Haneen Abuzaid
Apoferritin-Encapsulated Jerantinine A for Transferrin Receptor Targeting and Enhanced Selectivity in Breast Cancer Therapy
Abuzaid, Haneen; Abdelrazig, Salah; Ferreira, Lenny; Collins, Hilary M.; Kim, Dong Hyun; Lim, Kuan Hon; Kam, Toh Seok; Turyanska, Lyudmila; Bradshaw, Tracey D.
Authors
Salah Abdelrazig
Lenny Ferreira
Hilary M. Collins
DONG-HYUN KIM Dong-hyun.Kim@nottingham.ac.uk
Associate Professor
Kuan Hon Lim
Toh Seok Kam
Dr LYUDMILA TURYANSKA LYUDMILA.TURYANSKA@NOTTINGHAM.AC.UK
Associate Professor
Dr TRACEY BRADSHAW tracey.bradshaw@nottingham.ac.uk
Associate Professor
Contributors
Dr TRACEY BRADSHAW tracey.bradshaw@nottingham.ac.uk
Other
Abstract
The O-acetyl (or acetate) derivative of the Aspidosperma alkaloid Jerantinine A (JAa) elicits anti-tumor activity against cancer cell lines including mammary carcinoma cell lines irrespective of receptor status (0.14 < GI 50 < 0.38 μM), targeting microtubule dynamics. By exploiting breast cancer cells' upregulated transferrin receptor 1 (TfR1) expression and apoferritin (AFt) recognition, we sought to develop an AFt JAa-delivery vehicle to enhance tumor-targeting and reduce systemic toxicity. Optimizing pH-mediated reassembly, ∼120 JAa molecules were entrapped within AFt. Western blot and flow cytometry demonstrate TfR1 expression in cancer cells. Enhanced internalization of 5-carboxyfluorescein-conjugated human AFt in SKBR3 and MDA-MB-231 cancer cells is observed compared to MRC5 fibroblasts. Accordingly, AFt−JAa delivers significantly greater intracellular JAa levels to SKBR3 and MDA-MB-231 cells than naked JAa (0.2 μM) treatment alone. Compared to naked JAa (0.2 μM), AFt−JAa achieves enhanced growth inhibition (2.5−14-fold; <0.02 μM < GI 50 < 0.15 μM) in breast cancer cells; AFt−JAa treatment results in significantly reduced clonal survival, more profound cell cycle perturbation including G2/M arrest, greater reduction in cell numbers, and increased apoptosis compared to the naked agent (p < 0.01). Decreased PLK1 and Mcl-1 expression, together with the appearance of cleaved poly (ADP-ribose)-polymerase, corroborate the augmented potency of AFt−JAa. Hence, we demonstrate that AFt represents a biocompatible vehicle for targeted delivery of JAa, offering potential to minimize toxicity and enhance JAa activity in TfR1-expressing tumors.
Citation
Abuzaid, H., Abdelrazig, S., Ferreira, L., Collins, H. M., Kim, D. H., Lim, K. H., Kam, T. S., Turyanska, L., & Bradshaw, T. D. (2022). Apoferritin-Encapsulated Jerantinine A for Transferrin Receptor Targeting and Enhanced Selectivity in Breast Cancer Therapy. ACS Omega, 7(25), 21473–21482. https://doi.org/10.1021/acsomega.2c00997
Journal Article Type | Article |
---|---|
Acceptance Date | May 22, 2022 |
Online Publication Date | Jun 13, 2022 |
Publication Date | Jun 13, 2022 |
Deposit Date | Jun 13, 2022 |
Publicly Available Date | Jun 20, 2022 |
Journal | ACS Omega |
Electronic ISSN | 2470-1343 |
Publisher | American Chemical Society |
Peer Reviewed | Peer Reviewed |
Volume | 7 |
Issue | 25 |
Pages | 21473–21482 |
DOI | https://doi.org/10.1021/acsomega.2c00997 |
Keywords | General Chemical Engineering; General Chemistry |
Public URL | https://nottingham-repository.worktribe.com/output/8494404 |
Publisher URL | https://pubs.acs.org/doi/10.1021/acsomega.2c00997 |
Files
Acsomega.2c00997
(3.2 Mb)
PDF
Publisher Licence URL
https://creativecommons.org/licenses/by/4.0/
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