Estrone-Conjugated PEGylated Liposome Co-Loaded Paclitaxel and Carboplatin Improve Anti-Tumor Efficacy in Ovarian Cancer and Reduce Acute Toxicity of Chemo-Drugs

Huan Tang; Yizhuo Xie; Ming Zhu; Juan Jia; Rui Liu; Yujia Shen; Yucui Zheng; Xin Guo; Dongfanghui Miao; Jin Pei

doi:10.2147/IJN.S362263

Estrone-Conjugated PEGylated Liposome Co-Loaded Paclitaxel and Carboplatin Improve Anti-Tumor Efficacy in Ovarian Cancer and Reduce Acute Toxicity of Chemo-Drugs

Int J Nanomedicine. 2022 Jul 7:17:3013-3041. doi: 10.2147/IJN.S362263. eCollection 2022.

Authors

Huan Tang¹, Yizhuo Xie¹, Ming Zhu¹, Juan Jia¹, Rui Liu¹, Yujia Shen¹, Yucui Zheng¹, Xin Guo¹, Dongfanghui Miao¹, Jin Pei¹

Affiliation

¹ Department of Biopharmacy, School of Pharmaceutical Sciences, Jilin University, Changchun, People's Republic of China.

Abstract

Purpose: Ovarian cancer is the most lethal gynecologic malignancy. The combination of paclitaxel (PTX) and carboplatin (CBP) is the first-line remedy for clinical ovarian cancer. However, due to the limitations of adverse reaction and lacking of targeting ability, the chemotherapy of ovarian cancer is still poorly effective. Here, a novel estrone (ES)-conjugated PEGylated liposome co-loaded PTX and CBP (ES-PEG-Lip-PTX/CBP) was designed for overcoming the above disadvantages.

Methods: ES-PEG-Lip-PTX/CBP was prepared by film hydration method and could recognize estrogen receptor (ER) over-expressing on the surface of SKOV-3 cells. The characterizations, stability and in vitro release of ES-PEG-Lip-PTX/CBP were studied. In vitro cellular uptake and its mechanism were observed by fluorescence microscope. In vivo targeting effect in tumor-bearing mice was determined. Pharmacokinetics and biodistribution were studied in ICR mice. In vitro cytotoxicity and in vivo anti-tumor efficacy were evaluated on SKOV-3 cells and tumor-bearing mice, respectively. Finally, the acute toxicity in ICR mice was explored for assessing the preliminary safety of ES-PEG-Lip-PTX/CBP.

Results: Our results showed that ES-PEG-Lip-PTX/CBP was spherical shape without aggregation. ES-PEG-Lip-PTX/CBP exhibited the optimum targeting effect on uptake in vitro and in vivo. The pharmacokinetics demonstrated ES-PEG-Lip-PTX/CBP had improved the pharmacokinetic behavior. In vitro cytotoxicity showed that ES-PEG-Lip-PTX/CBP maximally inhibited SKOV-3 cell proliferation and its IC₅₀ values was 1.6 times lower than that of non-ES conjugated liposomes at 72 h. The in vivo anti-tumor efficacy study demonstrated that ES-PEG-Lip-PTX/CBP could lead strong SKOV-3 tumor growth suppression with a tumor volume inhibitory rate of 81.8%. Meanwhile, acute toxicity studies confirmed that ES-PEG-Lip-PTX/CBP significantly reduced the toxicity of the chemo drugs.

Conclusion: ES-PEG-Lip-PTX/CBP was successfully prepared with an optimal physicochemical and ER targeting property. The data of pharmacokinetics, anti-tumor efficacy and safety study indicated that ES-PEG-Lip-PTX/CBP could become a promising therapeutic formulation for human ovarian cancer in the future clinic.

Keywords: combination therapy; drug delivery system; estrogen receptor; liposome; ovarian cancer.

MeSH terms

Animals
Antineoplastic Agents* / therapeutic use
Antineoplastic Agents* / toxicity
Carboplatin / therapeutic use
Carboplatin / toxicity
Carcinoma, Ovarian Epithelial / drug therapy
Cell Line, Tumor
Drug Delivery Systems / methods
Estrone / therapeutic use
Female
Humans
Liposomes / therapeutic use
Mice
Mice, Inbred ICR
Ovarian Neoplasms* / drug therapy
Paclitaxel / therapeutic use
Polyethylene Glycols / chemistry
Tissue Distribution

Substances

Antineoplastic Agents
Liposomes
Estrone
Polyethylene Glycols
Carboplatin
Paclitaxel