Intrarenal Arterial Transplantation of Dexmedetomidine Preconditioning Adipose Stem-Cell-Derived Microvesicles Confers Further Therapeutic Potential to Attenuate Renal Ischemia/Reperfusion Injury through miR-122-5p/Erythropoietin/Apoptosis Axis

Yu-Hsuan Cheng; Kuo-Hsin Chen; Yi-Ting Sung; Chih-Ching Yang; Chiang-Ting Chien

doi:10.3390/antiox11091702

Intrarenal Arterial Transplantation of Dexmedetomidine Preconditioning Adipose Stem-Cell-Derived Microvesicles Confers Further Therapeutic Potential to Attenuate Renal Ischemia/Reperfusion Injury through miR-122-5p/Erythropoietin/Apoptosis Axis

Antioxidants (Basel). 2022 Aug 30;11(9):1702. doi: 10.3390/antiox11091702.

Authors

Yu-Hsuan Cheng¹, Kuo-Hsin Chen^{2

3}, Yi-Ting Sung¹, Chih-Ching Yang^{1

4

5}, Chiang-Ting Chien¹

Affiliations

¹ Department of Life Science, School of Life Science, College of Science, National Taiwan Normal University, No. 88, Section 4, Tingzhou Road, Taipei 11677, Taiwan.
² Department of Surgery, Division of General Surgery, Far-Eastern Memorial Hospital, New Taipei City 22056, Taiwan.
³ Department of Electrical Engineering, Yuan Ze University, Taoyuan City 32003, Taiwan.
⁴ Office of Public Relation of Ministry of Health and Welfare, No. 488, Section 6, Zhongxiao E. Rd., Nangang District, Taipei 115204, Taiwan.
⁵ MacKay Junior College of Medicine, Nursing and Management, New Taipei City 11260, Taiwan

Abstract

Intravenous adipose mesenchymal stem cells (ADSCs) attenuate renal ischemia/reperfusion (IR) injury but with major drawbacks, including the lack of a specific homing effect after systemic infusion, cell trapping in the lung, and early cell death in the damaged microenvironment. We examined whether intrarenal arterial transplantation of dexmedetomidine (DEX) preconditioning ADSC-derived microvesicles (DEX-MVs) could promote further therapeutic potential to reduce renal IR injury. We evaluated the effect of DEX-MVs on NRK-52E cells migration, hypoxia/reoxygenation (H/R)-induced cell death, and reactive oxygen species (ROS) amount and renal IR model in rats. IR was established by bilateral 45 min ischemia followed by 4 h reperfusion. Intrarenal MVs or DEX-MVs were administered prior to ischemia. Renal oxidative stress, hemodynamics and function, western blot, immunohistochemistry, and tubular injury scores were determined. The miR-122-5p expression in kidneys was analyzed using microarrays and quantitative RT-PCR and its action target was predicted by TargetScan. DEX-MVs were more efficient than MVs to increase migration capability and to further decrease H/R-induced cell death and ROS level in NRK-52E cells. Consistently, DEX-MVs were better than MV in increasing CD44 expression, improving IR-depressed renal hemodynamics and renal erythropoietin expression, inhibiting IR-enhanced renal ROS level, tubular injury score, miR-122-5p expression, pNF-κB expression, Bax/caspase 3/poly(ADP-ribose) polymerase (PARP)-mediated apoptosis, blood urea nitrogen, and creatinine levels. The use of NRK-52E cells confirmed that miR-122-5p mimic via inhibiting erythropoietin expression exacerbated Bax-mediated apoptosis, whereas miR-122-5p inhibitor via upregulating erythropoietin and Bcl-2 expression reduced apoptosis. In summary, intrarenal arterial DEX-MV conferred further therapeutic potential to reduce renal IR injury through the miR-122-5p/erythropoietin/apoptosis axis.

Keywords: adipose-derived mesenchymal stem cells; apoptosis; dexmedetomidine preconditioning; erythropoietin; ischemia/reperfusion; miR-122-5p; microvesicles.

Grants and funding

MOST 106-2320-B-003 -002-MY3/Ministry of Science and Technology