Spelling suggestions: "subject:"endometrial"" "subject:"ndometrial""
201 |
Prevention of Ovarian and Endometrial Cancer by Combined Oral Contraceptives: A Demographics StudyHeywood, Joanna S. 01 January 2017 (has links)
Endometrial cancer is the most common gynecologic cancer with 54,870 cases occurring in the United States in 2015 and causing 10,170 deaths, an 18.5% mortality rate (Elit and Reade, 2015). Ovarian cancer, while less common, is much more fatal. In 2015 in the United States, 21,290 cases occurred and resulted in 14,180 deaths, a 66.6% mortality rate. This mortality rate makes ovarian cancer the fifth most deadly cancer for women in the United States, which is largely explained by ineffective screening strategies and limited treatment possibilities (Cramer, 2012). Thus, developing effective prevention strategies is especially important to saving the lives of women who will develop ovarian or endometrial cancer. Women taking combined oral contraceptives (COCs), a type of hormonal birth control, have shown a significant reduced risk of developing ovarian and endometrial cancer. However, the Centers for Disease Control and Prevention (CDC) does not currently recommend taking COCs for the prevention gynecologic cancer (CDC, 2014a). Since the efficacy of COCs for reducing risk of ovarian and endometrial cancer is well established, guidelines need to be determined for populations of women that should take hormonal birth control to minimize cancer risk. This paper highlights the current understanding of ovarian and endometrial cancer, populations of women at highest risk for developing either of these two cancers, and then proposes a case-control study to help determine which populations of women should take hormonal birth control to reduce their gynecologic cancer risk.
|
202 |
Comparison of a leukocyte esterase test with endometrial cytology for the diagnosis of subclinical endometritis and correlation with first service pregnancy rate in postpartum Holstein cowsCouto, Gabriel B. 11 1900 (has links)
L’objectif de la présente étude était d’évaluer un test d’estérase leucocytaire (LE) pour le diagnostic de l’endométrite subclinique chez les vaches Holstein en période postpartum. Les tests effectués à partir d’échantillons provenant soit de l’endomètre (UtLE) ou du col utérin (CxLE) ont été comparés à la cytologie endométriale (CE). Par ailleurs, deux méthodes d’évaluation des lames ont été comparées. Deux cent quatre vingt-cinq vaches Holstein de 5 troupeaux laitiers commerciaux ont été évaluées entre 21 et 47 jours en lait (JEL). Soixante sept vaches ont été diagnostiquées avec une endométrite clinique suite à un examen transrectal et vaginoscopique et ont été exclues de l’étude. Deux cent dix-huit vaches ont eu des prélèvements pour la CE et le test LE. La fonction ovarienne a été déterminée à la palpation transrectale. La banque de données utilisée pour chacune des vaches a été effectuée à partir du logiciel DSA (Dossier de Santé Animale) laitier. Le pourcentage de neutrophiles était significativement corrélé avec les scores de LE utérin et cervical. L’activité de CxLE et UtLE diminuait significativement avec les JEL, mais n’était pas associée au risque de gestation à 90 JEL (n= 186). Le pourcentage de neutrophiles mesuré à la CE entre 32 et 47 JEL était associé significativement au risque de gestation à 90 JEL (n=94, P=0.04). Pour la même période, selon une analyse de survie, les vaches avec >2,6% de neutrophiles à la CE étaient définies comme étant atteintes d’une endométrite subclinique avec une prévalence de 56%. Les résultats indiquent que le test d’estérase utérin ou cervical a une bonne concordance avec le pourcentage de neutrophiles à la CE. Une endométrite subclinique diagnostiquée par cytologie endometriale entre 32 et 47 JEL est associée à une réduction du risque de gestation au premier service. / The point toward this study was to determine the diagnostic test characteristics of the leukocyte esterase activity test for subclinical endometritis in postpartum Holstein dairy cows. The objectives were 1) to compare uterine leukocyte esterase activity and the endometrial cytology (EC), 2) to compare leukocyte esterase activity of the cervix (CxLE) and the uterus (UtLE), 3) Compare two methods of assessing the slides (i.e. an exhaustive method and a rapid method). Two hundred eighty five post partum Holstein cows from 5 commercial dairy herds had a post partum evaluation between 21 and 47 days in milk (DIM). Sixty seven cows where diagnosed with clinical endometritis by transrectal and vaginoscopy examinations and were excluded from the study. Two hundred eighteen cows were enrolled for endometrial cytology and esterase activity test. The ovarian status was determined by transrectal examination. Computerized databank, dairy DSA (Dossier de Santé Animale) indexing all the cows was used to retrieve individual information for analysis. The percentage of neutrophils was significantly correlated with the LE from the uterus and cervix. The LE from cervix and uterus decreased significantly with DIM, however, they were not statistically associated with pregnancy risk at 90 DIM (n=186). Between 32-47 DIM, the percentage of neutrophils and risk of pregnancy at 90 DIM were associated (n=94, P=0.04). For the same period, survival analysis identified cows with > 2.6 % neutrophils on EC as subclinical endometritis cows with a prevalence of 56%. The two methods for assessing the slides were correlated by 81%. Subclinical endometritis diagnosed by endometrial cytology between 32 and 47 DIM was associated with reduced risk of pregnancy at first service.
