JNCI: Journal of the National Cancer Institute
 2009
DOI: 10.1093/jnci/djp106
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Concatenated Multitype L2 Fusion Proteins as Candidate Prophylactic Pan-Human Papillomavirus Vaccines

Subhashini Jagu1,
Balasubramanyam Karanam2,
Ratish Gambhira3
et al.

Abstract: BackgroundVaccination with minor capsid protein L2 induces antibodies that cross-neutralize diverse papillomavirus types. However, neutralizing antibody titers against the papillomavirus type from which the L2 vaccine was derived are generally higher than the titers against heterologous types, which could limit effectiveness against heterologous types. We hypothesized that vaccination with concatenated multitype L2 fusion proteins derived from known cross-protective epitopes of several divergent human papillom… Show more

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Cited by 141 publications
(181 citation statements)
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References 59 publications
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“…Вследствие низкой иммуногенности белка L2 в естественно протекающей инфекции анти-тел против него не возникает вовсе [6]. Однако N-конец белка L2 содержит консервативные эпитопы, к которым возможно образование нейтрализующих антител [14,20,33]. В литера-туре описаны успешные попытки повышения иммуногенности N-конца молекулы L2 путем слияния в одном белке N-концов белка L2 сразу нескольких штаммов [20,21,22,24].…”
Section: Discussionunclassified
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Human Papilloma Virus Immunogen Creation on the Base of Chimeric Recombinant Protein L2e7

Malakhov
1
,
Al-Shehadat
2
,
Duckhovlinov
3
et al. 2017
Russian Journal of Infection and Immunity
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0
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“…Вследствие низкой иммуногенности белка L2 в естественно протекающей инфекции анти-тел против него не возникает вовсе [6]. Однако N-конец белка L2 содержит консервативные эпитопы, к которым возможно образование нейтрализующих антител [14,20,33]. В литера-туре описаны успешные попытки повышения иммуногенности N-конца молекулы L2 путем слияния в одном белке N-концов белка L2 сразу нескольких штаммов [20,21,22,24].…”
Section: Discussionunclassified
“…Некорректное взаи-модействие между остатками цистеина фрагмен-тов L2 и остатками цистеина Е7 предполагается, исходя из-за анализа литературы. Рекомбинант-ный белок, состоящий из пяти слитых N-концов белков L2 различных штаммов вируса, успешно ренатурировался одноступенчатым диализом против PBS [20], то же самое относится и к Пен-тариксу, молекуле, состоящей из 5 слитых вместе копий Е7 различных штаммов вируса папилло-мы человека [41]. Однако в случае слитых вме-сте белков L2 и E7 (например, рекомбинантного белка L2E6E7 [12], вакцины Ta-CIN, состоящей из слитых L2, E6 и E7 ВПЧ-16 [25], а также реком-бинантного белка, состоящего из L2 и E7 ВПЧ-6 [38]), в работах упоминается очистка белка в вос-станавливающих условиях.…”
Section: Discussionunclassified
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Human Papilloma Virus Immunogen Creation on the Base of Chimeric Recombinant Protein L2e7

Malakhov
1
,
Al-Shehadat
2
,
Duckhovlinov
3
et al. 2017
Russian Journal of Infection and Immunity
0
0
0
0
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“…This polymeric L2 approach gives rise to antisera, that neutralize at higher titers, not only the types included in the multimeric immunogen but also other types. So, immunization against L2 could be a candidate prophylactic pan-human papillomaviruses vaccine (Alphs et al, 2008;Jagu et al, 2009 …”
Section: Prophylactic Vaccines To Prevent Hpv Infectionmentioning
confidence: 99%

Human Papillomavirus and Related Diseases - From Bench to Bedside - A Clinical Perspective

Broeck1
2012
7
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“…Although natural infection and immunisation with L1/L2 VLPs fails to elicit anti-L2 antibody responses, vaccination with bacterially expressed L2 protein or peptides derived from L2, results in the production of neutralising antibodies that are protective in animal models. [50][51][52] Studies demonstrate that L2 is poorly exposed in native HPV virions, 53 but 1 or more L2 neutralising epitopes [54][55][56] are exposed when the HPV capsid undergoes a conformational change upon binding to its cellular receptors.…”
Section: Hpv L2 Minor Capsid Protein Vaccinesmentioning
confidence: 99%

EUROGIN 2008 roadmap on cervical cancer prevention

Franceschi
1
,
Cuzick
2
,
Herrero
3
et al. 2009
Intl Journal of Cancer
37
0
34
0
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