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Inhibition of HPV18 E6/E7 Protein-Expressing HeLa Cell Proliferation Using Optimized De Novo CRISPR/Cas9 Constructs Delivered by the LL-37 Peptide

Publish Year: 1403
Type: Journal paper
Language: English
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JR_JOMMID-12-4_004

Index date: 4 March 2025

Inhibition of HPV18 E6/E7 Protein-Expressing HeLa Cell Proliferation Using Optimized De Novo CRISPR/Cas9 Constructs Delivered by the LL-37 Peptide abstract

Introduction: CRISPR/Cas-mediated gene editing has emerged as a transformative therapeutic modality for targeting oncogenic pathways in cancer. This technology enables precise disruption of oncogenic processes, such as tumor cell migration and invasion, and facilitates targeted tumor eradication. This study employed CRISPR/Cas9-mediated genome editing to disrupt the HPV18 E6 and E7 oncogenes, which are critical drivers of tumorigenesis in HPV-associated cancers. Methods: Optimized single-guide RNA (sgRNA) sequences were designed to target the HPV18 E6 and E7 oncogenes, along with the p105 promoter region, for CRISPR/Cas9-mediated genome editing. The sgRNA sequences were cloned into CRISPR/Cas9 expression vectors. HPV18-positive HeLa cells, were transfected in vitro with the recombinant vectors to assess gene editing efficiency. For the in vivo evaluation, C57BL/6 mice bearing HeLa-derived tumors received intravenous injections of LL-37 peptide-complexed recombinant vectors. The therapeutic efficacy of this approach was quantitatively compared to cisplatin treatment. Results: The dual E6/E7-targeted group exhibited a statistically significant reduction in tumor volume compared to all other groups, including the single E6-targeted group, the single E7-targeted group, the cisplatin-treated group, and the untreated control group (P < 0.05). LL-37 peptide demonstrated efficient delivery of CRISPR/Cas9 vectors into HeLa tumor cells, with an optimal nitrogen-to-phosphate (N/P) ratio of 5: 1, achieving high transfection efficiency without systemic toxicity. Conclusion: These findings establish CRISPR/Cas9-mediated gene editing as a potent therapeutic strategy for HPV-associated tumors and highlight LL-37 as a promising non-viral delivery platform for CRISPR/Cas9 constructs. This study is the first to demonstrate the in vivo efficacy of multiplexed sgRNA delivery targeting HPV18 oncogenes in a preclinical model.

Inhibition of HPV18 E6/E7 Protein-Expressing HeLa Cell Proliferation Using Optimized De Novo CRISPR/Cas9 Constructs Delivered by the LL-37 Peptide Keywords:

Inhibition of HPV18 E6/E7 Protein-Expressing HeLa Cell Proliferation Using Optimized De Novo CRISPR/Cas9 Constructs Delivered by the LL-37 Peptide authors

Niloofar Khairkhah

Cellular and Molecular Research Center, Institute for Prevention of Non-Communicable Diseases, Qazvin University of Medical Sciences, Qazvin, Iran

Azam Bolhassani

Department of Hepatitis, AIDS and Blood-borne Diseases, Pasteur Institute of Iran, Tehran, Iran, Pasteur Institute of Iran, Tehran, Iran

Reza Najafipour

Cellular and Molecular Research Center, Institute for Prevention of Non-Communicable Diseases, Qazvin University of Medical Sciences, Qazvin, Iran; Genetics Research Center, University of Social Welfare and Rehabilitation Sciences, Tehran, Iran

Ali Namvar

Blood Diseases Research Center (BDRC), Iranian Comprehensive Hemophilia Care Center, Iran University of Medical Sciences (IUMS), Tehran, Iran

Alireza Milani

Department of Hepatitis, AIDS and Blood-borne Diseases, Pasteur Institute of Iran, Tehran, Iran, Pasteur Institute of Iran, Tehran, Iran

Elnaz Agi

Blood Diseases Research Center (BDRC), Iranian Comprehensive Hemophilia Care Center, Iran University of Medical Sciences (IUMS), Tehran, Iran

Ali Anvar

Blood Diseases Research Center (BDRC), Iranian Comprehensive Hemophilia Care Center, Iran University of Medical Sciences (IUMS), Tehran, Iran

Mohammad Sadeqh Khosravy

WHO Collaborating Center for Reference and Research on Rabies, Pasteur Institute of Iran, Tehran, Iran