|
203 |
Estudo comparativo das alterações morfológicas e vasculares do útero durante a prenhez precoce de embriões de clones bovinos produzidos por SCNT em três diferentes apresentações gestacionais / Comparative study of morphological and vascular changes of the uterus during the early pregnancy of bovine embryos clones produced by SCNT in three different gestational phenotypesOliveira, Marcelo de Luna Freire 19 July 2017 (has links)
A clonagem por transferência de núcleo de células somáticas (SCNT) em bovinos é uma biotécnica ineficiente, porém é uma ferramenta muito importante para pesquisas em biologia do desenvolvimento. Estudos prévios em nosso laboratório identificaram três fenótipos gestacionais de clones bovinos produzidos por SCNT: (1) gestação normal (CNG) - presença do embrião (EP), vesícula embrionária (VE) e corpo lúteo ativo (CL); (2) gestação anembrionada (CAG) - presença da VE e CL ativo e ausência de EP; (3) receptoras com CL ativo persistente sem a presença de EP e VE (CPCL). Vacas doadoras de embriões foram sincronizadas pelo protocolo de super-ovulação (SOV) e inseminadas artificialmente, os embriões obtidos após sete dias da ovulação foram transferidos para receptoras que ao ficarem gestantes formaram o grupo controle (GC). O objetivou do estudo foi investigar as características morfovasculares do útero nestes quatro fenótipos gestacionais. A hipótese central foi que as características morfovasculares do útero são moduladas diferentemente nos três fenótipos gestacionais de embriões clonados por SCNT e gestação controle. Vacas Nelores foram sincronizadas e utilizadas como receptoras de embriões. Coletas de sangue para análise de progesterona e exames ultrassonográficos nos modos B e Doppler para análise da morfologia e vascularização uterina foram realizados a cada dois dias a partir do dia 6 até o dia 30 pós-ovulação. Entre os dias 31 e 36, as receptoras foram abatidas e o útero coletado para análises in situ. A simetria entre cornos, o grau de desenvolvimento de carúnculas e da VE foram mensurados e amostras endometriais coletadas para quantificação relativa do fator de crescimento endotelial vascular (VEGF) e seu receptor do tipo 2 (VEGF-R2) por western-blotting. No total foram realizadas 212 sincronizações do ciclo estral, das quais 79 receptoras receberam embriões de clones por SCNT e 49 receberam embriões produzidos in vivo. Aos 25 dias pós-ovulação as taxas de concepção por grupo foram: CNG = 15,1% (12/79), CAG = 2,5% (2/79), CPCL = 8,8% (7/79) e CG = 24,4% (10/49). Duas receptoras da raça Tabapuã (Bos taurus indicus) do fenótipo do grupo CAG provindas de outro experimento foram incluídas nas análises. Algumas receptoras foram excluídas do experimento devido a perdas gestacionais ocorridas antes do momento do abate, restando para as análises sete receptoras no grupo CNG, três no CAG, quatro no CPCL e nove no CG. Somente o grupo CG apresentou diferença de perfusão vascular entre os cornos uterinos ipso e contralateral (P<0,05). Em relação ao corno ipsolateral, os grupos CG e CNG apresentaram maior perfusão vascular em relação ao grupo CPCL do dia 24 ao 30 (P<0,05). Porém, com a média dos escores da perfusão vascular endometrial de ambos os cornos, o grupo CNG apresentou maiores valores em relação aos grupos CAG e CPCL nos dias 24 e 30. Os índices de resistência vascular (RI) nas artérias uterinas confirmaram os dados subjetivos de diferença de perfusão vascular entre cornos, o corno ipsolateral do grupo CG apresentou menor RI em relação ao contralateral nos dias 22, 24, 28 e 30 (P<0,05) e os grupos CNG e CPCL não apresentaram diferença entre cornos (P>0,05). Entre os grupos, o RI no CG e CAG foi menor que no CPCL no dia 30 (P<0,05). A concentração de progesterona (P4) sanguínea foi menor no grupo CPCL em relação aos grupos CG e CNG nos dias 18 e 26 (P<0,05). A P4 atingiu valores próximos de 8 ng/ml a partir do dia 22 nos grupos CG e CNG, sendo que no grupo CPCL os valores foram inferiores à 6 ng/ml a partir do dia 14. As análises in situ revelaram maior frequência de assimetria de cornos uterinos no grupo CG em relação aos grupos CNG, CAG e CPCL; o grupo CNG obteve maior frequência de ocorrência de carúnculas e VE desenvolvidas nos dois cornos uterinos em relação aos grupos CAG e CPCL (P<0,05), não diferindo do grupo CG (P>0,05). O comprimento dos embriões do grupo CNG foi maior que dos embriões do grupo CG (P<0,05), entre os dias 28 e 34. Não foi detectada diferença de abundância relativa das proteínas VEGF e VEGF-R2 entre os quatro grupos estudados, porém quando os grupos de gestações normais (CG e CNG) foram comparados com os grupos de gestações alteradas (CAG e CPCL) foi detectada maior abundância relativa para o fragmento de 75 kDa da proteína do VEGF-R2 no grupo de gestações alteradas. A hipótese central do estudo, que afirma que as alterações morfovasculares do útero gestante durante o primeiro mês são moduladas em diferentes graus de forma dependente à qualidade de desenvolvimento do concepto foi confirmada. Por fim, este estudo proporcionou um melhor entendimento da fisiologia endócrina, morfológica e vascular das gestações normais e alteradas de embriões clonados por SCNT durante o primeiro mês gestacional, fornecendo base para novos estudos sobre o desenvolvimento e manutenção da gestação inicial em bovinos. / Cloning by nuclear transfer of somatic cells (SCNT) in cattle is an inefficient biotechnique. However, it is a very important tool for research in developmental biology. Previous studies from our lab have identified three gestational phenotypes of bovine clones: (1) Clone normal gestation (CNG) - presence of embryo (EP = embryo proper), embryonic vesicle (EV) and corpus luteum (CL); (2) Clone anembryonic gestation (CAG) - presence of EV and CL and no EP; (3) Recipient presenting only a persistent CL (CPCL). Embryo donor cows were synchronized by superovulation protocol (SOV) and artificially inseminated, embryos obtained after seven days of ovulation were transferred to the control group (CG). This study aimed to investigate whether modulation of the morphological and vascular abnormalities of the uterus by the presence of the cloned conceptus is different between the three gestational clone phenotypes and control. The central hypothesis was that the morphovascular characteristics of the uterus are modulated differently in the three gestational phenotypes of embryos cloned by SCNT and control gestation. Nellore cows were synchronized and used as embryo