Umbilical Cord Blood-Derived M1 Macrophage Exosomes Loaded with Cisplatin Target Ovarian Cancer In Vivo and Reverse Cisplatin Resistance

Xiaohui Zhang; Jiapo Wang; Na Liu; Weimin Wu; Hong Li; Wen Lu; Xiaoqing Guo

doi:10.1021/acs.molpharmaceut.3c00132

Umbilical Cord Blood-Derived M1 Macrophage Exosomes Loaded with Cisplatin Target Ovarian Cancer In Vivo and Reverse Cisplatin Resistance

Mol Pharm. 2023 Nov 6;20(11):5440-5453. doi: 10.1021/acs.molpharmaceut.3c00132. Epub 2023 Oct 11.

Authors

Xiaohui Zhang¹, Jiapo Wang¹, Na Liu¹, Weimin Wu¹, Hong Li², Wen Lu¹, Xiaoqing Guo¹

Affiliations

¹ Shanghai First Maternity and Infant Hospital, Tong Ji University School of Medicine, Shanghai 201204, China.
² Shanghai Institute of Biochemistry and Cell Biology, Shanghai 200031, China.

PMID: 37819754
DOI: 10.1021/acs.molpharmaceut.3c00132

Abstract

We investigated the therapeutic efficacy of umbilical cord blood (UCB)-derived M1 macrophage exosomes loaded with cisplatin (CIS) in ovarian cancer and platinum resistance. M1 macrophages were purified by using CD14 magnetic beads and characterized by flow cytometry. Our analyses included morphology, particle size, particle concentration, potential, drug loading capacity, counts of entry into cells, antitumor effect in vivo, and the ability to reverse drug resistance. A2780, SKOV3, and A2780/DDP, SKOV3/DDP ovarian cancer cells (CIS-sensitive and CIS-resistant cell lines, respectively) were treated with CIS or CIS-loaded M1 macrophage exosomes (M1exoCISs). The encapsulation efficiency of CIS loading into M1 macrophage exosomes was approximately 30%. In vitro, M1exoCIS treatment reduced the CIS IC50 values of both A2780, SKOV3, and A2780/DDP, SKOV3/DDP cells. We evaluated the effect of M1exoCIS on tumor growth using a mouse ovarian cancer subcutaneous transplantation tumor model inoculated with A2780/DDP cells. M1exoCIS was observed in the liver, spleen, and tumor sites 24 h posttreatment; the fluorescence intensity of M1exoCIS is higher than that of CIS. After 7 days, M1exoCIS significantly inhibited the growth of subcutaneously transplanted tumors compared with CIS alone and had a longer survival time. Moreover, the toxicity test shows that M1exoCIS has less hepatorenal toxicity than CIS. To investigate the mechanism of M1exoCIS targeting, homing, and reversing drug resistance, we performed RT-PCR, Western blotting, and Proteome Profiler Human Receptor Array analyses. We found that A2780 and A2780/DDP cells expressed the integrin β1/CD29 receptor, while M1 exosomes expressed integrin β1/CD29. In addition, M1exos carries long noncoding RNA H19, implicated in PTEN protein upregulation and miR-130a and Pgp gene downregulation, leading to the reversal of CIS drug resistance. Therefore, UCB-derived M1exoCIS target tumor sites of ovarian cancer in vivo and can be used to increase the CIS sensitivity and cytotoxicity.

Keywords: cisplatin; cord blood; drug resistance; exosome; macrophages; ovarian cancer.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antineoplastic Agents* / pharmacology
Antineoplastic Agents* / therapeutic use
Apoptosis
Cell Line, Tumor
Cell Proliferation
Cisplatin / pharmacology
Cisplatin / therapeutic use
Drug Resistance, Neoplasm
Exosomes* / metabolism
Female
Fetal Blood / metabolism
Humans
Integrin beta1 / pharmacology
Integrin beta1 / therapeutic use
Ovarian Neoplasms* / drug therapy
Ovarian Neoplasms* / genetics

Substances

Cisplatin
Integrin beta1
Antineoplastic Agents