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一种新型的 C57BL/6J 小鼠草酸钙珠诱导输尿管纤维化的体内模型。

A novel in vivo model of ureteral fibrosis induced by calcium oxalate beads in C57BL/6J mice.

机构信息

Laboratory of Laboratory Animal Science and Medicine, School of Veterinary Medicine, Kitasato University, Towada, 034-8628, Japan.

Laboratory of Veterinary Pathology, School of Veterinary Medicine, Kitasato University, 35-1 Higashi-23, Towada, 034-8628, Japan.

出版信息

Urolithiasis. 2023 Oct 6;51(1):119. doi: 10.1007/s00240-023-01491-x.

DOI:10.1007/s00240-023-01491-x
PMID:37801093
Abstract

The global incidence of ureteroliths in humans is increasing, particularly posing a problem in developed countries. The most common stone type is calcium oxalate, which is associated with a high recurrence rate. In veterinary medicine, stones are the most common cause of ureteral obstruction in cats, accounting for 72-87% of cases. In cats, stones cause irreversible ureteral damage, necessitating stone treatment as well as ureteral therapy. However, the mechanisms underlying the ureteral damage caused by stones remain unclear. Therefore, this study aimed to create a mouse model suitable for studying the ureteral fibrosis caused by oxalate stones by artificially embedding calcium oxalate in the ureter. Pathological tissue analysis was used to compare normal ureters without ligation and ureters with sham or oxalate bead implantation. The ureters of the sham and oxalate bead groups showed granulation tissue formation, transitional epithelium exfoliation, and densely packed connective tissue in the proprietary and muscle layer regions. Particularly in the oxalate bead group, infiltration of degenerated neutrophils, presence of foreign body giant cells, and hyperplasia of the transitional epithelium were observed. The proportion of fibrosis was higher in the oxalate group than in the sham group. Overall, this mouse model created using oxalate bead implantation has the potential to efficiently induce ureteral obstruction. This mouse model is expected to be used for elucidating the molecular mechanisms of ureteral fibrosis and evaluating therapeutic drugs in future.

摘要

人类输尿管结石的全球发病率正在增加,尤其是在发达国家。最常见的结石类型是草酸钙,其复发率较高。在兽医医学中,结石是猫中最常见的输尿管阻塞原因,占 72-87%的病例。在猫中,结石会导致不可逆转的输尿管损伤,因此需要进行结石治疗和输尿管治疗。然而,结石引起输尿管损伤的机制尚不清楚。因此,本研究旨在通过人工将草酸钙嵌入输尿管来创建一种适合研究草酸结石引起的输尿管纤维化的小鼠模型。通过病理组织分析比较了未结扎的正常输尿管与假手术或草酸珠植入组的输尿管。假手术和草酸珠组的输尿管均出现肉芽组织形成、移行上皮脱落以及固有层和肌肉层区域结缔组织紧密堆积的现象。特别是在草酸珠组中,观察到退化的中性粒细胞浸润、异物巨细胞存在以及移行上皮过度增生。草酸珠组的纤维化比例高于假手术组。总的来说,这种使用草酸珠植入法创建的小鼠模型能够有效地诱导输尿管阻塞。该小鼠模型有望用于阐明输尿管纤维化的分子机制,并在未来评估治疗药物。

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1
A novel in vivo model of ureteral fibrosis induced by calcium oxalate beads in C57BL/6J mice.一种新型的 C57BL/6J 小鼠草酸钙珠诱导输尿管纤维化的体内模型。
Urolithiasis. 2023 Oct 6;51(1):119. doi: 10.1007/s00240-023-01491-x.
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本文引用的文献

1
Ureteral Obstruction Promotes Ureteral Inflammation and Fibrosis.输尿管梗阻会促进输尿管炎症和纤维化。
Eur Urol Focus. 2023 Mar;9(2):371-380. doi: 10.1016/j.euf.2022.09.014. Epub 2022 Oct 13.
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CAV1 alleviated CaOx stones formation suppressing autophagy-dependent ferroptosis.CAV1 通过抑制自噬依赖性铁死亡缓解 CaOx 结石形成。
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Transforming growth factor-β in tissue fibrosis.组织纤维化中的转化生长因子-β。
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