recipients. Blood collections for progesterone analysis and ultrasound examinations in B and Doppler modes for analysis of uterine morphology and vascularization were performed every two days from day 6 to day 30. Between 31-36 days, the recipients were slaughtered and the uteri were collected for in situ analyzes. The symmetry between horns, the degree of caruncle and EV development were measured and endometrial samples were collected for relative quantification of vascular endothelial growth factor (VEGF) and its receptor type 2 (VEGF-R2) by western blotting. A total of 212 estrous cycle synchronizations were performed, 79 recipients cows received clone embryos by SCNT and 49 embryos produced in vivo. At 25 days after ovulation the conception rates by group were: CNG = 15.1% (12/79), CAG = 2.5% (2/79), CPCL = 8.8% (7/79), and CG = 24.4% (10/49). Two pregnant cows Tabapuã (Bos taurus indicus) of CAG phenotype from another experiment were included in the analyzes. Some recipients were excluded from the experiment due to gestational losses occurring before the time of slaughter, remaining seven recipients in CNG group, three in CAG, four in CPCL and nine in CG. Only the CG group had a difference in vascular perfusion between the ipso and contralateral uterine horns (P<0.05). In relation to the ipsilateral horn, the CG and CNG groups presented higher vascular perfusion compared to the CPCL group from day 24 to 30 (P<0.05). However, with the average of endometrial vascular perfusion scores of both uterine horns, the CNG group presented higher values in compared to the CAG and CPCL groups on days 24 and 30. The vascular resistance index (RI) of the uterine arteries confirmed the subjective data of vascular perfusion between horns. The ipsilateral horn of the CG group presented lower RI in compared to the contralateral on days 22, 24, 28 and 30 (P<0, 05) and the CNG and CPCL groups did not show this difference between horns (P>0.05). Among groups, the RI in CG and CAG was lower than in the CPCL on day 30 (P<0.05). The blood progesterone (P4) concentration was lower in the CPCL group than in the CG and CNG groups on days 18 and 26 (P<0.05). P4 reached values close to 8 ng/ml after day 22 in the CG and CNG groups, and in the CPCL group the values were lower than 6 ng/ml after day 14. In situ analyzes revealed a higher frequency of uterine horn asymmetry in the CG group compared to the CNG, CAG and CPCL groups; the CNG group had a higher frequency of caruncles and EV development in the two uterine horns compared to the CAG and CPCL groups (P<0.05), not differing from the CG group (P>0.05). The length of the embryos of the CNG group was higher than that of the embryos of the CG group (P<0.05) between days 28 to 34. No difference was detected in the relative abundance of VEGF and VEGF-R2 proteins among the four groups, but when the normal gestation groups (CG and CNG) were compared with the altered pregnancies groups (CAG and CPCL) a greater relative abundance was detected for the 75 kDa fragment of the VEGF-R2 protein in the group of altered pregnancies. The central hypothesis of the study, which states that the morphovascular changes of the pregnant uterus during the first month are modulated in different degrees depending on the quality of development of the concept was confirmed. Finally, this study provided a better understanding of the endocrine, morphological and vascular physiology of normal and altered embryos of cloning by SCNT during the first gestational month, providing a basis for new studies on the development and maintenance of initial gestation in cattle.
|
204 |
Avaliação do risco de metástases linfonodais no câncer do endométrio, através de parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos / Risk assessment of lymph node metastasis in endometrial cancer through clinical, laboratory, radiological and anatomopathological parameters.Anton, Cristina 11 August 2015 (has links)
INTRODUÇÃO: O câncer de endométrio é a sexta neoplasia maligna mais frequente nas mulheres no mundo. Com o crescimento mundial da obesidade, fator associado ao desenvolvimento do câncer de endométrio, estima-se que haja avanço no número de casos da doença. O tratamento cirúrgico do câncer de endométrio inclui a linfadenectomia pélvica e para-aórtica para o conhecimento do status linfonodal utilizado para determinação do tratamento adjuvante segundo a FIGO. Este é um procedimento que requer profissionais com treinamento cirúrgico avançado e não é isento de complicações. Algumas pacientes não se beneficiam da realização sistemática da linfadenectomia. O estudo das características clínicas, laboratoriais, radiológicas e anatomopatológicas das pacientes com câncer de endométrio em nossa população é fundamental para entendermos quais pacientes poderiam prescindir da linfadenectomia. MÉTODOS: Foram avaliadas 408 pacientes atendidas no Instituto do câncer do Estado de São Paulo entre janeiro de 2009 a março de 2015 com diagnóstico de carcinoma de endométrio submetidas ao tratamento cirúrgico. Foram avaliados parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos e sua capacidade de predizer metástases linfonodais. Foram construídas curvas Kaplan Meyer de sobrevivência. Além disso, as complicações relacionadas à realização da linfadenectomia também foram avaliadas. RESULTADOS: Das 405 pacientes elegíveis para o estudo 236(58,3%) foram submetidas à linfadenectomia pélvica e para-aórtica e não foi obtida amostra linfonadal em 73(18%). Os parâmetros significativos predição de acometimento linfonodal obtido através de regressão logística foram infiltração miometrial > 50%, presença de invasão linfovascular, presença de acometimento linfonodal pélvico por exame de imagem e CA125 > 21,5U/mL. A ausência dos quatro parâmetros implica em um risco de acometimento linfonodal de 2,7% enquanto que na presença de todos os quatro parâmetros o risco é de 82,3%. Nas curvas de sobrevida global (p=0,0001) e livre de doença (p=0,0004), a realização da linfadenectomia teve impacto positivo nas pacientes submetidas à linfadenectomia quando comparadas as não submetidas a este procedimento. CONCLUSÕES: A avaliação do risco de metástases linfonodais em pacientes com carcinoma do endométrio, baseadas em parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos foi capaz de identificar quatro variáveis com significativo valor preditivo de acometimento linfonodal que foram: linfonodos pélvicos pela imagem, CA125 com valor de corte 21,5U/mL, infiltração