TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells

TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells

Induced pluripotent stem cell (iPSC) holds a magnificent place in the medical revolution. Its emergence is expected to instigate development of novel therapies for regenerative medicine and treatment of malignant diseases. Moreover, iPSC usage also resolved a long-time ethical controversy on the usa...

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Main Authors: Ubashini Vijakumaran, Fazlina Nordin, Zariyantey Abd Hamid, Maha Abdullah, Gee, Jun Tye
Format: Article
Language:English
Published: Penerbit Universiti Kebangsaan Malaysia 2022
Online Access:http://journalarticle.ukm.my/19146/1/20.pdf
http://journalarticle.ukm.my/19146/
https://www.ukm.my/jsm/malay_journals/jilid51bil2_2022/KandunganJilid51Bil2_2022.html
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Institution: Universiti Kebangsaan Malaysia
Language: English
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spelling my-ukm.journal.191462022-08-01T03:26:35Z http://journalarticle.ukm.my/19146/ TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells Ubashini Vijakumaran, Fazlina Nordin, Zariyantey Abd Hamid, Maha Abdullah, Gee, Jun Tye Induced pluripotent stem cell (iPSC) holds a magnificent place in the medical revolution. Its emergence is expected to instigate development of novel therapies for regenerative medicine and treatment of malignant diseases. Moreover, iPSC usage also resolved a long-time ethical controversy on the usage of the embryo as a pluripotent stem cells source. Since Yamanaka’s iPSC discovery in 2006, several pieces of research have proven that the enforced expression of transcription factors Oct-3/4, KLF4, and Sox2 can induce the reprogramming of previously differentiated cells, to generate iPSC. However, the conventional method using viral vectors leads to genetic modification due to exogene integration and subsequently tumorigenicity, which is unsafe for clinical application. Therefore, our study utilised an improved novel protein transduction domain, trans-activator of transcription kappa (TAT), a synthetic TAT-HIV to deliver these transcription factors gene as an alternative method for iPSC generation via non-viral reprogramming. With this new strategy, we have established a stable clone of 293T cells expressing TATκ fusion proteins (TATκ-GFP, TATκ-KLF4, TATκ-Sox2, and TATκ-Oct-3/4) that expresses and secretes their respective cloned reprogramming proteins. These stable clones successfully transduced our target cell (U937) monocyte cell line. TATκ-GFP, a marker protein and fusion proteins TATκ-KLF4, TATκ-Sox2, and TATκ-Oct-3/4 transduced the targeted (U937) monocyte cell line, proving that this novel TATκ possesses an ability to translocate across the cell membrane. Morphological changes were successfully observed in U937 cells after 20 days of transduction, however the presence of bonifide iPSC colonies were unable to be elicited. This might be due to the incomplete reprogramming or insufficient duration of protein transduction to generate iPSC cells. Penerbit Universiti Kebangsaan Malaysia 2022-02 Article PeerReviewed application/pdf en http://journalarticle.ukm.my/19146/1/20.pdf Ubashini Vijakumaran, and Fazlina Nordin, and Zariyantey Abd Hamid, and Maha Abdullah, and Gee, Jun Tye (2022) TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells. Sains Malaysiana, 51 (2). pp. 567-576. ISSN 0126-6039 https://www.ukm.my/jsm/malay_journals/jilid51bil2_2022/KandunganJilid51Bil2_2022.html
institution Universiti Kebangsaan Malaysia
building Tun Sri Lanang Library
collection Institutional Repository
continent Asia
country Malaysia
content_provider Universiti Kebangsaan Malaysia
content_source UKM Journal Article Repository
url_provider http://journalarticle.ukm.my/
language English
description Induced pluripotent stem cell (iPSC) holds a magnificent place in the medical revolution. Its emergence is expected to instigate development of novel therapies for regenerative medicine and treatment of malignant diseases. Moreover, iPSC usage also resolved a long-time ethical controversy on the usage of the embryo as a pluripotent stem cells source. Since Yamanaka’s iPSC discovery in 2006, several pieces of research have proven that the enforced expression of transcription factors Oct-3/4, KLF4, and Sox2 can induce the reprogramming of previously differentiated cells, to generate iPSC. However, the conventional method using viral vectors leads to genetic modification due to exogene integration and subsequently tumorigenicity, which is unsafe for clinical application. Therefore, our study utilised an improved novel protein transduction domain, trans-activator of transcription kappa (TAT), a synthetic TAT-HIV to deliver these transcription factors gene as an alternative method for iPSC generation via non-viral reprogramming. With this new strategy, we have established a stable clone of 293T cells expressing TATκ fusion proteins (TATκ-GFP, TATκ-KLF4, TATκ-Sox2, and TATκ-Oct-3/4) that expresses and secretes their respective cloned reprogramming proteins. These stable clones successfully transduced our target cell (U937) monocyte cell line. TATκ-GFP, a marker protein and fusion proteins TATκ-KLF4, TATκ-Sox2, and TATκ-Oct-3/4 transduced the targeted (U937) monocyte cell line, proving that this novel TATκ possesses an ability to translocate across the cell membrane. Morphological changes were successfully observed in U937 cells after 20 days of transduction, however the presence of bonifide iPSC colonies were unable to be elicited. This might be due to the incomplete reprogramming or insufficient duration of protein transduction to generate iPSC cells.
format Article
author Ubashini Vijakumaran,
Fazlina Nordin,
Zariyantey Abd Hamid,
Maha Abdullah,
Gee, Jun Tye
spellingShingle Ubashini Vijakumaran,
Fazlina Nordin,
Zariyantey Abd Hamid,
Maha Abdullah,
Gee, Jun Tye
TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
author_facet Ubashini Vijakumaran,
Fazlina Nordin,
Zariyantey Abd Hamid,
Maha Abdullah,
Gee, Jun Tye
author_sort Ubashini Vijakumaran,
title TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
title_short TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
title_full TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
title_fullStr TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
title_full_unstemmed TAT Kappa (TATK) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
title_sort tat kappa (tatk) : a novel cell penetrating peptide for delivery of pluripotent proteins into target cells
publisher Penerbit Universiti Kebangsaan Malaysia
publishDate 2022
url http://journalarticle.ukm.my/19146/1/20.pdf
http://journalarticle.ukm.my/19146/
https://www.ukm.my/jsm/malay_journals/jilid51bil2_2022/KandunganJilid51Bil2_2022.html
_version_ 1740826816815300608

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