Permanent acceptance of mouse cardiac allografts with CD40 siRNA to induce regulatory myeloid cells by use of a novel polysaccharide siRNA delivery system

FOXP3型 CD11c公司 过继性细胞移植 生物 免疫学 CD154 CD40 基因沉默 小干扰RNA 脾细胞 免疫耐受 CD8型 化疗增敏剂 移植 免疫系统 癌症研究 细胞生物学 医学 转染 细胞毒性T细胞 T细胞 细胞培养 基因 体外 表型 外科 细胞毒性 生物化学 遗传学
作者
Qi Zhang,Naotsugu Ichimaru,Shohei Higuchi,Songjie Cai,Jun Hou,M Fujino,Norio Nonomura,M. Kobayashi,Hisami Ando,Akiko Uno,Kazuo Sakurai,Shinichi Mochizuki,Yoshiyuki Adachi,Norioki Ohno,Hai Zou,Jin Xu,Li Xk,S. Takahara
出处
期刊:Gene Therapy [Springer Nature]
卷期号:22 (3): 217-226 被引量:19
标识
DOI:10.1038/gt.2014.119
摘要

The CD40/CD154 co-stimulatory pathway is crucial in alloimmune response. We developed a novel small interfering RNA (siRNA) delivery system with a poly-dA extension at the 5'-end of the siRNA sense strand that was stably incorporated into 1,3-β-glucan (schizophyllan, SPG). This was captured and incorporated into dendritic cells (DCs) through its receptor, Dectin-1, specifically silencing CD40 genes (siCD40) to exert immunoregulatory activity. siCD40/SPG-treated CBA mice permanently accepted B10 fully mismatched cardiac allografts. Consistent with graft survival, the infiltration of CD4(+), CD8(+) T cells into the graft was lower, and that the numbers of CD40(low)CD11c(+) DCs cells and CD4(+)Foxp3(+)cells were increased in both the graft and in the recipient spleen. In addition, naive CBA recipients given an adoptive transfer of splenocytes from the primary recipients with siCD40/SPG accepted a heart graft from donor-type B10, but not third-party Balb/c mice. In conclusion, the treatment with siCD40/SPG targeting DCs could generate antigen-specific Tregs, resulting in the permanent acceptance of mouse cardiac allografts. These findings have important implications for clarifying the mechanism underlying the induction of tolerance in DCs, and also highlight the potential of immunomodulation and the feasibility of siRNA-based clinical therapy in the transplantation field.
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