Literature DB >> 30407790

Epidermal Growth Factor Receptor-Targeting Peptide Nanoparticles Simultaneously Deliver Gemcitabine and Olaparib To Treat Pancreatic Cancer with Breast Cancer 2 ( BRCA2) Mutation.

Chong Du1,2, Yingqiu Qi2,3, Yinlong Zhang2,4, Yazhou Wang1,2, Xiao Zhao2, Huan Min2,3, Xuexiang Han2,5, Jiayan Lang2,5, Hao Qin2,5, Quanwei Shi2,5, Zhengkui Zhang1, Xiaodong Tian1, Greg J Anderson6, Ying Zhao2,5, Guangjun Nie2,5, Yinmo Yang1.   

Abstract

Pancreatic cancer (PCa) is one of the most lethal malignancies, with a 5 year survival rate of less than 8%. Current treatment regiments have a low response rate in unselected patients. However, the subgroup of PCa patients with BRCA mutations may benefit from poly-ADP-ribose polymerase inhibitors (PARPi) due to their biological properties in DNA repair. Dose-limiting toxicity in normal tissues is frequently observed when PARPi are combined with other chemotherapies, and the co-delivery of two drugs to tumor sites at an adequate concentration is challenging. To address this issue, we have engineered an epidermal growth factor receptor (EGFR) targeting (with GE11 peptide) self-assembly amphiphilic peptide nanoparticle (GENP) to co-deliver gemcitabine and the PARPi olaparib to treat BRCA mutant PCa. The GENP was relatively stable, exhibited high encapsulation efficiency, and could coordinately release the two drugs in tumor milieu. Gemcitabine and olaparib showed strong synergistic actions in optimized conditions in vitro. The nanoparticle prolonged the half-life of both drugs and resulted in their tumor accumulation at the optimal therapeutic ratio in vivo. The drug-loaded nanoparticles were able to significantly suppress tumor growth in a murine PCa model with minimal side effects. Drug co-delivery of DNA damaging agents and PARP inhibitors via the GENP represents a promising approach for treatment of pancreatic cancers with molecular defects in the DNA repair pathway.

Entities:  

Keywords:  BRCA2 mutation; drug co-delivery; pancreatic cancer; self-assembly peptide nanoparticle; synthetic lethality

Mesh:

Substances:

Year:  2018        PMID: 30407790     DOI: 10.1021/acsnano.8b01573

Source DB:  PubMed          Journal:  ACS Nano        ISSN: 1936-0851            Impact factor:   15.881


  15 in total

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3.  A Combined Self-Assembled Drug Delivery for Effective Anti-Breast Cancer Therapy.

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Review 4.  Nanomedicine to Overcome Multidrug Resistance Mechanisms in Colon and Pancreatic Cancer: Recent Progress.

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5.  Targeted drug delivery strategies for precision medicines.

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Journal:  Nat Rev Mater       Date:  2021-02-02       Impact factor: 66.308

Review 6.  Self-assembling peptides-based nano-cargos for targeted chemotherapy and immunotherapy of tumors: recent developments, challenges, and future perspectives.

Authors:  Xue-Jun Wang; Jian Cheng; Le-Yi Zhang; Jun-Gang Zhang
Journal:  Drug Deliv       Date:  2022-12       Impact factor: 6.419

7.  Synthesis, Microtubule-Binding Affinity, and Antiproliferative Activity of New Epothilone Analogs and of an EGFR-Targeted Epothilone-Peptide Conjugate.

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Journal:  Int J Mol Sci       Date:  2019-03-05       Impact factor: 5.923

Review 8.  Advances in synthetic lethality for cancer therapy: cellular mechanism and clinical translation.

Authors:  Win Topatana; Sarun Juengpanich; Shijie Li; Jiasheng Cao; Jiahao Hu; Jiyoung Lee; Kenneth Suliyanto; Diana Ma; Bin Zhang; Mingyu Chen; Xiujun Cai
Journal:  J Hematol Oncol       Date:  2020-09-03       Impact factor: 17.388

Review 9.  Nanoparticle Formulations of Poly (ADP-ribose) Polymerase Inhibitors for Cancer Therapy.

Authors:  Bijay Singh; Shicheng Yang; Apurva Krishna; Srinivas Sridhar
Journal:  Front Chem       Date:  2020-11-23       Impact factor: 5.221

Review 10.  Molecular alterations and targeted therapy in pancreatic ductal adenocarcinoma.

Authors:  Yunzhen Qian; Yitao Gong; Zhiyao Fan; Guopei Luo; Qiuyi Huang; Shengming Deng; He Cheng; Kaizhou Jin; Quanxing Ni; Xianjun Yu; Chen Liu
Journal:  J Hematol Oncol       Date:  2020-10-02       Impact factor: 17.388

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