How Azanucleosides Affect Myeloid Cell Fate

Stein, Anna, Platzbecker, Uwe, Cross, Michael

27 February 2024

The azanucleosides decitabine and azacytidine are used widely in the treatment of myeloid neoplasia and increasingly in the context of combination therapies. Although they were long regarded as being largely interchangeable in their function as hypomethylating agents, the azanucleosides actually have different mechanisms of action; decitabine interferes primarily with the methylation of DNA and azacytidine with that of RNA. Here, we examine the role of DNA methylation in the lineage commitment of stem cells during normal hematopoiesis and consider how mutations in epigenetic regulators such as DNMT3A and TET2 can lead to clonal expansion and subsequent neoplastic progression. We also consider why the efficacy of azanucleoside treatment is not limited to neoplasias carrying mutations in epigenetic regulators. Finally, we summarise recent data describing a role for azacytidine-sensitive RNA methylation in lineage commitment and in the cellular response to stress. By summarising and interpreting evidence for azanucleoside involvement in a range of cellular processes, our review is intended to illustrate the need to consider multiple modes of action in the design and stratification of future combination therapies.

info:eu-repo/classification/ddc/610

ddc:610

Investigation of Altered Cell-Cell Interactions and Signaling Mechanisms in <i>Drosophila</i> Tumor Models

Waghmare, Indrayani

08 September 2016

No description available.

Biology

Identification of the presence and activity of the JAK-STAT pathway in canine solid tumors

Fagan, Erin A.

22 May 2017

Background: The JAK-STAT pathway is a cellular signaling pathway, which acts normally in humans and animals in the control of multiple important functions. Dysregulation of this pathway has been identified in human cancers, as well as a limited number of veterinary cancers. Objectives: The aims of this study were to identify the presence and tentative activity of components of the JAK-STAT pathway in selected canine tumors. Methods: Formalin-fixed, paraffin-embedded samples from mast cell tumors (MCT), hemangiosarcomas (HSA), thyroid carcinomas, and apocrine gland anal sac adenocarcinomas (AGASACA) were obtained from the Diagnostic Histopathology Laboratory at the Virginia Maryland College of Veterinary Medicine. Immunohistochemistry was performed to evaluate protein levels of JAK1, phospho-JAK1, JAK2, phospho-JAK2, STAT3, and phospho-STAT3. Signalment, treatment information, and survival information was obtained from the medical record for each case. Results: Tumor samples were scored for percent positive neoplastic cells. Positive staining was seen for all antibodies in all tumor types, with expression of JAK1, STAT3, and pSTAT3 being highest overall for all tumor types. Significant associations were seen between JAK1 and survival time in MCT (p = 0.03), pJAK1 and survival time in HSA (p = 0.009) and MCT (p = 0.04), and pSTAT3 and metastasis in MCT (p = 0.0008). Conclusions: The finding of positive staining for the components of the JAK-STAT pathway in the tumor samples evaluated indicates presence and tentative activity of this pathway in the studied cancers. Further study of JAK1, pJAK1, and pSTAT3 should be pursued to evaluate their potential as therapeutic targets. / MS / The JAK-STAT pathway is a cellular signaling pathway which acts in humans and animals to control functions, such as development of the immune system, and development of the mammary glands during pregnancy. This pathway can become dysregulated, and contribute to development of cancer in both humans and animals. Development of cancer drugs that can target this pathway when dysregulated may aid in controlling further growth of spread of cancer, and may help to prolong survival in patients affected. In our study, four different cancer types were investigated in dogs for the presence and activity of components of the JAK-STAT pathway. Evidence of presence and activity was identified in the cancers evaluated, suggesting that more work should be done to determine if the JAK-STAT pathway is activated in other canine tumor types, and whether the pathway can be targeted as a cancer treatment.

JAK-STAT

canine

hemangiosarcoma

mast cell tumor

thyroid carcinoma

apocrine gland anal sac adenocarcinoma

neoplasia

Eicosapentaenoic acid free fatty acid prevents and suppresses colonic neoplasia in colitis-associated colorectal cancer acting on Notch signaling and gut microbiota

Piazzi, G., D'Argenio, G., Prossomariti, A., Lembo, V., Mazzone, G., Candela, M., Biagi, E., Brigidi, P., Vitaglione, P., Fogliano, V., D'Angelo, L., Fazio, C., Munarini, A., Belluzzi, A., Ceccarelli, C., Chieco, P., Balbi, T., Loadman, Paul, Hull, M.A., Romano, M., Bazzoli, F., Ricciardiello, L.

