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. 2020 Nov 28;2020:4640605. doi: 10.1155/2020/4640605

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Copyright © 2020 Min Tang et al.

This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

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Recombinant rat ANXA5 reversed the testicular oxidative stress promoting injury of miR-506-3p in DBP-treated rats: (a) H&E staining of testis tissues in DBP-treated rats following Agomir-506-3p and cotransfection of recombinant rat ANXA5 and Agomir-506-3p; (b) DHE staining of testis tissues in DBP-treated rats following Agomir-506-3p and cotransfection of recombinant rat ANXA5 and Agomir-506-3p, ROS exhibit red fluorescence under fluorescent microscope; (c) immunohistochemical staining showed ANXA5 expression level of testis tissues in DBP-treated rats following Agomir-506-3p and cotransfection of recombinant rat ANXA5 and Agomir-506-3p; (d) Western blotting showed the expression levels of Nrf2, ANXA5, HO-1, NQO1, and GST proteins of testis tissues in DBP-treated rats following Agomir-506-3p and cotransfection of recombinant rat ANXA5 and Agomir-506-3p. The data are showed as mean ± SD. ^∗Significantly different from the DBP + Agomir-506-3p group. ^∗P < 0.05, ^∗∗P < 0.01.