miometrial e invasão linfovascular. Na presença desses quatro parâmetros a probabilidade de acometimento linfonodal é de 82,3% / BACKGROUND: Endometrial cancer is the sixth most common malignancy in women worldwide. Obesity is a factor associated with this type of cancer development. Thus, the increase of obesity among women leads to a higher number of endometrial cancer cases. The surgical treatment of endometrial cancer includes pelvic lymphadenectomy and para-aortic to the knowledge of lymph node status used for determining the adjuvant treatment according to FIGO. This procedure requires professionals with advanced surgical training and is associated to complication. Moreover, some patients do not benefit from systematic lymphadenectomy. The study of clinical, laboratory, radiological and pathological data of patients with endometrial cancer in our population is critical to understand which patients could dispense lymphadenectomy. METHODS: This study analyzed 408 patients with the diagnosis of endometrial carcinoma undergoing surgical treatment at the Sao Paulo Cancer Institute between January 2009 and March 2015. Clinical, laboratory, radiologic and pathologic parameters were used to test the ability to predict lymph node metastasis. In addition, Kaplan Meyer survival curves were constructed. Complications related to lymphadenectomy were also evaluated. RESULTS: Out of 405 patients eligible for the study, 236 (58.3%) underwent pelvic and para-aortic lymphadenectomy and 73 (18%) had no lymph node samples. Significant parameters prediction of lymph node involvement obtained through logistic regression were myometrium infiltration > 50%, lymphovascular space invasion, pelvic lymph node involvement by imaging and CA125 > 21,5U/mL. The absence of the four parameters implies a risk of lymph node metastasis of 2.7%, whereas in the presence of all four parameters the risk is 82.3%. The overall survival curves (p = 0.0001) and the disease-free survival curves (p = 0.0004), had a positive impact on patients undergoing lymphadenectomy compared to the subject without lymphadenectomy. CONCLUSIONS: The assessment of lymph node metastasis in patients with carcinoma of the endometrial, based on clinical, laboratorial, radiologic and pathologic parameters was able to identify four variables with significant predictive value of lymph node metastasis. Those were pelvic lymph nodes by the image, CA125 > 21,5U/ml, myometrium infiltration > 50% and lymphovascular space invasion. In the presence of these four parameters, the probability of lymph node involvement is 82.3%
|
205 |
Rôle de la neurotensine dans la progression des adénocarcinomes de l’endomètre et de l’ovaire / Role of neurotensin in the progression of endometrial and ovarian adenocarcinomasAgopiantz, Mikaël 26 June 2018 (has links)
Le récepteur de haute affinité 1 (NTSR1) et son agoniste, la neurotensine (NTS), sont corrélés avec l’agressivité tumorale dans la plupart des tumeurs solides, y compris les cancers hormono-dépendants. Comme l’endomètre et l’ovaire sont également soumis à une régulation hormonale, nous avons évalué la contribution de NTS/NTSR1 à la carcinogenèse de l’endomètre et de l’ovaire. L’expression du récepteur de la neurotensine 1 (NTSR1) et la méthylation du promoteur NTSR1 (HM450) ont été analysées dans 385 cas de carcinome de l’endomètre du Cancer Genome Atlas (TCGA). De plus, à partir d’une série de 100 carcinomes de l’endomètre et de 66 échantillons d’endomètre bénin, l’expression de NTS et NTSR1 a été évalué par immunohistochimie. La série TCGA d’adénocarcinomes ovariens séreux de haut grade et une série de 46 tissus ovariens ont également été analysés. Dans la série TCGA de carcinomes de l’endomètre, le taux d’ARN messager de NTSR1 (ARNm) était négativement corrélé avec la survie globale (SG) et la survie sans progression (SSP) (p = 0,0012 et p = 0,0116, respectivement), et positivement corrélé avec le grade (p = 0,0008). En incluant seulement les carcinomes endométrioïdes, le niveau d’ARNm de NTSR1 était également négativement corrélé avec la SG (log-rank:p < 0.0001) et la SSP (log-rank: p = 0.002). Une forte expression d’ARNm de NTSR1 était significativement associée à une perte de méthylation du promoteur NTSR1. L’expression immunohistochimique de NTS et NTSR1 était significativement augmentée dans l’adénocarcinome (n = 100), par rapport à l’endomètre bénin (p <0,001). L’expression de NTSR1 était positivement corrélée avec le grade (p = 0,004). Une forte expression du NTSR1 cytoplasmique était significativement corrélée avec une SG et une SSP plus courtes (p < 0,001 et p = 0,001, respectivement). Cette corrélation restait significative en excluant les sous-types non-endométrioïdes (p = 0,04 et p = 0,02, respectivement). En analyse multivariée, l’expression de NTSR1 était un facteur de mauvais pronostic indépendant (p = 0,004). Nos résultats indiquent également la présence d’une corrélation positive entre l’expression du marqueur de prolifération MCM6 et le grade histologique dans le sous-type endométrioïde (grade I, 66,7 %, grade II, 75,3 %, grade III, 81,4 %, p <0,001) et une corrélation inverse à la SG et à la SSP (p = 0,02 pour les deux). Dans la cohorte TCGA, les analyses de Cox univariées et multivariées (p = 0,003 et p = 0,03, respectivement) ont révélé que les z-scores élevés de l’ARNm de MCM6 étaient associés à une SG réduite. Ces associations étaient absentes pour Ki-67. Il n’y avait pas de corrélation significative entre NTSR1 et MCM6 ou Ki-67. Dans l’adénocarcinome de l’ovaire, la NTS et NTSR1 ont été détectés dans 72 % et 74 % des cancers de l’ovaire, respectivement. En outre, dans la grande série d’adénocarcinomes ovariens séreux de haut grade, l’ARNm de NTSR1 s’est avéré être en corrélation avec des stades plus élevés et la résistance au platine (p = 0.02). Ceci est concordant avec les résultats expérimentaux montrant que l’antagoniste très spécifique de NTSR1, le SR48692, a augmenté la réponse au carboplatine dans les cellules cancéreuses de l’ovaire et les tumeurs expérimentales induites. Lorsque le SR48692 est combiné avec du carboplatine, une augmentation majeure des dommages à l’ADN induits par le platine et de la mort cellulaire, ainsi qu’une diminution de la croissance tumorale, a été notée. La surexpression de NTSR1 est un facteur de mauvais pronostic dans les cancers de l’endomètre et de l’ovaire, mettant en évidence la contribution de NTS dans la progression du cancer et ses utilisations en tant que