28 March 2014

No / Inflammatory bowel diseases are associated with increased risk of developing colitis-associated colorectal cancer (CAC). Epidemiological data show that the consumption of ω-3 polyunsaturated fatty acids (ω-3 PUFAs) decreases the risk of sporadic colorectal cancer (CRC). Importantly, recent data have shown that eicosapentaenoic acid-free fatty acid (EPA-FFA) reduces polyp formation and growth in models of familial adenomatous polyposis. However, the effects of dietary EPA-FFA are unknown in CAC. We tested the effectiveness of substituting EPA-FFA, for other dietary fats, in preventing inflammation and cancer in the AOM-DSS model of CAC. The AOM-DSS protocols were designed to evaluate the effect of EPA-FFA on both initiation and promotion of carcinogenesis. We found that EPA-FFA diet strongly decreased tumor multiplicity, incidence and maximum tumor size in the promotion and initiation arms. Moreover EPA–FFA, in particular in the initiation arm, led to reduced cell proliferation and nuclear β-catenin expression, whilst it increased apoptosis. In both arms, EPA-FFA treatment led to increased membrane switch from ω-6 to ω-3 PUFAs and a concomitant reduction in PGE2 production. We observed no significant changes in intestinal inflammation between EPA-FFA treated arms and AOM-DSS controls. Importantly, we found that EPA-FFA treatment restored the loss of Notch signaling found in the AOM-DSS control and resulted in the enrichment of Lactobacillus species in the gut microbiota. Taken together, our data suggest that EPA-FFA is an excellent candidate for CRC chemoprevention in CAC.

Eicosapentaenoic acid

Free fatty acid

FFA

Colonic neoplasia

Colorectal cancer

Notch signalling

Gut microbiota

Detecção e rastreamento de mutações no proto-oncogene RET em pacientes com neoplasia endócrina múltipla tipo 2 por meio de eletroforese em gel sensível à conformação / RET proto-oncogene mutations screening and detection in patients with multiple endocrine neoplasia type 2 using conformation sensitive gel electrophoresis

Santos, Marcelo Augusto Cortina Gonçalves dos

10 April 2007

A neoplasia endócrina múltipla tipo 2 (NEM-2) é uma síndrome tumoral herdada por mutações germinativas no proto-oncogene RET (RET) e transmitida por herança autossômica dominante. Atualmente, a indicação de tireoidectomia total preventiva é recomendada a indivíduos portadores de mutações no RET. Analisamos a aplicação do método Eletroforese em Gel Sensível à Conformação (CSGE) no rastreamento de mutações hot-spots do RET. Sete famílias com NEM-2 foram rastreadas pelo CSGE, seqüenciamento gênico e análise do Polimorfismo Conformacional de Cadeia Simples (SSCP). Usando o CSGE e SSCP, identificamos cinco das seis (83,3%) mutações verificadas pelo seqüenciamento: Cys620Arg, Cys634Arg, Cys634Tyr, Val648Ile e Met918Thr. Foram analisados 128 amplicons englobando mutações hot-spots do RET e 116 dentre 128 (90.6%) concordaram com o seqüenciamento genético. Os polimorfismos 691 e 769 também foram documentados pelo CSGE e SSCP. Os dados obtidos por CSGE e SSCP foram totalmente (100%) concordantes. O CSGE revelou ser metodologia sensível, rápida, fácil de ser executada e de baixo custo na detecção de mutações nos códons 620, 634, 648, e 918, as quais constituem grande maioria (~95%) dos pacientes com NEM-2. Quanto à mutação Val804Met (prevalência na população inferior a 3%), o método necessita ser otimizado. Concluímos que o CSGE é uma metodologia efetiva para o rastreamento de mutações que mais freqüentemente ocorrem no RET como causadora de NEM-2. / Multiple endocrine neoplasia type 2 (MEN2) is an autosomal dominant inherited tumor syndrome caused by activating germline mutations in RET proto-oncogene (RET). Presently, the prophylactic total thyroidectomy is recommended to all RET mutations carriers. Here we tested the Conformation Sensitive Gel Electrophoresis (CSGE) as a screening method for the RET hot-spot mutations. Seven MEN2 families were studied by CSGE, as well as by Single Strand Conformational Polymorphism (SSCP) and direct sequencing analysis. Using CSGE and SSCP, we were able to detect five out of the six (83.3%) RET mutations verified by direct sequencing analysis: Cys620Arg, Cys634Arg, Cys634Tyr, Val648Ile and Met918Thr. RET polymorphisms 691 and 769 were verified by CSGE and SSCP. In our sample, data obtained using CSGE were fully concordant (100%) with SSCP findings. Thus, CSGE showed to be a sensitive, fast, low-cost, and ease procedure to detect RET mutations in codons 620, 634, 648, and 918 which are reported as the most prevalent RET variants (~95%) in large MEN2 series. As to the Val804Met mutation (prevalence in the population lower than 3%), this method still needs to be optimized. We concluded that CSGE is an effective screening method for the most frequent RET hot-spot disease-causing mutations.