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Bruni LAG, Serrano B, Mena M, Collado JJ, Gómez D, ...
Santacroce L, Di Cosola M, Bottalico L, Topi S, Charitos ...
Peng S, Ferrall L, Gaillard S, Wang C, Chi WY, ...
Bulk S, Berkhof J, Rozendaal L, Daalmeijer N, Gök M, ...
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Pal A, Kundu R. Human papillomavirus E۶ and E۷: the ...
Ghaemi A, Bagheri E, Abnous K, Taghdisi SM, Ramezani M, ...
Zhen S, Hua L, Takahashi Y, Narita S, Liu YH, ...
Jubair L, Fallaha S, McMillan NA. Systemic delivery of CRISPR/Cas۹ ...
Chen Y, Jiang H, Wang T, He D, Tian R, ...
Labun K, Montague TG, Krause M, Torres Cleuren YN, Tjeldnes ...
Bae S, Park J, Kim JS. Cas-OFFinder: a fast and ...
Heigwer F, Kerr G, Boutros M. E-CRISP: fast CRISPR target ...
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Sandgren S, Wittrup A, Cheng F, Jönsson M, Eklund E, ...
Khairkhah N, Bolhassani A, Agi E, Namvar A, Nikyar A. ...
Aloul KM, Nielsen JE, Defensor EB, Lin JS, Fortkort JA, ...
Büchau AS, Morizane S, Trowbridge J, Schauber J, Kotol P, ...
Yang B, Good D, Mosaiab T, Liu W, Ni G, ...
Khairkhah N, Bolhassani A, Rajaei F, Najafipour R. Systemic delivery ...
Xiang X, Li C, Chen X, Dou H, Li Y, ...
Fu Y, Foden JA, Khayter C, Maeder ML, Reyon D, ...
Langmead B, Trapnell C, Pop M, Salzberg SL. Ultrafast and ...
Li H, Durbin R. Fast and accurate short read alignment ...
Sadeghian I, Heidari R, Sadeghian S, Raee MJ, Negahdaripour M. ...
Tripathi S, Wang G, White M, Qi L, Taubenberger J, ...
Currie SM, Findlay EG, McHugh BJ, Mackellar A, Man T, ...
Moret I, Peris JE, Guillem VM, Benet M, Revert F, ...
Sadeghian F, Hosseinkhani S, Alizadeh A, Hatefi A. Design, engineering ...
Masters JR. HeLa cells ۵۰ years on: the good, the ...
Søndergaard JN, Geng K, Sommerauer C, Atanasoai I, Yin X, ...
Guschin DY, Waite AJ, Katibah GE, Miller JC, Holmes MC, ...
Skelton D, Satake N, Kohn D. The enhanced green fluorescent ...
Ansari AM, Ahmed AK, Matsangos AE, Lay F, Born LJ, ...
Comune M, Rai A, Chereddy KK, Pinto S, Aday S, ...
Nikyar A, Bolhassani A, Rouhollah F, Heshmati M. In vitro ...
Jinek M, Chylinski K, Fonfara I, Hauer M, Doudna JA, ...
Rasul MF, Hussen BM, Salihi A, Ismael BS, Jalal PJ, ...
Moreno-Angarita A, Aragón CC, Tobón GJ. Cathelicidin LL-۳۷: A new ...
Zhang X, Oglęcka K, Sandgren S, Belting M, Esbjörner EK, ...
Chamilos G, Gregorio J, Meller S, Lande R, Kontoyiannis DP, ...
Yoshiba T, Saga Y, Urabe M, Uchibor R, Matsubara S, ...
Inturi R, Jemth P. CRISPR/Cas۹-based inactivation of human papillomavirus oncogenes ...
Noroozi Z, Shamsara M, Valipour E, Esfandyari S, Ehghaghi A, ...
Ehrke-Schulz E, Heinemann S, Schulte L, Schiwon M, Ehrhardt A. ...
Taha EA, Lee J, Hotta A. Delivery of CRISPR-Cas tools ...
Ye J, Liu E, Yu Z, Pei X, Chen S, ...
Henzler-Wildman KA, Martinez GV, Brown MF, Ramamoorthy A. Perturbation of ...
Wu WK, Wang G, Coffelt SB, Betancourt AM, Lee CW, ...
Kuroda K, Okumura K, Isogai H, Isogai E. The human ...
Coffelt SB, Waterman RS, Florez L, Bentrup KHZ, Zwezdaryk KJ, ...
Weber G, Chamorro CI, Granath F, Liljegren A, Zreika S, ...
Zhou X, Jiang W, Liu Z, Liu S, Liang X. ...
Jiang P, Yue Y. Human papillomavirus oncoproteins and apoptosis. Experimental ...
Galus R, Wlodarski P, Wlodarski K. Fluvastatin increases heterotopically induced ...
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