marqueur pronostique, et en tant que cible thérapeutique potentielle. L’ajout d’un inhibiteur de NTSR1 en association avec une thérapie à base de sel de platine pourrait améliorer la réponse au traitement / The high affinity receptor 1 (NTSR1) and its agonist, neurotensin (NTS), are correlated with tumor cell aggressiveness in most solid tumors, including hormone-dependent cancers. As the endometrium and ovary are also subjected to hormonal regulation, we evaluated the contribution of NTS to endometrial and ovarian carcinogenesis. Neurotensin receptor 1 (NTSR1) expression and NTSR1 promoter methylation (HM450) were analyzed in 385 cases of endometrial carcinoma from The Cancer Genome Atlas (TCGA). Additionally, from a series of 100 endometrial carcinomas, and 66 benign endometrium samples, NTS and NTSR1 labeling was evaluated by immunohistochemistry. The TCGA series for ovarian high-grade serous adenocarcinoma and a series of 46 ovarian tissues were also analyzed. Using TCGA series, NTSR1 messenger RNA (mRNA) level was negatively correlated with overall survival (OS) and progression-free survival (PFS) (p = 0.0012 and p = 0.0116, respectively), and positively correlated with the grade (p = 0.0008). When including only endometrioid carcinomas, NTSR1 mRNA level continued to be negatively correlated with OS (log-rank: p < 0.0001) and PFS (log-rank: p = 0.002). A higher NTSR1 mRNA level was significantly associated with a loss of NTSR1 promoter methylation. Immunohistochemical expression of NTS and NTSR1 was significantly increased in adenocarcinoma (n = 100), as compared to benign endometrium (p < 0.001). NTSR1 expression was positively correlated with grade (p = 0.004). High immunohistochemical expression of cytoplasmic NTSR1 was significantly correlated with a shorter OS and PFS (p < 0.001 and p = 0.001, respectively). This correlation remained significant when excluding non-endometrioid subtypes (p = 0.04 and p = 0.02, respectively). In multivariate analysis, the expression of NTSR1 was an independent prognostic factor (p = 0.004). Our evidence indicated also the presence of a positive correlation between expression of proliferation marker, MCM6 and the histological grade of endometrioid endometrial adenocarcinoma (grade I, 66.7 %; grade II, 75.3 %; grade III, 81.4 %; p < 0.001) and an inverse correlation with OS ans PFS (p = 0.02 for both). For in silico analyses of the TCGA cohort, both univariate and multivariate Cox analyses (p = 0.003 and p = 0.03, respectively) revealed high MCM6 mRNA Z-scores associated with reduced OS. These associations were absent for Ki-67. No significant correlation between NTSR1 and MCM6 or Ki-67 was found. In ovarian adenocarcinoma, NTS and NTSR1 were detected in 72 % and 74 % of ovarian cancer, respectively. Furthermore, in a large series of high-grade ovarian cancer, NTSR1 mRNA was shown to correlate with higher stages and platinum resistance (p = 0.02). This correlates with experimental results showing the very specific NTSR1 antagonist, SR48692, enhanced the response to carboplatin in ovarian cancer cells and experimental tumors. When SR48692 is combined with carboplatin, a major improvement of platinum-induced DNA damage and cell death, as well as a decrease in tumor growth, was noted. NTSR1 overexpression is a poor prognostic factor in endometrial and ovarian cancer, highlighting the contribution of NTS in cancer progression and its uses as a prognostic marker, and as a potential therapeutic target. The addition of NTSR1 inhibitor in combination with platinum salt-based therapy could improve the response to the drug
|
206 |
Análise de expressão gênica da via de sinalização do receptor do fator de crescimento semelhante à insulina tipo 1 no câncer de endométrioReis, Vania Marisia Santos Fortes dos January 2018 (has links)
O câncer de endométrio tem incidência crescente, principalmente nos países desenvolvidos, devido ao estilo de vida moderno, aumento de casos de obesidade e diabetes, e diversos outros fatores que, em conjunto, estão tornando esta neoplasia na mais comum no trato reprodutor feminino. Ele é bastante influenciado pelo estado hormonal e por fatores reprodutivos das pacientes. Assim, é mais frequente no período pós-menopausa, quando pode ocorrer um desequilíbrio na sinalização do estrogênio. A diabetes e a obesidade são causadas, principalmente, pelo excesso de triglicerídeos e glicose circulantes, e pela resistência à insulina. A hiperglicemia leva à produção excessiva de insulina e do fator de crescimento semelhante à insulina tipo 1 (IGF1), sendo que estes hormônios são considerados antiapoptóticos e promotores da proliferação celular. Sabe-se que eles agem por vias semelhantes e que, provavelmente, o mecanismo responsável pela proliferação provocada por eles está associado à via PI3K/Akt/mTOR. Desta forma, avaliamos a expressão gênica de 92 genes na rota de sinalização do IGF1R em câncer de endométrio (n=3) e endométrio normal (n=2), através da técnica de qRT-PCR (ensaio TaqMan® Array Human IGF1R Signaling). Dentro destes genes, alguns estão envolvidos diretamente com a via PI3K/Akt/MAPK, outros estão implicados em processos como proliferação, diferenciação, tumorigênese, apoptose, resposta imune, síntese proteica, entre outros. Avaliamos, também, os níveis proteicos do receptor do fator de crescimento semelhante à insulina (IGF1R), IGF1 e receptor da insulina (IR) pela técnica de imunohistoquímica, além da funcionalidade geral dos 4 genes mais diferencialmente expressos no câncer de endométrio Observamos que, dos 92 genes, 26 foram expressos somente no grupo câncer - CACNA1H, CRK, EIF2B5, ELK1, FRAP1 (MTOR), GYS1, HRAS, IGF2, IKBKB, IKBKE, ITPR3, KRAS, NFAT5, NFATC1, NFKB1, NFKBIB, NFKBIE, PIK3CA, PIK3CB, PLCB1, PLCB2, PLCG2, PRKCZ, RELB, SHC1 e YWHAZ; 46 tiveram expressão aumentada no grupo câncer de endométrio - AKT1, AKT2, ARAF, ATF4, BAD, BRAF, CACNA1C, CALM1, CALM2, CALM3, CREB1, EIF4E, FOXO3, GSK3B, IGF1, IGF1R, IKBKG, IRS1, MAP2K1, MAP2K2, MAPK3, MEF2C, MEF2D, NFATC2, NFATC3. NFKB2, NFKBIA, NRAS, PDPK1, PIK3CD, PIK3R1, PIK3R2, PLCG1, PPP3CA, PPP3R1, PRKCI, RAF1, RAPGEF1, RELA, RPS6, RPS6KB1, SOS1, YWHAB, YWHAE, YWHAH e YWHAQ, um não apresentou expressão em nenhum dos grupos (SLC2A4) e não foi possível analisar os restantes 20 genes, pois não foram expressos em todas as amostras. Quanto à expressão das proteínas IGF1R, IGF1 e IR, todas se mostraram mais expressas no câncer de endométrio e que se encontram localizadas principalmente no citoplasma