Carcinoma medular/genética

DNA mutational analyses/methods

Electrophoresis/methods

Eletroforese/métodos

Medullary carcinoma/genetic

Mutação/genética

Mutation/genetic

Neoplasias da tireóide/diagnóstico

Polymerase chain reaction/methods

Proto-oncogene/genetic

Proto-oncogenes/genética

Thyroid neoplasia/diagnosis

Detecção e rastreamento de mutações no proto-oncogene RET em pacientes com neoplasia endócrina múltipla tipo 2 por meio de eletroforese em gel sensível à conformação / RET proto-oncogene mutations screening and detection in patients with multiple endocrine neoplasia type 2 using conformation sensitive gel electrophoresis

Marcelo Augusto Cortina Gonçalves dos Santos

10 April 2007

A neoplasia endócrina múltipla tipo 2 (NEM-2) é uma síndrome tumoral herdada por mutações germinativas no proto-oncogene RET (RET) e transmitida por herança autossômica dominante. Atualmente, a indicação de tireoidectomia total preventiva é recomendada a indivíduos portadores de mutações no RET. Analisamos a aplicação do método Eletroforese em Gel Sensível à Conformação (CSGE) no rastreamento de mutações hot-spots do RET. Sete famílias com NEM-2 foram rastreadas pelo CSGE, seqüenciamento gênico e análise do Polimorfismo Conformacional de Cadeia Simples (SSCP). Usando o CSGE e SSCP, identificamos cinco das seis (83,3%) mutações verificadas pelo seqüenciamento: Cys620Arg, Cys634Arg, Cys634Tyr, Val648Ile e Met918Thr. Foram analisados 128 amplicons englobando mutações hot-spots do RET e 116 dentre 128 (90.6%) concordaram com o seqüenciamento genético. Os polimorfismos 691 e 769 também foram documentados pelo CSGE e SSCP. Os dados obtidos por CSGE e SSCP foram totalmente (100%) concordantes. O CSGE revelou ser metodologia sensível, rápida, fácil de ser executada e de baixo custo na detecção de mutações nos códons 620, 634, 648, e 918, as quais constituem grande maioria (~95%) dos pacientes com NEM-2. Quanto à mutação Val804Met (prevalência na população inferior a 3%), o método necessita ser otimizado. Concluímos que o CSGE é uma metodologia efetiva para o rastreamento de mutações que mais freqüentemente ocorrem no RET como causadora de NEM-2. / Multiple endocrine neoplasia type 2 (MEN2) is an autosomal dominant inherited tumor syndrome caused by activating germline mutations in RET proto-oncogene (RET). Presently, the prophylactic total thyroidectomy is recommended to all RET mutations carriers. Here we tested the Conformation Sensitive Gel Electrophoresis (CSGE) as a screening method for the RET hot-spot mutations. Seven MEN2 families were studied by CSGE, as well as by Single Strand Conformational Polymorphism (SSCP) and direct sequencing analysis. Using CSGE and SSCP, we were able to detect five out of the six (83.3%) RET mutations verified by direct sequencing analysis: Cys620Arg, Cys634Arg, Cys634Tyr, Val648Ile and Met918Thr. RET polymorphisms 691 and 769 were verified by CSGE and SSCP. In our sample, data obtained using CSGE were fully concordant (100%) with SSCP findings. Thus, CSGE showed to be a sensitive, fast, low-cost, and ease procedure to detect RET mutations in codons 620, 634, 648, and 918 which are reported as the most prevalent RET variants (~95%) in large MEN2 series. As to the Val804Met mutation (prevalence in the population lower than 3%), this method still needs to be optimized. We concluded that CSGE is an effective screening method for the most frequent RET hot-spot disease-causing mutations.

