PO.CH01.04 · 化学

Targeted delivery of suicide gene to tumor cells using PD-L1-targeted extracellular vesicles for cancer therapy

海报缩略图:Targeted delivery of suicide gene to tumor cells using PD-L1-targeted extracellular vesicles for cancer therapy
编号 6385 展板 17 时间 4/21 02:00–05:00 区域 Section 38 主讲 Geuna Park, MS
分会场 Drug Delivery
查看完整资料 下载 PDF 登录后可访问当前开放资料 AACR 官方页面 ↗

作者与单位

Geuna Park1, SeokMin Lee1, Eun Jung Park2, Byungheon Lee1

1Kyungpook National Univ. School of Med, Daegu, Korea, Republic of,2National Cancer Center, Goyang, Korea, Republic of

摘要 Abstract

Herpes simplex virus-thymidine kinase (HSV-TK) gene, a well-known suicide gene, causes cell death in rapidly dividing cells when treated with ganciclovir (GCV). The HSV-TK activates GCV and makes GCV-triphosphate. Insertion of activated GCV-triphosphate in elongating DNA by cellular DNA polymerases interferes DNA duplication and eventually leads to cell death. The suicide gene therapy, however, has been limited by non-specific cytotoxicity in off-target cells such as normal cells. In this study, we explored PD-L1-targeted extracellular vesicles (EVs) carrying the HSV-TK mRNA to deliver the HSV-TK selectively into tumor cells. HEK 293FT cells were transduced using lentivirus with the GFP-tagged, HSV-TK gene containing a sequence that is recognized by EV-trafficking RNA-binding protein. Stable HEK 293FT cells expressing the HSV-TK gene were established. EVs were isolated from the stable cells and labeled with a PD-L1-binding peptide (CVRARTR) using click chemistry to target PD-L1-high tumor cells. Delivery of the HSV-TK mRNA after incubation of cells with the EVs was validated by observing the fluorescence of GFP tag under a microscope. The PD-L1-targeted EVs carrying the HSV-TK mRNA exerted an efficient cytotoxicity in PD-L1-high MDA-MB-231 tumor cells. On the other hand, the EVs showed low levels of cytotoxicity in PD-L1-low tumor cells and normal cells. Systemic administration of the EVs inhibited the growth of MDA-MB-231 tumor xenografts in mice. These results demonstrate that the PD-L1-targeted EVs containing the HSV-TK mRNA provide a new avenue for the targeted delivery of a suicide gene. Keywords: HSV-TK; Peptide; PD-L1; Suicide gene therapy
利益披露 Disclosure
G. Park, None.. S. Lee, None.. E. Park, None.. B. Lee, None.

在会议检索中打开