Safety of menstrual blood-derived stromal cell transplantation in treatment of intrauterine adhesion

Qi-Yuan Chang; Si-Wen Zhang; Ping-Ping Li; Zheng-Wei Yuan; Ji-Chun Tan

doi:10.4252/wjsc.v12.i5.368

Safety of menstrual blood-derived stromal cell transplantation in treatment of intrauterine adhesion

World J Stem Cells. 2020 May 26;12(5):368-380. doi: 10.4252/wjsc.v12.i5.368.

Authors

Qi-Yuan Chang¹, Si-Wen Zhang¹, Ping-Ping Li¹, Zheng-Wei Yuan², Ji-Chun Tan¹

Affiliations

¹ Department of Obstetrics and Gynecology, Shengjing Hospital of China Medical University, Shenyang 110022, Liaoning Province, China.
² Key Laboratory of Health Ministry for Congenital Malformation, Shengjing Hospital of China Medical University, Benxi 117004, Liaoning Province, China.

Abstract

Background: Intrauterine adhesion (IUA) can cause serious damage to women's reproductive health, yet current treatment methods are difficult to achieve satisfactory results. In our previous studies, we demonstrated that menstrual-derived stromal stem cells (MenSCs), with high proliferative capacity and self-renewal ability, have a powerful therapeutic effect in patients with severe IUA. However, safety assessment of MenSCs transplantation is essential for its further application.

Aim: To evaluate the short-, medium-, and long-term biosafety of MenSCs via intrauterine transplantation in a rat model of IUA, with a focus on toxicity and tumorigenicity.

Methods: MenSCs were injected into the sub-serosal layer of the uterus in an IUA rat model, for 3 d, 3 mo, and 6 mo separately, to monitor the corresponding acute, sub-chronic, and chronic effects. Healthy rats of the same age served as negative controls. Toxicity effects were evaluated by body weight, organ weight, histopathology, hematology, and biochemistry tests. Tumorigenicity of MenSCs was investigated in Balb/c-nu mice in vivo and by colony formation assays in vitro.

Results: Compared with the same week-old control group, all of the IUA rats receiving MenSC transplantation demonstrated no obvious changes in body weight, main organ weight, or blood cell composition during the acute, sub-chronic, and chronic observation periods. At the same time, serum biochemical tests showed no adverse effects on metabolism or liver and kidney function. After 4 wk of subcutaneous injection of MenSCs in Balb/c-nu nude mice, no tumor formation or cell metastasis was observed. Moreover, there was no tumor colony formation of MenSCs during soft agar culture in vitro.

Conclusion: There is no acute, sub-chronic, or chronic poisoning, infection, tumorigenesis, or endometriosis in rats with IUA after MenSC transplantation. The above results suggest that intrauterine transplantation of MenSCs is safe for endometrial treatment.

Keywords: Biosafety; Endometrial treatment; Intrauterine adhesion; Menstrual blood-derived stromal cells; Stem cell transplantation; Toxicity.