Carcinoma medular/genética

Eletroforese/métodos

Mutação/genética

Neoplasias da tireóide/diagnóstico

Proto-oncogenes/genética

DNA mutational analyses/methods

Electrophoresis/methods

Medullary carcinoma/genetic

Mutation/genetic

Polymerase chain reaction/methods

Proto-oncogene/genetic

Thyroid neoplasia/diagnosis

Expressão de indoleamina 2,3-dioxigenase (IDO) e triptofano 2,3-dioxigenase(TDO) no ambiente cervicovaginal normal, na vaginose bacteriana e nas lesões cervicais associadas ao HPV / Expression of indoleamine 2,3-dioxygenase (IDO) and tryptophan 2,3-dioxygenase (TDO) in normal cervicovaginal environment, bacterial vaginosis and cervical lesions associated with HPV

Venancio, Paloma Almeida

04 October 2018

Neste estudo avaliamos o papel do metabolismo do triptofano (Trp) na homeostasia, na vaginose bacteriana e nas lesões cervicais associadas ao HPV. A importância do metabolismo do Trp se deve a sua ação na proliferação de microrganismos e de células do sistema imune. O consumo de triptofano tem sido identificado como uma forma de controlar o crescimento bacteriano limitando a infecção. Por outro lado, a oxidação de Trp produz quinurenina (QUIN), que tem papel chave na tolerância imunológica. A formação de QUIN se dá através das enzimas indoleamina 2,3-dioxigenase (IDO) e triptofano 2,3- dioxigenase (TDO). A mais estudada delas no âmbito das infecções/ imuno escape é a enzima IDO. Mais recentemente, tem-se dado ênfase ao papel da TDO no câncer. Nesta dissertação, o interesse foi avaliar a expressão da IDO no epitélio cervicovaginal de mulheres com vaginose bacteriana e de IDO e TDO em amostras cervicais de mulheres com diferentes graus de lesão cervical associada ao HPV. Foram incluídas 165 mulheres atendidas no CAISM/UNICAMP, as quais foram divididas em dois grupos: grupo caso composto por mulheres com lesão de baixo ou alto grau e carcinoma invasor (n=42) e grupo controle composto por mulheres com citologia oncológica normal, independente de apresentar infecção genital (n=123). IDO foi avaliada por imunocitoquímica em citologia em base líquida e IDO e TDO em biópsias cervicais. Mulheres com vaginose bacteriana apresentaram expressão aumentada de IDO em células escamosas em comparação às mulheres sem vaginose bacteriana (OR=7.41; IC 95%= 2.50 a 21.4; p <0.0001). No epitélio vaginal normal com ou sem infecção por HPV houve uma expressão leve de IDO em células escamosas. Na presença de lesões ou carcinoma, houve um aumento no número de células escamosas displásicas e de leucócitos IDO-positivos; aumento de IDO também pôde ser observada em culturas de pele organotípicas transduzidas com as oncoproteínas E6/ E7 do HPV16. Nas lesões cervicais, assim como visto para a IDO, a TDO esteve expressa em leucócitos, especialmente os infiltrados na região estromal e na parede dos vasos sanguíneos. A expressão basal de IDO no epitélio cervical normal e sua regulação positiva na infecção por HPV e lesões associadas sugerem a participação do metabolismo do Trp nos mecanismos imunossupressores envolvidos na doença. Embora o papel do IDO já tenha sido abordada anteriormente, até onde sabemos esta é a primeira evidência da expressão de TDO no epitélio vaginal, na neoplasia intraepitelial cervical e carcinoma de células escamosas. Ainda, em leucócitos, especialmente aqueles com morfologia típica de polimorfonucleares, parecem ser importantes fontes de IDO na cérvix uterina. / In this study we evaluated the role of tryptophan (Trp) metabolism in cervix homeostasis, bacterial vaginosis and HPV-associated lesions. The importance of Trp metabolism is due to its action on microorganisms and immune cells. Tryptophan consumption has been identified as a way to controlling bacterial growth limiting infection. On the other hand, the oxidation of Trp produces kynurenine (Kyn) which plays a key role in immunological tolerance. The formation of Kyn occurs through the enzymes indoleamine 2,3-dioxygenase (IDO) and tryptophan 2,3-dioxygenase (TDO). IDO is the most studied of them within the context of infections / immune escape. More recently, TDO has also been considered in studies of cancer progression. In this thesis, we were interested in cervicovaginal epithelium IDO expression in women with bacterial vaginosis and of IDO and TDO in cervical samples of women with different degrees of cervical lesion associated with HPV. A total of 165 women attended at CAISM/UNICAMP were divided into two groups: a case group composed of women with low or high grade lesions and invasive carcinoma (n = 42) and a control group composed of women with normal cytology, independent to present genital infection (n =123). IDO was evaluated by immunocytochemistry in liquid-based cytology and IDO and TDO in cervical biopsies. Women with bacterial vaginosis had increased IDO expression in squamous cells compared to women without bacterial vaginosis (OR = 7.41, 95% CI = 2.50- 21.74; p<0.0001). In normal vaginal epithelium with or without HPV infection there was a mild IDO expression in squamous cells. In the presence of cervical intraepithelial lesions or squamous cell carcinoma, there was an increase in the number of IDO-positive dysplastic squamous cells and leukocytes; increase in IDO can also be observed in organotypic skin cultures transduced with HPV-16 E6/E7 oncoproteins. In cervical lesions, as observed for IDO, TDO was expressed in leukocytes, especially infiltrates in the stromal region and in the wall of blood vessels. The basal expression of IDO in the normal cervical epithelium and its positive regulation in HPV infection and associated lesions suggests the participation of Trp metabolism in the immunosuppressive mechanisms involved in the disease. Although some previous data have already considered the role of IDO, as far as we know this is the first evidence of the participation of TDO in the vaginal epithelium, cervical intraepithelial neoplasia and squamous cell carcinoma. In addition, in leukocytes, especially those with a typical polymorphonuclear morphology, appear to be important sources of IDO in the uterine cervix.

