Avaliação da presença do Papilomavírus humano (HPV) em tumores de pulmão

AMARAL, Carolina Maria Medeiros Do

15 December 2015

Submitted by Fabio Sobreira Campos da Costa (fabio.sobreira@ufpe.br) on 2017-04-03T14:39:58Z No. of bitstreams: 2 license_rdf: 1232 bytes, checksum: 66e71c371cc565284e70f40736c94386 (MD5) Tese - Carolina Amaral (2).pdf: 3097271 bytes, checksum: a09eebe935773ec4b3446a95c4507f5c (MD5) / Made available in DSpace on 2017-04-03T14:39:58Z (GMT). No. of bitstreams: 2 license_rdf: 1232 bytes, checksum: 66e71c371cc565284e70f40736c94386 (MD5) Tese - Carolina Amaral (2).pdf: 3097271 bytes, checksum: a09eebe935773ec4b3446a95c4507f5c (MD5) Previous issue date: 2015-12-15 / FACEPE / Os Papilomavírus humano (HPV) infectam mucosas e epitélio contribuindo para o desenvolvimento de tumores benignos como também malignos. São amplamente conhecidos como causadores do câncer cervical, contudo, atualmente, vem apresentando evidências de associação com diversos outros tipos de canceres, como o câncer de pulmão. Sendo assim, o presente estudo avaliou a presença do DNA do HPV em tumores de pulmão de pacientes do Estado de Pernambuco bem como a expressão de suas oncoproteínas E6 e E7. Para isto, a detecção foi feita em amostras de tecidos de tumores frescos e parafinados de 63 pacientes. HPV estava presente em 52% das amostras, sendo detectados os tipos 16 e 18 com frequências de 81 e 19%, respectivamente. Quanto a presença do vírus nos diferentes tipos histológicos dos tumores, foi detectado HPV em 40% dos carcinomas escamosos, 33% dos adenocarcinomas, 18% dos carcinomas de células pequenas e 9% em carcinoma de células grandes. Através da técnica de imunohistoquimica detectou-se a presença das oncoproteinas virais E6 (anticorpo anti-HPV 16 e anti-HPV 18) e E7 (anticorpo anti-HPV 16 e anti-HPV 18) com frequências de 85 e 75%, respectivamente. Tal resultado confirma os resultados obtidos molecularmente quanto à presença do HPV e é sugestivo de que o vírus esteja em atividade nas células tumorais e provavelmente esteja desempenhando um papel na carcinogênese de pulmão. No entanto, mais estudos são necessários para se ter um maior esclarecimento sobre interação de E6 e E7 com proteínas celulares na tumorigenese pulmonar. / Small DNA viruses - Human Papillomavirus (HPV) - infect oral mucosa and the epthelium, which leads to the development of both benign and malign tumors. They are widely known as the principal causes of cervical cancer although currently there is evidence to show that they are associated with several other types of cancer, such as lung cancer. In the light of this, this study evaluated the presence of HPV in the tumors of lungs of patients from the State of Pernambuco, as well as the E6 and E7 oncoproteins expression. This involved carrying out the detection in tumor tissue samples that were fresh and paraffin-embedded and taken from 63 patients. HPV was found to be present in 52% of the samples, and types 16 and 18 were detected with frequencies of 81% and 19% respectively. With regard to the presence of the vírus in different histological types of tumors, HPV was detected in 40% of the squamous carcinomas, 33% of the adenocarcinomas, 18% of the small cell carcinomas and 9% in large cell carcinomas. The presence of the E6 (antibody anti-HPV 16 and anti-HPV 18) and E7 (antibody anti-HPV 16 and anti-HPV 18) oncoproteins was detected by means of the immunohistochemical technique and this confirmed the results obtained from a molecular analysis with regard to the presence of the virus and it is suggestive that the virus is active in tumor cells and is probably playing a role in lung carcinogenesis. However, further studies are required to have a clearer understanding of the interaction of E6 and E7 with the cell proteins in pulmonary tumorigenesis.

Câncer de pulmão

HPV

oncoproteína E6

oncoproteína E7

Lung cancer

HPV

E6 oncoprotein

E7 oncoprotein

Exploration de nouvelles voies thérapeutiques contre le cancer du col de l'utérus : approche combinée par adénovirus et ARN interférence / Adenovirus mediated RNA interference as new therapeutic tool against cervical cancer

Bonetta, Anaëlle

16 January 2013

Le cancer du col de l’utérus est le troisième cancer le plus fréquent chez la femme, dont l’agent étiologique majeur est l’infection par les papillomavirus humain (notamment HPV-16 et 18), qui sont de petits virus infectant les épithéliums muqueux et cutanés, et pouvant induire la formation de tumeurs. L’inducteur majeur du processus oncogène est le processus d’intégration des régions codantes pour les oncoprotéines E6 et E7, au sein de la cellule hôte suite à l’infection. Elles interférent avec le cycle cellulaire et induisent notamment l’immortalisation, voire la transformation des cellules. Les fonctions les plus connue de ces deux oncoprotéines sont la dégradation des suppresseurs de tumeur p53 et pRb, respectivement. Mon travail de thèse à consisté en la mise au point des vecteurs adénoviraux exprimant des miARN dirigés contre l’oncoprotéine E6. Exprimés in vitro ils induisent l’induction de la mort cellulaire par apoptose des cellules tumorales traitées, via l’activation de la voie de caspases, et in vivo permettent le ralentissement de la croissance de tumeurs xénogreffées à des souris Nude. De plus, la stratégie thérapeutique adénovirale a montré ses extensions possibles sur d’autres types de cancers HPV-positifs, mais également via l’expression de différentes moléculaires thérapeutiques, visant à empêcher l’interaction des oncoprotéines telles qu’E6 avec leurs partenaires cellulaires et ainsi les empêcher d’exercer les activités biologiques impliquées dans le développement de cancers. Pour finir, les adénovirus peuvent également être vu comme des outils d’extinction fonctionnels d’E6 et permettant d’étudier les répercutions sur d’autres processus cellulaires. / Cervical cancer is the third most common female cancer. Infection by human papillomavirus (mainly HPV-16 and 18), with tropisms for mucosal or cutaneous squamous surfaces, is the major etiological agent implicated in cancer and tumor development. After infection, the oncogenic process is triggered by integration of oncoproteins E6 and E7 coding regions into the host cell genome. After integration, these oncoproteins interfere with the cell cycle and induce immortalization and cellular transformation of normal cells. The best known function of these two oncoproteins is the degradation of tumors suppressors p53 and pRb respectively. My thesis project consisted in the development of adenoviral vectors expressing miRNA directed against E6 oncoprotein. Their in vitro expression resulted in cellular death by apoptosis of the treated tumor cells, and allowed reduction of tumor growth in vivo in nude mice xenografts. In addition, the adenoviral therapeutical strategy showed its possible extensions on other types of HPV-positive cancers, but also through the possible expression of different therapeutic molecules aimed at preventing the interaction of viral oncoproteins, such as E6, with their cellular partners. These abolished interactions prevent oncoproteins from exercising their biological activities implicated in the development of cancers. In conclusion, we can say that adenoviruses can also be seen as functional tools suppressing E6 and enabling to highlight the repercussions of its suppression on other cellular processes.

Papillomavirus

Cancer du col de l’utérus

Adénovirus

ARN interférence

Oncoprotéine E6

Thérapie génique

Phase préclinique

Knockdown

Papillomavirus

Cervical cancer

Adénovirus

RNA interference

E6 oncoprotein

Preclinical phase

Knockdown

572.8

616.99

571.9