das células. Assim, este trabalho mostra que a sinalização do IGF1R pode ter participação importante na aquisição do fenótipo maligno das células endometriais, e que o aumento das moléculas efetoras desta via no câncer de endométrio provavelmente está relacionado ao seu papel mitogênico. / Endometrial cancer has a growing incidence, especially in developed countries, because of the modern lifestyle, increased cases of obesity and diabetes, and several other factors that together make this disease the most common in the female reproductive tract. Endometrial cancer is strongly influenced by the hormonal state and by the reproductive factors of the patients. Thus, it is attributed to the postmenopausal period, when estrogen signaling can be unbalanced, and consequently lead to malignant proliferative patterns. Diabetes and obesity are caused mainly by the excess of circulating triglycerides and glucose, and by insulin resistance. Hyperglycemia leads to excessive production of insulin and IGF1.These hormones are considered to have antiapoptotic effects and to promote cell proliferation. It is known that they are very similar pathways, and the mechanism responsible for this proliferation is associated with the PI3K/Akt/mTOR pathway. Thus, we evaluated the expression of 92 genes in IGF1R signaling pathway in endometrial cancer (n = 3) and normal endometrium (n = 2), using qRT-PCR (TaqMan® Array Human IGF1R Signaling test). Within these genes, some are in the PI3K/Akt/MAPK pathways, others are involved in proliferation, differentiation, tumorigenesis, apoptosis, immune response, protein synthesis, among others We also evaluated the protein levels of IGF1R, IGF1 and IR by immunohistochemistry, as well as the general functionality of the 4 most differentially expressed genes in endometrial cancer. We found that 26 genes were expressed only in endometrial cancer - CACNA1H, CRK, EIF2B5, ELK1, FRAP1 (mTOR), GYS1, HRAS, IGF2, IKBKB, IKBKE, ITPR3, KRAS, NFAT5, NFATc1, NFKB1, NFKBIB, NFKBIE, PIK3CA, PIK3CB, PLCB1, PLCB2, PLCG2, PRKCZ, RELB, SHC1 and YWHAZ; 46 had increased expression in endometrial cancer, when compared to control group - AKT1, AKT2, ARAF, ATF4, BAD, BRAF, CACNA1C, CALM1, CALM2, CALM3, CREB1, eIF4E, FOXO3, GSK3B, IGF1, IGF1R IKBKG, IRS1, MAP2K1, MAP2K2, MAPK3 , MEF2C, MEF2D, NFATC2, NFATC3. NFKB2, NFKBIA, PIK3R1, PIK3R2, PLCG1, PPP3CA, PPP3R1, PRKCI, RAF1, RAPGEF1, RELA, RPS6, RPS6KB1, SOS1, YWHAB, YWHAE, YWHAH and YWHAQ, one showed no expression in neither groups (SLC2A4) and the other 20 were not expressed in all samples, so we decided not to analyze them. As for the expression of IGF1R, IGF1 and IR proteins, all them showed increased expression in endometrial cancer and were localized in the citoplasm. Thus, this work shows that IGF1R signaling may play an important role in the acquisition of a malignant phenotype by endometrial cells, and that the increase of these effectors in endometrial cancer is related to its mitogenic effects.
|
207 |
Efeito do tratamento com metformina sobre o desenvolvimento, potencial metastásico e vias de sinalização do câncer de endométrio in vitroMachado, Amanda de Barros January 2017 (has links)
Endometriumkrebs ist eine der häufigsten gynäkologischen Malignomen weltweit und wird in einen Typ I eingeteilt, welcher östrogenabhängig ist, und in eine Typ-II-Östrogen-unabhängige Form. Typ I ist der häufigste Fall und kommt in etwa für 75% bis 85% aller diagnostizierten Fälle in Frage. Erhöhte Östrogenspiegel haben gezeigt, das Risiko von Gebärmutterkrebsentwicklung zu erhöhen, genauso wie Östrogen die Proliferation von Endometriumzellen stimuliert und die Apoptose hemmt. Die Insulinresistenz scheint eine zentrale Rolle in der endometrialen Karzinogenese zu spielen und darüber hinaus werden Erkrankungen mit Insulinresistenz, wie zum Beispiel das polyzystische Ovarialsyndrom (PCOS) und Adipositas, sowie Typ II-Diabetes mellitus (DM) als signifikantes Risiko angesehen, Faktoren für die Entwicklung und Progression von Typ-I-Endometrium-Krebs zu sein. Zusätzlich können PCOS-Patienten durch eine Fettleibigkeit in einem normoglykämischen Status eine unabhängige Insulin-Resistenz haben. In diesem Fall scheint die Hyperinsulinämie der fördernde Faktor zu sein, nicht nur für die Entwicklung als auch für die Tumorprogression.Aber auch erhöhte Blutzuckerspiegel tragen zum Wachstum und die Karzinogenese in Endometriumkarzinom bei und dienen als wichtige Verbindung zwischen dem beobachteten erhöhten Krebsrisiko bei Patienten mit Typ-II-DM. Die Behandlung mit einem Anti-Diabetikum, welches den Insulinspiegel senken kann, könnte einen allgemeinen Ansatz bieten gegen die Entwicklung von Krebs und zur Verringerung der Metastasierung. Das Ziel dieser Studie war es, die Wirkung einer 0,1 mM Metformin-Dosis auf das proliferative und metastatische Potential von Endometriumkrebszellen bewerten zu können, sowie die Analyse der Auswirkungen von kurz- und langfristigen Behandlungen auf intrazelluläre Signalwege der Endometriumkrebszellen.(Fortsetzung) (Fortsetzung)Ebenso soll der Zusammenhang der Entwicklung und der Progression von Krebszellen untersucht werden, wenn sie einer Umgebung mit unterschiedlichen Glucosekonzentrationen und hohen Insulinspiegeln ausgesetzt werden. Darüber hinaus ist eine endometriale dreidimensionale (3D) Cokultur zu standardisieren, für eine viabele Kultur bei 20 Tagen Kultivierung. Das proliferative Potential wurde unter Verwendung des CellTitle-Glo-Tests durchgeführt, und das metastatische Potential wurde unter Verwendung von Transwell-Migration und Invasion untersucht. Die mRNAExpression von MKI67, mTOR, NOTCH1, NOTCH3 und JAG1 Gene wurden durch real-time PCR gemessen. Die kumulative Populationsverdopplungsrate wurde durch das Replikationsverhalten einer Endometriumkrebszelllinie durchgehend von 20 Tagen nach einer Behandlungsdauer bestimmt. In allen Assays wurden die Zellen durch Medien mit normaler (5,5 mM) oder hoher (17 mM) Glucosekonzentration, sowie in verschiedenen Gruppen behandelt: Kontrolle, Insulin, Metformin und Insulin+Metformin. Das 3D-Kokulturmodell wurde unter Verwendung von endometrialen Primärzellen und einer Endometriumkrebszelllinie hergestellt, wobei die Modellkonstruktion durch Matrigel® als extrazelluläre Matrix verwendet wurde. In dieser Studie hemmte die 0,1 mM Metformin-Dosis die Insulinwirkung stark und verringerte die Fähigkeit der endometrialen Krebszelllinie, in einer hohen und normalen Glukoseumgebung zu migrieren und einzudringen.