Bacterial vaginosis

Carcinoma de células escamosas

Cervical intraepithelial neoplasia

HPV

HPV

Indoleamina 2,3-dioxigenase

Indoleamine 2,3-dioxygenase

Neoplasia intraepitelial cervical

Squamous cell carcinoma

Triptofano 2,3-dioxigenase

Tryptophan 2,3-dioxygenase

Vaginose bacteriana

Estudo do HPV e variáveis sócio-comportamentais em mulheres com lesão intra-epitelial de alto grau / HPV and sociodemographic characteristics in women with highgrade squamous intraepithelial lesion.

Ramos, Karina Serravalle

10 March 2010

A infecção pelo HPV em mulheres abaixo de 30 anos é transitória, entretanto, algumas destas mulheres progridem para Lesão Intra-Epitelial de Alto Grau (LIAG). Este estudo investigou características virais, morfológicas e variáveis sócio-comportamentais em mulheres com LIAG, entre estas a determinação dos genótipos oncogênicos do HPV, a carga viral total e específica de HPV 16, a expressão da proteína p16INK4a assim como variáveis epidemiológicas. Foram selecionadas 88 mulheres provenientes de dois serviços de oncologia ginecológica de Salvador, Bahia, a Clínica IDEM e o CICAN, entre julho de 2006 e janeiro de 2009 com diagnóstico citopatológico de LIAG. As pacientes preencheram o Termo de Consentimento Livre e Esclarecido e responderam um questionário contendo informações sócio-demográficas e clínicas. Em seguida, foi realizada a colheita de células esfoliadas do colo uterino para genotipagem através da técnica Linear Array e avaliação da carga viral do HPV por PCR em tempo real, e a biópsia para análise histopatológica. Destas 88 mulheres, apenas 41 (46,6%) tiveram o diagnóstico de LIAG confirmado através do exame histopatológico. Desta forma, as pacientes foram divididas em 3 grupos: sem LIAG (< NIC 2), com LIAG ( NIC 2) menores que 30 anos e com LIAG ( NIC 2) com idade igual ou superior a 35 anos. Dentre os co-fatores analisados, a escolaridade, o uso de anticoncepcional oral e paridade diferiram nos dois grupos de idade com LIAG. A expressão da proteína p16INK4a foi observada em todos os graus histopatológicos com LIAG, entretanto, sua intensidade não diferiu entre estes. Foi observada uma maior prevalência de LIAG em mulheres mais jovens. Os genótipos mais prevalentes nas mulheres com LIAG foram: HPV 16, HPV 35, HPV 56, HPV 45 e HPV 70; no grupo sem LIAG foram: HPV 16, HPV 31, HPV 56, HPV 61 e HPV CP6108. A carga viral total foi maior em mulheres com LIAG em relação a mulheres sem LIAG. Houve associação entre aumento da carga viral específica para HPV 16 e aumento da severidade das lesões intraepiteliais. As cargas virais total e específica do HPV 16 não diferiram entre os dois grupos de idade com LIAG, indicando não ser esta o fator que leva ao raro desenvolvimento de LIAGs em mulheres jovens. / HPV infection in young women, below 30 years old is commonly transitory. However, some women may progress to high-grade squamous intraepithelial lesion (HSIL). This study aimed to investigate viral and host factors in young women with a diagnosis of HSIL, such as viral load both total and HPV 16- specific, genotypes, p16INK4a expression and sociodemographic characteristics. Eighty-eight women with a cytological diagnosis of HSIL were recruited from 2 specialized oncoginecologyc services from Salvador, Bahia, in between July 2006 and January 2009. After providing written informed consent, cervical scrapes were obtained for DNA extraction for further molecular testing, including HPV genotyping by Linear array and viral load determination by Real-Time PCR. Biopsies were taken for confirmatory histopathologyc analysis. Forty-one out of 88 enrolled women (46,6%) had the HSIL diagnosis confirmed. Based on that they were classified into three groups: No SIL, HSIL less than 30 years old and HSIL older than 35 years old. Among co-factors studied, education, oral contraceptive use and parity significantly differed between HSIL age groups. p16INK4a expression was observed with similar intensity among all histological grades of CIN. A higher prevalence of HSIL was detected in younger women. The most prevalent genotypes in HSIL patients were HPV 16, HPV 35, HPV 56, HPV 45 and HPV 70; whereas in the No SIL group were: HPV 16, HPV 31, HPV 56, HPV 61 and HPV CP6108. Total HPV viral load was significantly higher in women bearing CIN than in the normal group. A positive association between HPV 16 viral load and increasing histological grades was observed. Total and HPV 16 viral loads were similar among young and older women with HSIL, suggesting that this is not the main factor leading to the early development of these lesions.

