Application of bone marrow mesenchymal stem cells attached poly(lactic-co-glycolic acid)-collagen I scaffold patch in rat inguinal hernia model

Abstract

Abstract: Objective To study the repair effect of PLGA-collagen I patch on inguinal hernia. Methods First, the PLGA-collagen I patch was prepared. Then, the rat bone marrow mesenchymal stem cells were extracted, and the rat model of abdominal wall defect was made. Bone marrow mesenchymal stem cells (BMSCs) bearing tissue engineering patches (experimental group) and cell-free tissue engineering patches (control group) were implanted into the groin respectively. The changes of pro-inflammatory factor IL-6 (interleukin -6) and IL-10 (interleukin -10) were detected by ELISA kit after operation. Immunohistochemistry was used to detect the change of macrophage surface antigen to analyze the inflammatory reaction. HE staining was used to observe the regeneration of tissue in the patch and the degradation state of the material. SEM was used to observe the integrity of peritoneum. The angiogenesis state was detected by immunohistochemistry. The formation of collagen fiber was detected by trichrome staining of Masson. Results After a week, the macrophages invasion in the patch of both the experimental group and the control group were significantly increased. For one month, the inflammatory reaction gradually subsided and the number of macrophages decreased. Long term tests showed that the BMSCs patch could promote the synthesis of collagen fibers, regeneration of blood vessels, and repair of abdominal wall injury. One month after surgery, there was no swelling in the abdominal wall of the experimental group and the control group. The rats were healthy. In one month, two months and six months after the operation, the tissue morphology and SEM electron microscope were observed. The PLGA-collagen I patch of BMSCs can promote cell infiltration, angiogenesis and tissue regeneration. The degradation rate of PLGA material was faster. In sixth months, the cell - based patch was almost completely degraded. However, PLGA-collagen I patches that were not planted cells were degraded, though. It degraded to pieces and remained in the body as a foreign body. Conclusions In this study, PLGA-collagen I tissue engineering materials planted with BMSCs can repair the defects more quickly and reliably, so as to achieve the purpose of treatment of hernia.

Key words: PLGA-Collagen I patch, inguinal hernia, macrophage, inflammatory response

CLC Number:

R656.21

[1]	. Soybean isoflavone reduces cerebral ischemia-reperfusion injury in rats [J]. , 2019, 39(11): 1543-1547.
[2]	. Role of prostaglandin E receptor in inhibition on the inflammatory reaction of human pulmonary macrophages [J]. Basic & Clinical Medicine, 2019, 39(1): 90-91.
[3]	. Impact of celastrol on polarization of mouse peritoneal macrophage [J]. Basic & Clinical Medicine, 2018, 38(5): 643-648.
[4]	. Evodiamine decreases blood glucose in type II diabetes rats [J]. Basic & Clinical Medicine, 2018, 38(10): 1443-1445.
[5]	. Effects of different anesthetic methods on the patients quality of recovery score and surgical satisfaction after oblique inguinal hernia repair [J]. Basic & Clinical Medicine, 2017, 37(12): 1746-1749.
[6]	. Effect of E3 ubiquitin ligase RNF121 on expression of proinflammatory cytokines in LPS-treated macrophages [J]. Basic & Clinical Medicine, 2016, 36(5): 581-585.
[7]	. Lenalidomide significantly inhibit the differentiation of monocytes to M2 polarized macrophages and down-regulate secretion of associated cytokines [J]. Basic & Clinical Medicine, 2015, 35(6): 786-791.
[8]	. Lactic Acid Regulates Phenotype Polarization and Function of Macrophages in Tumor Microenvironment [J]. Basic & Clinical Medicine, 2014, 34(6): 740-745.
[9]	. Ulinastatin alleviates patients’ inflammatory response, acute and chronic pain after bilateral total knee arthroplasty [J]. Basic & Clinical Medicine, 2014, 34(4): 514-518.
[10]	. Toll-like receptor activation and stimulation promote the secretion of matrix metalloproteinases 9 of human ovarian cancer via co-cultrued with tumor associated macrophage [J]. Basic & Clinical Medicine, 2014, 34(10): 1315-1320.
[11]	. Sodium hydrosulfide inhibits inflammatory factor secretion in macrophages [J]. Basic & Clinical Medicine, 2012, 32(12): 1374-1377.
[12]	Ru ZHENG; Xiao-jian HAO; Lei GUO; Juan LI; Xiao-li YU; Cai-ying YE; De-chang ZHANG. Inhibitory effect of CAI on iNOS expression and NF-κB activation degradation in rat peritoneal macrophages [J]. Basic & Clinical Medicine, 2010, 30(5): 466-470.
[13]	Dan-dan ZHANG; Zhan-min XU; Ai-li SONG; Quan-ming ZHAO; Xiao-li DONG. Image of pathology in rabbit unstable plaque with18F-FDG PET/CT detection [J]. Basic & Clinical Medicine, 2010, 30(1): 33-36.
[14]	Li-kun ZHENG; Lei ZHANG; Nai-yao CHEN; Shou-ling WU; Hui ZHAO. Progress in the treatment of acute lung injury with Mesenchymal stem cells [J]. Basic & Clinical Medicine, 2009, 29(9): 1002-1006.
[15]	Jian-yun ZHOU; Jun YAN; Ce YANG; Qing LIU; Ying CHENG; Jian-xin JIANG. The enhancing effects of Norepinephrine on immune functions of rat peritoneal macrophages [J]. Basic & Clinical Medicine, 2009, 29(1): 85-86.

Application of bone marrow mesenchymal stem cells attached poly(lactic-co-glycolic acid)-collagen I scaffold patch in rat inguinal hernia model

PDF

Knowledge

Abstract

Cite this article

share this article

References

Related Articles 15

Recommended Articles

Metrics

Comments