Characterization of pancreatic islet cell tumors and renal tumors induced by a combined treatment of streptozotocin and nicotinamide in male SD rats

Yuki Kato , Koichi Masuno , Kae Fujisawa , Noriko Tsuchiya , Mikinori Torii , Atsuko Hishikawa , Takeshi Izawa , Mitsuru Kuwamura , Jyoji Yamate
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引用次数: 1

Abstract

We herein investigated the histopathological features, including proliferative activity and immunoexpression, of pancreatic islet cell tumors (ICTs) in male SD rats induced by streptozotocin (STZ) and nicotinamide (NA), and discussed their relevance to biological behaviors and prognoses. A total of 70 and 43% of rats developed ICTs 37–45 weeks after the treatment with STZ (50 or 75 mg/kg, i.v.) and NA (350 mg/kg, twice, p.o.), respectively. Among the islet tumors observed in the STZ/NA-treated groups, 75% were adenomas, while 25% were carcinomas. Most STZ/NA-induced carcinomas were characterized by well-differentiated tumor cells with/without local invasion into the surrounding tissues, and weak proliferative activity. No outcome such as distance metastasis and death was noted. All of the ICTs strongly expressed insulin, part of which had hormone productivity; however there were no hypoglycemia-related clinical signs such as convulsion in these rats 36 weeks after the treatment. These results suggested that rat ICTs induced STZ/NA have small impact on biological activity or prognosis. STZ/NA treatment significantly increased of focal proliferative lesions in the kidney, liver and adrenal glands other than pancreatic islets. Of the STZ/NA-induced kidney tumors, more than 60% were renal cell adenomas, and many of them were basophilic type. The incidence of eosinophilic or clear cell type of tumors was less than 10%, respectively. Immunohistochemical analyses revealed that many of the STZ/NA-induced basophilic type of renal tumors were derived from proximal tubules, whereas the clear cell and eosinophilic types were derived from collecting tubules.

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链脲佐菌素和烟酰胺联合治疗SD雄性大鼠胰岛细胞瘤和肾肿瘤的研究
本文研究了链脲佐菌素(STZ)和烟酰胺(NA)诱导雄性SD大鼠胰岛细胞肿瘤(ICTs)的组织病理学特征,包括增殖活性和免疫表达,并讨论了其与生物学行为和预后的相关性。STZ(50或75 mg/kg,静脉注射)和NA (350 mg/kg,两次,口服)治疗37-45周后,分别有70%和43%的大鼠出现ict。STZ/ na治疗组胰岛肿瘤中腺瘤占75%,癌占25%。大多数STZ/ na诱导的癌的特点是肿瘤细胞分化良好,局部浸润周围组织,增殖活性弱。未观察到远处转移和死亡等结果。所有的ict都强烈表达胰岛素,其中一部分具有激素生产力;然而,治疗36周后,这些大鼠没有出现与低血糖相关的临床症状,如抽搐。这些结果表明,ict诱导的STZ/NA对大鼠的生物活性和预后影响较小。STZ/NA治疗显著增加了除胰岛外肾、肝和肾上腺的局灶性增生性病变。在STZ/ na诱导的肾肿瘤中,60%以上为肾细胞腺瘤,且多为嗜碱性型。嗜酸性细胞型和透明细胞型肿瘤的发生率均小于10%。免疫组织化学分析显示,许多STZ/ na诱导的嗜碱性肾肿瘤来源于近端小管,而透明细胞型和嗜酸性肾肿瘤来源于集合小管。
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来源期刊
CiteScore
2.08
自引率
0.00%
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0
审稿时长
5.3 weeks
期刊介绍: Cessation. The international multidisciplinary journal is devoted to the publication of studies covering the whole range of experimental research on disease processes and toxicology including cell biological investigations. Its aim is to support progress in the interdisciplinary cooperation of researchers working in pathobiology, toxicology, and cell biology independent of the methods applied. During the past decades increasing attention has been paid to the importance of toxic influence in the pathogenesis of human and animal diseases. This is why Experimental and Toxicologic Pathology meets the urgent need for an interdisciplinary journal felt by a wide variety of experts in medicine and biology, including pathologists, toxicologists, biologists, physicians, veterinary surgeons, pharmacists, and pharmacologists working in academic, industrial or clinical institutions.
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