Adolescent

Adolescente

Adult

Adulto

Carga viral

Fatores de risco

Papillomaviridae

Papillomaviridae

Polimerase chain reaction

Reação em cadeia da polimerase

Risk factors

Viral load

Identificação de moduladores genéticos em uma grande família com neoplasia endócrina múltipla (NEM1) / Identification of modifying genetic fatctors in a large family with multiple endocrine neoplasia type 1

Longuini, Viviane Cristina

18 March 2011

A Neoplasia endócrina múltipla tipo 1 (NEM1; OMIM 131100) é uma síndrome endócrina hereditária, que envolve tumores nas glândulas paratireóides, pâncreas endócrino/duodeno e hipófise. Mutações germinativas no gene supressor de tumor MEN1 são identificadas em aproximadamente 80% dos casos familiais. Os casos restantes podem apresentar grandes deleções no gene MEN1 (raras), não identificáveis ao seqüenciamento direto, ou mutações em outros genes, ainda pouco conhecidos. Recentemente, mutações germinativas em genes que codificam quinases dependentes de ciclinas, como o gene supressor de tumor p27Kip1, foram identificadas em cerca de 1-2% dos pacientes NEM1 sem mutação no gene MEN1. Esses pacientes apresentam uma clínica similar à NEM1, sendo chamada de NEM-like ou NEM4. Estudos in vitro mostraram que a proteína codificada pelo gene MEN1, MENIN, controla a expressão gênica de p27Kip1, indicando que ambos os genes fazem parte da mesma via celular supressora de tumor. Devido à correlação genótipo-fenótipo ser muito fraca nessa síndrome e à grande variabilidade fenotípica encontrada em pacientes com NEM1 (mesmo entre indivíduos/familiares que possuem mesma mutação no gene MEN1), no presente estudo investigamos a hipótese do envolvimento do gene p27Kip1, e de outro gene supressor de tumor recentemente associado com um fenótipo tumores hipofisários famílias, o gene AIP, como possíveis moduladores de fenótipo entre os pacientes com NEM1 de uma extensa família brasileira com a mutação germinativa MEN1 c.308delC e ampla variabilidade fenotípica. Dentre uma série de variáveis clínicas investigadas, observamos um possível papel modulador de fenótipo do gene p27Kip1 nesta família com NEM1. Foi encontrada associação significante entre o genótipo do polimorfismo p.V109G do gene p27Kip1, localizado em um domínio de ligação com a proteína p38 (que é um regulador negativo de p27 por levar à degradação dessa proteína), com os seguintes aspectos clínicos: maior agressividade do tumor hipofisário (macro vs. microadenomas), precocidade no desenvolvimento do tumor pancreático, e presença de carcinóides e metástases nos pacientes analisados (p< 0,05). Não foi observada nenhuma associação do gene AIP e o fenótipo dos pacientes com NEM1. O presente estudo investigou, pela primeira vez, o status germinativo do gene p27Kip1 em pacientes com mutação MEN1 e identificou uma associação significante em relação à susceptibilidade e agressividade dos tumores na coorte estudada / Multiple endocrine neoplasia type 1 (MEN1) is an inherited tumoral syndrome that involves tumors in the parathyroids, anterior pituitary and in the pancreatic islet(s) cells. Germline mutations in the tumor suppressor gene MEN1 are detectable through direct sequencing in the majority (80%) of the patients with familial MEN1. The remaining patients may present large MEN1 gene deletions, not detectable through direct sequencing, or mutations in other genes, so far largely unknown. Recently, rare mutations in genes that encode cyclin-dependent kinases, as p27Kip1, have been reported in approximately 1-2% of the patients without a MEN1 mutation. These patients were reported as presenting a MEN1-like (or the MEN4) syndrome phenotype. In vitro studies have demonstrated that the protein encoded by the MEN1 gene, MENIN, controls the expression of the p27Kip1 gene and, therefore, these two genes seem to act in the same intracellular tumor suppressor pathway. Due to the lack of genotype-phenotype correlation in MEN1 and the large clinical variability usually observed within unrelated patients carrying the same MEN1 mutation, we hypothesized that p27Kip1 (as well as AIP gene, recently associated with familial predisposition to pituitary tumors) may act as phenotypic modifying gene(s) in the MEN1 syndrome. Herein, we analyzed possible correlations between p27Kip1 genotype and a number of clinical features. We identified significant statistic associations between the p.V109G p27Kip1 polymorphism and phenotype manifestations, indicating a potential role of p27Kip1 in modifying MEN1 phenotype, as follows: pituitary tumor size; early development of pancreatic tumors, and presence of carcinoids and metastasis (p< 0,05). In addition, a possible association with the AIP gene was excluded. The present study analyzed, for the first time, the germline status of p27Kip1 gene in MEN1-mutated patients and identified a potential interaction between the genotype of this tumor suppressor gene in regulating susceptibility and the tumor aggressiveness in MEN1 patients

Gene supressor de tumor p27Kip1

Genes neoplásicos

Genes supressores de tumor

Moduladores de fenótipo

Multiple endocrine neoplasia type 1

Neoplasia endócrina múltipla tipo 1

Neoplasic genes

Phenotypic modifiers

Tumor suppressor gene p27Kip1

Tumor suppressor genes

Avaliação de novos marcadores prognósticos e preditivos em neoplasia mamária de cadelas: avaliação sérica e molecular do VEGF e do HIF-1&#945;

