Literature DB >> 33795712

Antibody-drug nanoparticle induces synergistic treatment efficacies in HER2 positive breast cancer cells.

Muhammad Raisul Abedin1, Kaitlyne Powers1, Rachel Aiardo1, Dibbya Barua2, Sutapa Barua3.   

Abstract

Chemotherapeutic drugs suffer from non-specific binding, undesired toxicity, and poor blood circulation which contribute to poor therapeutic efficacy. In this study, antibody-drug nanoparticles (ADNs) are engineered by synthesizing pure anti-cancer drug nanorods (NRs) in the core of nanoparticles with a therapeutic monoclonal antibody, Trastuzumab on the surface of NRs for specific targeting and synergistic treatments of human epidermal growth factor receptor 2 (HER2) positive breast cancer cells. ADNs were designed by first synthesizing ~ 95 nm diameter × ~ 500 nm long paclitaxel (PTX) NRs using the nanoprecipitation method. The surface of PTXNRs was functionalized at 2' OH nucleophilic site using carbonyldiimidazole and conjugated to TTZ through the lysine residue interaction forming PTXNR-TTZ conjugates (ADNs). The size, shape, and surface charge of ADNs were characterized using scanning electron microscopy (SEM), SEM, and zeta potential, respectively. Using fluorophore labeling and response surface analysis, the percentage conjugation efficiency was found > 95% with a PTX to TTZ mass ratio of 4 (molar ratio ≈ 682). In vitro therapeutic efficiency of PTXNR-TTZ was evaluated in two HER2 positive breast cancer cell lines: BT-474 and SK-BR-3, and a HER2 negative MDA-MB-231 breast cancer cell using MTT assay. PTXNR-TTZ inhibited > 80% of BT-474 and SK-BR-3 cells at a higher efficiency than individual PTX and TTZ treatments alone after 72 h. A combination index analysis indicated a synergistic combination of PTXNR-TTZ compared with the doses of single-drug treatment. Relatively lower cytotoxicity was observed in MCF-10A human breast epithelial cell control. The molecular mechanisms of PTXNR-TTZ were investigated using cell cycle and Western blot analyses. The cell cycle analysis showed PTXNR-TTZ arrested > 80% of BT-474 breast cancer cells in the G2/M phase, while > 70% of untreated cells were found in the G0/G1 phase indicating that G2/M arrest induced apoptosis. A similar percentage of G2/M arrested cells was found to induce caspase-dependent apoptosis in PTXNR-TTZ treated BT-474 cells as revealed using Western blot analysis. PTXNR-TTZ treated BT-474 cells showed ~ 1.3, 1.4, and 1.6-fold higher expressions of cleaved caspase-9, cytochrome C, and cleaved caspase-3, respectively than untreated cells, indicating up-regulation of caspase-dependent activation of apoptotic pathways. The PTXNR-TTZ ADN represents a novel nanoparticle design that holds promise for targeted and efficient anti-cancer therapy by selective targeting and cancer cell death via apoptosis and mitotic cell cycle arrest.

Entities:  

Year:  2021        PMID: 33795712      PMCID: PMC8016985          DOI: 10.1038/s41598-021-86762-6

Source DB:  PubMed          Journal:  Sci Rep        ISSN: 2045-2322            Impact factor:   4.379


  122 in total

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5.  Polymeric conjugates for drug delivery.

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Journal:  Chem Mater       Date:  2012-01-04       Impact factor: 9.811

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Review 7.  Clinical efficacy of taxane-trastuzumab combination regimens for HER-2-positive metastatic breast cancer.

Authors:  Karen Bullock; Kimberly Blackwell
Journal:  Oncologist       Date:  2008-05

Review 8.  The spindle assembly checkpoint.

Authors:  Pablo Lara-Gonzalez; Frederick G Westhorpe; Stephen S Taylor
Journal:  Curr Biol       Date:  2012-11-20       Impact factor: 10.834

9.  2 years versus 1 year of adjuvant trastuzumab for HER2-positive breast cancer (HERA): an open-label, randomised controlled trial.

Authors:  Aron Goldhirsch; Richard D Gelber; Martine J Piccart-Gebhart; Evandro de Azambuja; Marion Procter; Thomas M Suter; Christian Jackisch; David Cameron; Harald A Weber; Dominik Heinzmann; Lissandra Dal Lago; Eleanor McFadden; Mitch Dowsett; Michael Untch; Luca Gianni; Richard Bell; Claus-Henning Köhne; Anita Vindevoghel; Michael Andersson; A Murray Brunt; Douglas Otero-Reyes; Santai Song; Ian Smith; Brian Leyland-Jones; Jose Baselga
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Review 1.  Nanoparticles as Physically- and Biochemically-Tuned Drug Formulations for Cancers Therapy.

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Review 2.  Nanomaterials for cancer therapy: current progress and perspectives.

Authors:  Zhe Cheng; Maoyu Li; Raja Dey; Yongheng Chen
Journal:  J Hematol Oncol       Date:  2021-05-31       Impact factor: 17.388

Review 3.  Nanoparticles for Cancer Therapy: Current Progress and Challenges.

Authors:  Shreelaxmi Gavas; Sameer Quazi; Tomasz M Karpiński
Journal:  Nanoscale Res Lett       Date:  2021-12-05       Impact factor: 4.703

Review 4.  A Nanoparticle's Journey to the Tumor: Strategies to Overcome First-Pass Metabolism and Their Limitations.

Authors:  Joshua J Milligan; Soumen Saha
Journal:  Cancers (Basel)       Date:  2022-03-29       Impact factor: 6.639

Review 5.  Current Progress in Cancer Treatment Using Nanomaterials.

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Review 6.  Nanomaterial-Based Drug Delivery Systems: A New Weapon for Cancer Immunotherapy.

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Review 7.  Role of Nanotechnology in Overcoming the Multidrug Resistance in Cancer Therapy: A Review.

Authors:  Suhail Ahmad Mir; Laraibah Hamid; Ghulam Nabi Bader; Ambreen Shoaib; Mohamed Rahamathulla; Mohammad Y Alshahrani; Prawez Alam; Faiyaz Shakeel
Journal:  Molecules       Date:  2022-10-05       Impact factor: 4.927

  7 in total

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