Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics

The production of short anticancer peptides in recombinant form is an alternative method for costly chemical manufacturing. However, the limitations of host toxicity, bioactivity and column purification have impaired production in mass quantities. In this study, short cationic peptides were produced...

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Autores principales: Rothan, Hussin A., Ambikabothy, Jamunaa, Abdulrahman, Ammar Y., Bahrani, Hirbod, Golpich, Mojtaba, Amini, Elham, A. Rahman, Noorsaadah, Teoh, Teow Chong, Mohamed, Zulqarnain, Yusof, Rohana
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4587966/
https://www.ncbi.nlm.nih.gov/pubmed/26418816
http://dx.doi.org/10.1371/journal.pone.0139248
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author Rothan, Hussin A.
Ambikabothy, Jamunaa
Abdulrahman, Ammar Y.
Bahrani, Hirbod
Golpich, Mojtaba
Amini, Elham
A. Rahman, Noorsaadah
Teoh, Teow Chong
Mohamed, Zulqarnain
Yusof, Rohana
author_facet Rothan, Hussin A.
Ambikabothy, Jamunaa
Abdulrahman, Ammar Y.
Bahrani, Hirbod
Golpich, Mojtaba
Amini, Elham
A. Rahman, Noorsaadah
Teoh, Teow Chong
Mohamed, Zulqarnain
Yusof, Rohana
author_sort Rothan, Hussin A.
collection PubMed
description The production of short anticancer peptides in recombinant form is an alternative method for costly chemical manufacturing. However, the limitations of host toxicity, bioactivity and column purification have impaired production in mass quantities. In this study, short cationic peptides were produced in aggregated inclusion bodies by double fusion with a central protein that has anti-cancer activity. The anticancer peptides Tachiplicin I (TACH) and Latarcin 1 (LATA) were fused with the N- and C-terminus of the MAP30 protein, respectively. We successfully produced the recombinant TACH-MAP30-LATA protein and MAP30 alone in E. coli that represented 59% and 68% of the inclusion bodies. The purified form of the inclusion bodies was prepared by eliminating host cell proteins through multiple washing steps and semi-solubilization in alkaline buffer. The purified active protein was recovered by inclusive solubilization at pH 12.5 in the presence of 2 M urea and refolded in alkaline buffer containing oxides and reduced glutathione. The peptide-fusion protein showed lower CC(50) values against cancer cells (HepG2, 0.35±0.1 μM and MCF-7, 0.58±0.1 μM) compared with normal cells (WRL68, 1.83±0.2 μM and ARPE19, 2.5±0.1 μM) with outstanding activity compared with its individual components. The presence of the short peptides facilitated the entry of the peptide fusion protein into cancer cells (1.8 to 2.2-fold) compared with MAP30 alone through direct interaction with the cell membrane. The cancer chemotherapy agent doxorubicin showed higher efficiency and selectivity against cancer cells in combination with the peptide- fusion protein. This study provides new data on the mass production of short anticancer peptides as inclusion bodies in E. coli by fusion with a central protein that has similar activity. The product was biologically active against cancer cells compared with normal cells and enhanced the activity and selective delivery of an anticancer chemotherapy agent.
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spelling pubmed-45879662015-10-02 Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics Rothan, Hussin A. Ambikabothy, Jamunaa Abdulrahman, Ammar Y. Bahrani, Hirbod Golpich, Mojtaba Amini, Elham A. Rahman, Noorsaadah Teoh, Teow Chong Mohamed, Zulqarnain Yusof, Rohana PLoS One Research Article The production of short anticancer peptides in recombinant form is an alternative method for costly chemical manufacturing. However, the limitations of host toxicity, bioactivity and column purification have impaired production in mass quantities. In this study, short cationic peptides were produced in aggregated inclusion bodies by double fusion with a central protein that has anti-cancer activity. The anticancer peptides Tachiplicin I (TACH) and Latarcin 1 (LATA) were fused with the N- and C-terminus of the MAP30 protein, respectively. We successfully produced the recombinant TACH-MAP30-LATA protein and MAP30 alone in E. coli that represented 59% and 68% of the inclusion bodies. The purified form of the inclusion bodies was prepared by eliminating host cell proteins through multiple washing steps and semi-solubilization in alkaline buffer. The purified active protein was recovered by inclusive solubilization at pH 12.5 in the presence of 2 M urea and refolded in alkaline buffer containing oxides and reduced glutathione. The peptide-fusion protein showed lower CC(50) values against cancer cells (HepG2, 0.35±0.1 μM and MCF-7, 0.58±0.1 μM) compared with normal cells (WRL68, 1.83±0.2 μM and ARPE19, 2.5±0.1 μM) with outstanding activity compared with its individual components. The presence of the short peptides facilitated the entry of the peptide fusion protein into cancer cells (1.8 to 2.2-fold) compared with MAP30 alone through direct interaction with the cell membrane. The cancer chemotherapy agent doxorubicin showed higher efficiency and selectivity against cancer cells in combination with the peptide- fusion protein. This study provides new data on the mass production of short anticancer peptides as inclusion bodies in E. coli by fusion with a central protein that has similar activity. The product was biologically active against cancer cells compared with normal cells and enhanced the activity and selective delivery of an anticancer chemotherapy agent. Public Library of Science 2015-09-29 /pmc/articles/PMC4587966/ /pubmed/26418816 http://dx.doi.org/10.1371/journal.pone.0139248 Text en © 2015 Rothan et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Rothan, Hussin A.
Ambikabothy, Jamunaa
Abdulrahman, Ammar Y.
Bahrani, Hirbod
Golpich, Mojtaba
Amini, Elham
A. Rahman, Noorsaadah
Teoh, Teow Chong
Mohamed, Zulqarnain
Yusof, Rohana
Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title_full Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title_fullStr Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title_full_unstemmed Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title_short Scalable Production of Recombinant Membrane Active Peptides and Its Potential as a Complementary Adjunct to Conventional Chemotherapeutics
title_sort scalable production of recombinant membrane active peptides and its potential as a complementary adjunct to conventional chemotherapeutics
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4587966/
https://www.ncbi.nlm.nih.gov/pubmed/26418816
http://dx.doi.org/10.1371/journal.pone.0139248
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