Moschetta, Marina Gobbe

16 September 2013

Made available in DSpace on 2016-01-26T12:51:46Z (GMT). No. of bitstreams: 1 marinagobbemoschetta_dissert.pdf: 2656918 bytes, checksum: d63acce15a1feb7170b4c9270fd920d9 (MD5) Previous issue date: 2013-09-16 / Fundação de Amparo a Pesquisa do Estado de São Paulo / Introduction: Mammary tumors are the most common type of tumor in dogs, with approximately half of these tumors are malignant. Hypoxia, characterized by oxygen levels below normal, is a known adverse factor to cancer treatment. The transcription factor HIF-1&#945; is the central regulator of pathophysiological response of mammalian cells to low oxygen levels, able to activate transcription of the vascular endothelial growth factor (VEGF), which in turn promotes angiogenesis through its ability to stimulate growth, migration and invasion of endothelial cells, contributing to tumor growth. Objectives: To evaluate the serum concentration and the gene expression of VEGF and HIF-1&#945; linking them with clinicopathological parameters and survival of dogs with mammary tumors in order to infer the possible prognostic value of these factors. Material and Methods: We collected tumor fragments of 30 bitches with mammary tumors to verify protein expression of VEGF and HIF-1&#945; by immunohistochemistry and gene expression by RT-PCR. To determine the serum concentration of VEGF and HIF-1&#945; by ELISA (Enzyme-linked immunosorbent), serum was collected from 50 bitches control (healthy) and 30 bitches with mammary neoplasia (study group). The results were statistically related to clinicopathological features. Results: The comparison between immunohistochemical staining of the two proteins analyzed showed increased intensity of immunostaining of VEGF (p=0.03). By ELISA, we observed relationship between high serum levels of VEGF and abundant vascularization (p=0.02), metastasis (p=0.003), death rate (p=0.007) and low survival (p<0.0001). In addition, increased serum levels of VEGF in the study group compared to the control group (p=0.03). In contrast, the percentage of serum HIF-1&#945; bitches with mammary neoplasia was 20% lower than the control group of female dogs (p=0.0006). However, bitches with a history of recurrent tumor showed a 15% increase in the percentage of serum HIF-1&#945; (p=0.03). Regarding gene expression, there was a relationship between increased gene expression of VEGFA and tumor abundant vascularization (p=0.02), bitches with a history of recurrence (p=0.01) and death (p=0.02). Moreover, we observed a statistically significant increase in gene expression of HIF-1A with moderate vascularization (p=0.01) and bitches that remained alive during the follow-up period (p=0.003). Conclusions: Our results demonstrate a correlation between VEGF and features of poor prognosis, suggesting that this factor plays an important role in tumor progression and can be used as a potential prognostic marker in clinical practice and is useful in predicting tumor progression in dogs with mammary neoplasia. / Introdução: As neoplasias mamárias são o tipo mais