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来自过氧化物酶体素A1(毒素T-514)诱导的肾脏和肺脏细胞凋亡的组织病理学、超微结构及生化特征。

Histopathological, ultrastructural, and biochemical traits of apoptosis induced by peroxisomicine A1 (toxin T-514) from in kidney and lung.

作者信息

Soto-Domínguez Adolfo, Salas-Treviño Daniel, Guillén-Meléndez Gloria A, Castillo-Velázquez Uziel, Ballesteros-Elizondo Raquel G, Montes-de-Oca-Saucedo Carlos R, Villa-Cedillo Sheila A, Morales-Ávalos Rodolfo, Rodríguez-Tovar Luis E, Montes-de-Oca-Luna Roberto, Saucedo-Cárdenas Odila

机构信息

Universidad Autónoma de Nuevo León, Facultad de Medicina, Departamento de Histología, Av. Madero y E. Aguirre-Pequeño s/n, Col. Mitras Centro, Monterrey, N.L, C.P. 64460, Mexico.

Universidad Autónoma de Nuevo León, Facultad de Medicina Veterinaria y Zootecnia, Cuerpo Académico de Zoonosis y Enfermedades Emergentes. General Escobedo, N. L, C.P. 66050, Mexico.

出版信息

Toxicon X. 2022 Dec 22;17:100148. doi: 10.1016/j.toxcx.2022.100148. eCollection 2023 Mar.

Abstract

Peroxisomicine A1 (PA1) is a toxin isolated from the genus plants whose target organs are the liver, kidney, and lung. studies demonstrated the induction of apoptosis by PA1 in cancer cell lines, and in the liver. Apoptosis has a wide range of morphological features such as cell shrinkage, plasma membrane blistering, loss of microvilli, cytoplasm, and chromatin condensation, internucleosomal DNA fragmentation, and formation of apoptotic bodies that are phagocytized by resident macrophages or nearby cells. Early stages of apoptosis can be detected by mitochondrial alterations. We investigated the presence of apoptosis at the morphological, ultrastructural, and biochemical levels in two target organs of PA1: kidney and lung. Sixty CD-1 mice were divided into three groups (n = 20): untreated control (ST), vehicle control (VH), and PA1 intoxicated group (2LD50). Five animals of each group were sacrificed at 4, 8, 12, and 24 h post-intoxication. Kidney and lung were examined by morphometry, histopathology, ultrastructural, and DNA fragmentation analysis. Pre-apoptotic mitochondrial alterations were present at 4 h. Apoptotic bodies were observed at 8 h and increased over time. TUNEL positive cells were detected as early as 4 h, and the DNA ladder pattern was observed at 12 h and 24 h. The liver showed the highest value of fragmented DNA, followed by the kidney and the lung. We demonstrated the induction of apoptosis by a toxic dose of PA1 in the kidney and lung . These results could be useful in understanding the mechanism of action of this compound at toxic doses .

摘要

过氧新霉素A1(PA1)是一种从植物属中分离出的毒素,其靶器官为肝脏、肾脏和肺。研究表明,PA1可诱导癌细胞系以及肝脏中的细胞凋亡。细胞凋亡具有多种形态学特征,如细胞皱缩、质膜起泡、微绒毛丧失、细胞质和染色质浓缩、核小体间DNA片段化以及形成被驻留巨噬细胞或附近细胞吞噬的凋亡小体。凋亡的早期阶段可通过线粒体改变来检测。我们在PA1的两个靶器官——肾脏和肺中,从形态学、超微结构和生化水平研究了细胞凋亡的存在情况。将60只CD-1小鼠分为三组(n = 20):未处理对照组(ST)、溶剂对照组(VH)和PA1中毒组(2LD50)。每组5只动物在中毒后4、8、12和24小时处死。通过形态测量、组织病理学、超微结构和DNA片段化分析对肾脏和肺进行检查。中毒后4小时出现凋亡前期线粒体改变。8小时观察到凋亡小体,且随时间增加。最早在4小时检测到TUNEL阳性细胞,在12小时和24小时观察到DNA梯状图谱。肝脏的DNA片段化值最高,其次是肾脏和肺。我们证明了毒性剂量的PA1可诱导肾脏和肺中的细胞凋亡。这些结果可能有助于理解该化合物在毒性剂量下的作用机制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2a0c/9803956/0878831d24c0/ga1.jpg

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