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Sains Malaysiana 52(11)(2023): 3223-3237
http://doi.org/10.17576/jsm-2023-5211-15
In silico Design and
Evaluation of Novel Cell Targeting Melittin-Interleukin-24 Fusion Protein: A
Potential Drug Candidate Against Breast Cancer
(Reka Bentuk in silico dan Penilaian Penyasaran Sel Baru Protein Gabungan Melitin-Interleukin-24: Calon Dadah Berpotensi Melawan Kanser Payudara)
HAFIZ MUHAMMAD REHMAN1,4, HAFIZ MUZZAMMEL REHMAN5,6,
NADEEM AHMED2, MUHAMMAD IMRAN
AMIRZADA3, SHAKIRA ASLAM1 & HAMID BASHIR1,*
1Centre for
Applied Molecular Biology (CAMB), 87-West Canal, Bank Road, University of the
Punjab, Lahore-53700, Pakistan
2Centre of excellence in
Molecular Biology (CEMB), 87-West Canal, Bank Road, University of the Punjab,
Lahore-53700, Pakistan
3Department of Pharmacy
COMSATS University, Islamabad Abbottabad, Pakistan
4University Institute of
Medical Laboratory Technology, Faculty of Allied Health Sciences, The
University of Lahore -54590 Pakistan
5School of Biochemistry and
Biotechnology University of the Punjab, Lahore-53700, Pakistan
6Department of Human Genetics
and Molecular Biology, University of Health Science, Lahore
Received: 13 December 2022/Accepted: 16 October 2023
Abstract
Fusion proteins are
designed to achieve new functionality or improved properties synergistically by
incorporating multiple protein domains into one complex. The fusion of two
genes to translate a recombinant protein for cancer treatment can enhance the bioactivity
of drug and can introduce novel drug candidate with wide range of applications
in pharmaceuticals and biotechnology. Interleukin-24 (IL-24) is a novel cancer
growth-suppressing and apoptosis inducing cytokine while melittin is a natural honeybee derived cationic
polypeptide having anti-tumor activity against breast cancer cells. The
current study was aimed to perform in silico design and analyses of a melittin-IL-24 fusion protein against breast cancer.
The amino acid sequences of the IL-24 and melittin peptide were used to design the fusion protein via a rigid linker. Using the
online softwares we predicted the secondary and
tertiary structures along with physicochemical properties of the designed
fusion protein. The validation and quality of the fusion protein was confirmed
by Rampage and ERRAT2. The top ranked structure from I-TASSER showed 18.1KD
molecular weight by ProtParam, quality factor of
94.152 by ERRAT and a valid structure by Ramachandran plot with 88.5% residues
in favoured region. The docking and simulation
studies were performed using ClusPro and Desmond
software. The quality, validity, interaction analysis and stability of the
fusion protein depicted a functional molecule. The in silico analysis finding and expression predicted value of 0.86 in E. coli on SOLUPROT tool suggest that the melittin-
IL-24 fusion protein can lead to develop a potent therapeutic drug against
breast cancer.
Keywords: Breast cancer; fusion
protein; interleukin 24; melittin; molecular docking
Abstrak
Protein gabungan telah direka bentuk untuk mencapai fungsi baharu atau sifat yang dipertingkatkan secara sinergi dengan menggabungkan berbilang domain
protein ke dalam satu kompleks. Gabungan dua gen untuk menterjemah protein rekombinan untuk rawatan kanser boleh meningkatkan bioaktiviti dadah dan boleh memperkenalkan calon dadah baharu dengan pelbagai pengaplikasian dalam farmaseutikal dan bioteknologi. Interleukin-24 (IL-24) ialah sitokin penekan pertumbuhan kanser baharu dan apoptosis manakala melitin ialah polipeptida kation perolehan lebah madu semula jadi yang mempunyai aktiviti anti-tumor terhadap sel kanser payudara. Kajian semasa ini bertujuan untuk menjalankan reka bentuk in silico dan analisis protein gabungan melitin-IL-24 terhadap kanser payudara. Jujukan asid amino IL-24 dan peptida melitin digunakan untuk mereka bentuk protein gabungan melalui penghubung tegar. Dengan menggunakan perisian atas talian,
kami meramalkan struktur sekunder dan tertiari bersama-sama dengan sifat fizikokimia reka bentuk protein gabungan. Pengesahan dan kualiti protein gabungan telah disahkan oleh Rampage dan ERRAT2. Struktur kedudukan teratas daripada I-TASSER menunjukkan berat molekul 18.1KD oleh ProtParam, faktor kualiti 94.152 oleh ERRAT dan struktur yang sahih oleh plot Ramachandran dengan 88.5% residu di kawasan yang digemari. Kajian dok dan simulasi dilakukan menggunakan perisian ClusPro dan Desmond. Kualiti, kesahan, analisis interaksi dan kestabilan protein gabungan menggambarkan molekul fungsian. Penemuan analisis in silico dan pengekspresan nilai ramalan 0.86 dalam E. coli pada perkakas SOLUPROT menunjukkan bahawa protein gabungan melitin-IL-24 boleh membawa kepada pembangunan ubat terapeutik poten terhadap kanser payudara.
Kata kunci: Dok molekul;
interleukin 24; kanser payudara; melitin; protein gabungan
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*Corresponding author; email: hamid.camb@pu.edu.pk
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