comum de tumor na espécie canina, sendo aproximadamente metade desses tumores de caráter maligno. A hipóxia, caraterizada por níveis de oxigênio abaixo do normal, é um conhecido fator adverso ao tratamento do câncer. O fator de transcrição HIF -1&#945; é o regulador central da resposta fisiopatológica das células de mamíferos para baixos níveis de oxigênio, capaz de ativar a transcrição do fator de crescimento endotelial vascular (VEGF), que por sua vez, promove a angiogênese através da sua capacidade de estimular o crescimento, migração e invasão de células endoteliais, contribuindo para o crescimento tumoral. Objetivos: Avaliar a concentração sérica e a expressão gênica do VEGF e do HIF-1&#945; relacionando-os com os parâmetros clínico-patológicos e a sobrevida de cadelas com neoplasia mamária a fim de inferir o possível valor prognóstico desses fatores. Material e Métodos: Foram coletados fragmentos tumorais de 30 cadelas com neoplasia mamária para verificar a expressão protéica do VEGF e do HIF-1&#945; por imuno-histoquímica e a expressão gênica por PCR em Tempo Real. Para determinar a concentração sérica do VEGF e do HIF-1&#945; pelo método de ELISA (Enzyme-linked immunosorbent), foram coletados soro sanguíneo de 50 cadelas controle (saudáveis) e 30 cadelas com neoplasia mamária (grupo de estudo). Os resultados encontrados foram estatisticamente relacionados às características clínico-patológicas. Resultados: A comparação entre a marcação imuno-histoquímica das duas proteínas analisadas demonstrou aumento da intensidade da imunomarcação do VEGF (p=0,03). Por meio da técnica de ELISA, foi possível observar relação entre altos níveis séricos de VEGF com vascularização abundante (p=0,02), metástase (p=0,003), óbito (p=0,007) e baixa taxa de sobrevida (p<0,0001). Além disso, houve aumento dos níveis séricos de VEGF no grupo de estudo quando comparados ao grupo controle (p=0,03). Ao contrário, o percentual sérico de HIF-1&#945; das cadelas com neoplasia mamária foi 20% menor do que das cadelas do grupo controle (p=0,0006). No entanto, cadelas com histórico de recidiva tumoral demonstraram aumento de 15% no percentual sérico de HIF-1&#945; (p=0,03). Quanto à expressão gênica, houve relação entre o aumento da expressão gênica do VEGFA e tumores com vascularização abundante (p=0,02), cadelas com histórico de recidiva tumoral (p=0,01) e óbito (p=0,02). Por outro lado, foi observado aumento estatisticamente significante da expressão gênica do HIF-1A com vascularização moderada (p=0,01) e cadelas que continuaram vivas durante o período de acompanhamento (p=0,003). Conclusões: Nossos resultados demostram correlação entre o VEGF e as características de pior prognóstico, sugerindo que este fator desempenha um importante papel na progressão tumoral, podendo ser utilizado como um potencial marcador prognóstico na rotina clínica, sendo útil na predição da progressão tumoral em cadelas com neoplasia mamária.

angiogênese

ELISA

hipóxia

HIF-1&#945

qPCR

VEGF

neoplasia mamária canina

angiogenesis

ELISA

hypoxia

HIF-1&#945

qPCR

VEGF

canine mammary neoplasia