(Fortsetzung) (Fortsetzung) Auf das proliferative Potential wurde dieser Effekt nicht beobachtet, allerdings reagierte die relative Zellproliferation empfindlich auf Metformin im Bereich zwischen 1 und 5 mM, unabhängig von der vorliegenden Glucosekonzentration. In den intrazellulären molekularen Mechanismen wurde beobachtet, dass die hohe Glukosekonzentration eine optimale Umgebung für endometriale Krebszellen schafft, um einen aggressiveren Genotyp und eine Resistenz gegenüber Metformin während einer Langzeitbehandlung zu zeigen. Darüber hinaus blieb das endometriale 3DKokulturmodell über 20 Kulturtage lebensfähig. Daher zeigte sich, trotz der Endometriumkrebszellen, eine Resistenz gegenüber dem Metformin-Effekt, wenn sie einer hohen Glucoseumgebung ausgesetzt waren. Die 0,1 mM Metformin-Dosis war in der Lage, die Insulinwirkung zu hemmen und das metastatische Potential der Zellen zu verringern, was darauf hindeutet, dass Metformin klinisch in Verbindung mit Insulin wirkt, sowie die indirekten und direkten Effekte als potentieller Wirkstoff in der Krebstherapie eingesetzt werden könnten. / O câncer de endométrio é uma das neoplasias ginecológicas com maior incidência, classificado como tipo I, estrógeno dependente, e tipo II, estrógeno nãodependente. O tipo I é a forma mais comum, ocorrendo em torno de 75 – 85 % dos casos de câncer de endométrio. Altos níveis de estrogênio têm sido relacionados ao aumento do risco de desenvolvimento do câncer de endométrio, pois estimula a proliferação celular e inibe a apoptose. A resistência à insulina parece desempenhar um papel central nesta neoplasia, e as doenças associadas à resistência à insulina como obesidade, Diabetes Mellitus (DM) tipo II e Síndrome dos Ovários Policísticos (PCOS) também são consideradas fatores de risco significantes para o desenvolvimento e progressão do câncer de endométrio tipo I. Adicionalmente, pacientes com PCOS podem apresentar um quadro de resistência à insulina independente de obesidade, permanecendo em um estado glicêmico normal. Neste caso, a hiperinsulinemia isolada seria um fator tanto para a promoção, como também para a progressão do câncer. Entretanto, o aumento de níveis séricos de glicose, a hiperglicemia, também é considerada um fator independente para o desenvolvimento e progressão do câncer de endométrio sendo um elo crítico entre o aumento do risco do desenvolvimento de câncer observado em pacientes com DM tipo II Dessa forma, tratamento utilizando agentes insulino-sensibilizantes, que atuam diminuindo a resistência à insulina e consequentemente reduzindo seus níveis pode ser uma estratégia interessante para prevenir o câncer e reduzir a disseminação metastática. Os objetivos deste trabalho foram avaliar o efeito da dose de 0,1 mM de metformina sobre o potencial proliferativo e metastático das células de câncer de endométrio, assim como, avaliar o efeito do tratamento a curto e a longo prazo sobre vias de sinalização intracelular relacionadas ao desenvolvimento e progressão do câncer de endométrio quando exposta a um ambiente com diferentes concentrações de glicose e níveis elevados de insulina. Por fim, a padronização de um modelo tridimensional (3D) de cocultura de células de endométrio que permanecesse viável ao longo de 20 dias de cultivo. O potencial proliferativo foi determinado pelo método luminescente CellTitle Glo, e o potencial metastático pelo o ensaio transwell de migração e invasão. Análises de expressão do mRNA dos genes MKI67, mTOR, NOTCH1, NOTCH3 e JAG1 foram realizadas a partir da técnica de PCR em tempo real. O índice de duplicação populacional cumulativo das células determinou o comportamento de replicação da linhagem de câncer de endométrio ao longo do período de tratamento de 20 dias. Em todas os ensaios as células foram cultivadas em meio contendo concentrações normais (5,5 mM) ou altas (17 mM) de glicose, e divididas nos diferentes grupos de tratamento: controle, insulina, metformina e metformina associado a insulina. A padronização do modelo 3D de cocultura de células de endométrio foi realizado utilizando células primárias e células de linhagem de câncer de endométrio, a Matrigel® foi a matriz extracelular temporária utilizada para a construção do modelo. Neste estudo, a concentração de 0,1 mM de metformina inibiu a ação da insulina, diminuindo a habilidade de migração e invasão das células de câncer de endométrio independente da concentração de glicose presente no meio. Entretanto, este efeito não foi observado sobre o potencial proliferativo, sendo observada uma redução da proliferação das células de câncer de endométrio ao serem utilizadas concentrações maiores de metformina. Em relação aos mecanismos moleculares intracelulares, foi observado que na presença de altas concentrações de glicose as células de câncer de endométrio adquirem um genótipo mais agressivo e apresentam resistência ao efeito da metformina na dose de 0,1 mM durante o tratamento agudo. Além disso, foi possível a padronização de um modelo 3D de cocultura de células de câncer de endométrio que permanecesse viável ao longo dos 20 dias de cultivo. Contudo, apesar das células de câncer de endométrio apresentarem resistência ao efeito da metformina na presença de altas concentrações de glicose, a dose de 0,1 mM foi capaz de inibir o efeito da insulina e diminuir o potencial metastático dessas células, sugerindo que a metformina ao atuar clinicamente em combinação com seus efeitos indiretos e diretos pode ser um potencial agente adjuvante na terapia contra o câncer. / Endometrial cancer is one of the most common gynecological malignancies worldwide and is classified into a type I, which is estrogen-dependent, and a type II estrogen-independent form. The type I is the most common, accounting to 75%-85% of all cases of endometrial cancer. Elevated estrogen levels have been shown to increase the risk of endometrial cancer development, as estrogen stimulates endometrial cell proliferation and inhibits apoptosis. The insulin resistance seems to play a central role in endometrial carcinogenesis, furthermore, diseases associate with insulin resistance, as seen in polycystic ovary syndrome (PCOS), and obesity, as well as type II diabetes mellitus (DM) are considered as significant risk factors for the development and progression of type I endometrial cancer. Additionally, PCOS patients may have an insulin resistance independent of obesity remaining in a normoglycemic status. At this case, the hypeinsulinemia seems to be the promoter factor