inconsistent glycaemic levels. Interestingly, this shows an incomplete diabetes induction in female mice, of which we attribute to sex dimorphism and hormonal interferences. Transplantation failure of free-floating encapsulated cells was unable to decrease blood glucose hyperglycaemia to physiological ranges. The result is attributed to deprived cell-cell interactions, leading to decreased β-cells functionality. Overall, we highlight the necessity of refining T1DM disease models in female subjects when using multiple low-dose STZ injections together with transplantation protocols. Considerations need to be made regarding the different developmental stages of female mice and oestrogen load interfering with pancreatic β-cells susceptibility to STZ. The use of pseudo islets, cell aggregates and spheroids are sought to improve transplantation outcome in comparison to free-floating single cells.

摘要

6周龄雌性小鼠(C57BL/6黑6品系)连续5天接受低剂量链脲佐菌素(STZ)治疗,以模拟伴有胰岛炎的1型糖尿病(T1DM)。在注射STZ两周后,通过评估血糖水平升高来确认糖尿病。然后对糖尿病小鼠进行胰腺β细胞(MIN-6细胞系)移植。研究了四组小鼠。第一组仅注射生理盐水作为假手术对照,也称为假手术组(SHAM组),第二组和第三组分别注射MIN-6单细胞和聚乙二醇修饰的二棕榈酰甘油磷脂酰乙醇胺(PEG-DPPE)修饰的MIN-6单细胞(每1.10个细胞500μg),而第四组注射透明质酸(HA)包被的MIN-6单细胞(5层)。在移植后7天和14天,对小鼠实施安乐死。然后收集肾脏和胰腺组织并进行组织学分析。通过连续5天每日注射STZ诱导雌性小鼠患糖尿病,导致血糖水平不一致。有趣的是,这表明雌性小鼠的糖尿病诱导不完全,我们将其归因于性别二态性和激素干扰。游离包封细胞的移植失败无法将血糖高血糖水平降低到生理范围。结果归因于细胞间相互作用的缺乏,导致β细胞功能下降。总体而言,我们强调在使用多次低剂量STZ注射和移植方案时,完善雌性受试者T1DM疾病模型的必要性。需要考虑雌性小鼠的不同发育阶段以及雌激素负荷对胰腺β细胞对STZ易感性的干扰。与游离单细胞相比,使用伪胰岛、细胞聚集体和球体旨在改善移植结果。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/731e/8621706/a259faaf41d4/pharmaceutics-13-01925-g001.jpg

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