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采用胰岛β细胞计数而非胰岛β细胞质量来评估和定位结扎胰管后小鼠胰岛β细胞群体的生长情况。

Beta cell count instead of beta cell mass to assess and localize growth in beta cell population following pancreatic duct ligation in mice.

机构信息

Diabetes Research Center, Brussels Free University-VUB, and Center for Beta Cell Therapy in Diabetes, Brussels, Belgium.

出版信息

PLoS One. 2012;7(8):e43959. doi: 10.1371/journal.pone.0043959. Epub 2012 Aug 30.

DOI:10.1371/journal.pone.0043959
PMID:22952825
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3431350/
Abstract

BACKGROUND

Pancreatic-tail duct ligation (PDL) in adult rodents has been reported to induce beta cell generation and increase beta cell mass but increases in beta cell number have not been demonstrated. This study examines whether PDL increases beta cell number and whether this is caused by neogenesis of small clusters and/or their growth to larger aggregates.

METHODOLOGY

Total beta cell number and its distribution over small (<50 µm), medium, large (>100 µm) clusters was determined in pancreatic tails of 10-week-old mice, 2 weeks after PDL or sham.

PRINCIPAL FINDINGS

PDL increased total beta cell mass but not total beta cell number. It induced neogenesis of small beta cell clusters (2.2-fold higher number) which contained a higher percent proliferating beta cells (1.9% Ki67+cells) than sham tails (<0.2%); their higher beta cell number represented <5% of total beta cell number and was associated with a similar increase in alpha cell number. It is unknown whether the regenerative process is causally related to the inflammatory infiltration in PDL-tails. Human pancreases with inflammatory infiltration also exhibited activation of proliferation in small beta cell clusters.

CONCLUSIONS/SIGNIFICANCE: The PDL model illustrates the advantage of direct beta cell counts over beta cell mass measurements when assessing and localizing beta cell regeneration in the pancreas. It demonstrates the ability of the adult mouse pancreas for neogenesis of small beta cell clusters with activated beta cell proliferation. Further studies should investigate conditions under which neoformed small beta cell clusters grow to larger aggregates and hence to higher total beta cell numbers.

摘要

背景

已有研究报道成年啮齿动物的胰尾结扎(PDL)可诱导β细胞生成并增加β细胞质量,但β细胞数量的增加尚未得到证实。本研究旨在探讨 PDL 是否会增加β细胞数量,以及这种增加是否是由小簇的新生和/或其生长为更大的聚集物引起的。

方法

在 PDL 或假手术后 2 周,测定 10 周龄小鼠胰尾中小(<50 µm)、中、大(>100 µm)簇的总β细胞数量及其分布。

主要发现

PDL 增加了总β细胞质量,但不增加总β细胞数量。它诱导了小β细胞簇的新生(数量增加 2.2 倍),其中含有更高比例的增殖β细胞(1.9%的 Ki67+细胞),高于 sham 尾巴(<0.2%);它们更高的β细胞数量仅占总β细胞数量的<5%,并与α细胞数量的相似增加相关。尚不清楚再生过程是否与 PDL 尾巴中的炎症浸润有关。伴有炎症浸润的人类胰腺也表现出小β细胞簇中增殖的激活。

结论/意义:PDL 模型说明了在评估和定位胰腺中β细胞再生时,直接进行β细胞计数优于β细胞质量测量的优势。它证明了成年小鼠胰腺具有新生小β细胞簇的能力,同时激活β细胞增殖。进一步的研究应探讨新形成的小β细胞簇生长为更大聚集物从而增加总β细胞数量的条件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1e7/3431350/8b39d0b9401b/pone.0043959.g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1e7/3431350/755fcae52ec9/pone.0043959.g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1e7/3431350/8b39d0b9401b/pone.0043959.g002.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1e7/3431350/755fcae52ec9/pone.0043959.g001.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e1e7/3431350/8b39d0b9401b/pone.0043959.g002.jpg

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