Literature DB >> 28603028

Targeting of p32 in peritoneal carcinomatosis with intraperitoneal linTT1 peptide-guided pro-apoptotic nanoparticles.

Hedi Hunt1, Lorena Simón-Gracia1, Allan Tobi1, Venkata Ramana Kotamraju2, Shweta Sharma2, Mait Nigul3, Kazuki N Sugahara4, Erkki Ruoslahti5, Tambet Teesalu6.   

Abstract

Gastrointestinal and gynecological malignancies disseminate in the peritoneal cavity - a condition known as peritoneal carcinomatosis (PC). Intraperitoneal (IP) administration can be used to improve therapeutic index of anticancer drugs used for PC treatment. Activity of IP anticancer drugs can be further potentiated by encapsulation in nanocarriers and/or affinity targeting with tumor-specific affinity ligands, such as tumor homing peptides. Here we evaluated a novel tumor penetrating peptide, linTT1 (AKRGARSTA), as a PC targeting ligand for nanoparticles. We first demonstrated that the primary homing receptor for linTT1, p32 (or gC1qR), is expressed on the cell surface of peritoneal carcinoma cell lines of gastric (MKN-45P), ovarian (SKOV-3), and colon (CT-26) origin, and that peritoneal tumors in mice and clinical peritoneal carcinoma explants express p32 protein accessible from the IP space. Iron oxide nanoworms (NWs) functionalized with the linTT1 peptide were taken up and routed to mitochondria in cultured PC cells. NWs functionalized with linTT1 peptide in tandem with a pro-apoptotic [D(KLAKLAK)2] peptide showed p32-dependent cytotoxicity in MKN-45P, SKOV-3, and CT-26 cells. Upon IP administration in mice bearing MKN-45P, SKOV-3, and CT-26 tumors, linTT1-functionalized NWs showed robust homing and penetration into malignant lesions, whereas only a background accumulation was seen in control tissues. In tumors, the linTT1-NW accumulation was seen predominantly in CD31-positive blood vessels, in LYVE-1-positive lymphatic structures, and in CD11b-positive tumor macrophages. Experimental therapy of mice bearing peritoneal MKN-45P xenografts and CT-26 syngeneic tumors with IP linTT1-D(KLAKLAK)2-NWs resulted in significant reduction of weight of peritoneal tumors and significant decrease in the number of metastatic tumor nodules, whereas treatment with untargeted D(KLAKLAK)2-NWs had no effect. Our data show that targeting of p32 with linTT1 tumor-penetrating peptide improves tumor selectivity and antitumor efficacy of IP pro-apoptotic NWs. P32-directed intraperitoneal targeting of other anticancer agents and nanoparticles using peptides and other affinity ligands may represent a general strategy to increase their therapeutic index.
Copyright © 2017 Elsevier B.V. All rights reserved.

Entities:  

Keywords:  Iron oxide nanoworms; MR imaging; Nanomedicine; Neuropilin-1; Peptide; Peritoneal carcinomatosis; Pro-apoptotic peptide; Tumor targeting; p32

Mesh:

Substances:

Year:  2017        PMID: 28603028      PMCID: PMC6129970          DOI: 10.1016/j.jconrel.2017.06.005

Source DB:  PubMed          Journal:  J Control Release        ISSN: 0168-3659            Impact factor:   9.776


  58 in total

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4.  Proapoptotic peptide-mediated cancer therapy targeted to cell surface p32.

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Authors:  N Bakrin; J M Classe; C Pomel; S Gouy; G Chene; O Glehen
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9.  Mitochondrial p32 protein is a critical regulator of tumor metabolism via maintenance of oxidative phosphorylation.

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10.  Anticancer effects of gemcitabine are enhanced by co-administered iRGD peptide in murine pancreatic cancer models that overexpressed neuropilin-1.

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Journal:  Br J Cancer       Date:  2014-02-20       Impact factor: 7.640

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  14 in total

1.  Tumor-mesoporous silica nanoparticle interactions following intraperitoneal delivery for targeting peritoneal metastasis.

Authors:  Derek Hargrove; Brian Liang; Raana Kashfi-Sadabad; Gaurav N Joshi; Laura Gonzalez-Fajardo; Sterling Glass; Michael Jay; Andrew Salner; Xiuling Lu
Journal:  J Control Release       Date:  2020-11-07       Impact factor: 9.776

Review 2.  An approach to p32/gC1qR/HABP1: a multifunctional protein with an essential role in cancer.

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3.  Competition of charge-mediated and specific binding by peptide-tagged cationic liposome-DNA nanoparticles in vitro and in vivo.

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4.  Electrostatic Conjugation of Nanoparticle Surfaces with Functional Peptide Motifs.

Authors:  Natalie Boehnke; Kate J Dolph; Valeria M Juarez; Julia M Lanoha; Paula T Hammond
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Review 5.  Homing Peptides for Cancer Therapy.

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Review 6.  Multi-functional, multicompartmental hyaluronan-binding protein 1 (HABP1/p32/gC1qR): implication in cancer progression and metastasis.

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Review 7.  Neuropilins in the Context of Tumor Vasculature.

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9.  Application of polymersomes engineered to target p32 protein for detection of small breast tumors in mice.

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Journal:  Oncotarget       Date:  2018-04-10

Review 10.  Peritoneal Carcinomatosis Targeting with Tumor Homing Peptides.

Authors:  Lorena Simón-Gracia; Hedi Hunt; Tambet Teesalu
Journal:  Molecules       Date:  2018-05-16       Impact factor: 4.411

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