not only for the development but also for the cancer progression. However, also increased blood glucose levels are contributing to the growth and carcinogenesis in endometrial cancer and are acting as a critical link between the observed increased cancer risk in patients with type II DM. Therefore, the treatment with insulin-sensitizing agents that act through reducing insulin levels, could offer a general approach to prevent the development of cancer and reduce metastasis The aim of this study was to evaluate the effect of 0.1 mM metformin dose on the proliferative and metastatic potential of endometrial cancer cells, as well as, analyze the effects of short and long-term treatment on intracellular signaling pathways related to endometrial cancer development and progression when exposed to an environment with different glucose concentrations and high insulin levels. Additionally, the endometrial three-dimensional (3D) coculture standardization to remain viable over 20 culture days. The proliferative potential was performed by using CellTitle Glo assay, and the metastatic potential was performed by using transwell migration and invasion assay. The mRNA expression of MKI67, mTOR, NOTCH1, NOTCH3 and JAG1 genes were measured by real time PCR. The cumulative population doubling rate was evaluated to determine the replication behavior of an endometrial cancer cell line throughout 20 days of treatment period. In all assays the cells were cultured in medium containing normal (5.5 mM) or high (17 mM) glucose concentration, and treated in different groups: control, insulin,metformin or combined treatment The 3D coculture model was established by using endometrial primary cells and an endometrium cancer cell line, to the model construction Matrigel® was used as an extracellular matrix. In this study, the 0.1 mM metformin dose potently inhibited the insulin action, decreasing the ability of the endometrial cancer cell line to migrate and invade in a high and normal glucose environment. On the proliferative potential this effect was not observed, however, relative cell proliferation sensitivity to metformin was observed in the range between 1 and 5 mM regardless of the present glucose concentration. In the intracellular molecular mechanisms, it was observed that the high glucose concentration creates an optimal environment for endometrial cancer cells to exhibit a more aggressive genotype and resistance to metformin during a long-term treatment. Moreover, the endometrial 3D coculture model remained viable throughout 20 culture days. Therefore, despite of endometrial cancer cells show resistance to the metformin effect when exposed to high glucose environment, the 0.1 mM metformin dose was able to inhibit the insulin action and decrease the metastatic potential of the cells, suggesting that metformin is acting clinically in combination with indirectly and direct effects could emerge as a potential agent in cancer therapy.
|
208 |
Avaliação do risco de metástases linfonodais no câncer do endométrio, através de parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos / Risk assessment of lymph node metastasis in endometrial cancer through clinical, laboratory, radiological and anatomopathological parameters.Cristina Anton 11 August 2015 (has links)
INTRODUÇÃO: O câncer de endométrio é a sexta neoplasia maligna mais frequente nas mulheres no mundo. Com o crescimento mundial da obesidade, fator associado ao desenvolvimento do câncer de endométrio, estima-se que haja avanço no número de casos da doença. O tratamento cirúrgico do câncer de endométrio inclui a linfadenectomia pélvica e para-aórtica para o conhecimento do status linfonodal utilizado para determinação do tratamento adjuvante segundo a FIGO. Este é um procedimento que requer profissionais com treinamento cirúrgico avançado e não é isento de complicações. Algumas pacientes não se beneficiam da realização sistemática da linfadenectomia. O estudo das características clínicas, laboratoriais, radiológicas e anatomopatológicas das pacientes com câncer de endométrio em nossa população é fundamental para entendermos quais pacientes poderiam prescindir da linfadenectomia. MÉTODOS: Foram avaliadas 408 pacientes atendidas no Instituto do câncer do Estado de São Paulo entre janeiro de 2009 a março de 2015 com diagnóstico de carcinoma de endométrio submetidas ao tratamento cirúrgico. Foram avaliados parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos e sua capacidade de predizer metástases linfonodais. Foram construídas curvas Kaplan Meyer de sobrevivência. Além disso, as complicações relacionadas à realização da linfadenectomia também foram avaliadas. RESULTADOS: Das 405 pacientes elegíveis para o estudo 236(58,3%) foram submetidas à linfadenectomia pélvica e para-aórtica e não foi obtida amostra linfonadal em 73(18%). Os parâmetros significativos predição de acometimento linfonodal obtido através de regressão logística foram infiltração miometrial > 50%, presença de invasão linfovascular, presença de acometimento linfonodal pélvico por exame de imagem e CA125 > 21,5U/mL. A ausência dos quatro parâmetros implica em um risco de acometimento linfonodal de 2,7% enquanto que na presença de todos os quatro parâmetros o risco é de 82,3%. Nas curvas de sobrevida global (p=0,0001) e livre de doença (p=0,0004), a realização da linfadenectomia teve impacto positivo nas pacientes submetidas à linfadenectomia quando comparadas as não submetidas a este procedimento. CONCLUSÕES: A avaliação do risco de metástases linfonodais em pacientes com carcinoma do endométrio, baseadas em parâmetros clínicos, laboratoriais, radiológicos e anatomopatológicos foi capaz de identificar quatro variáveis com significativo valor preditivo de acometimento linfonodal que foram: linfonodos pélvicos pela imagem, CA125 com valor de corte 21,5U/mL, infiltração miometrial e invasão linfovascular. Na presença desses quatro parâmetros a probabilidade de acometimento linfonodal é de 82,3% / BACKGROUND: Endometrial cancer is the sixth most common malignancy in women worldwide. Obesity is a factor associated with this type of cancer development. Thus, the increase of obesity among women leads to a higher number of endometrial cancer cases. The surgical treatment of endometrial cancer includes pelvic lymphadenectomy and para-aortic to the knowledge of lymph node status used for determining the adjuvant treatment according to FIGO. This procedure requires professionals with advanced surgical training and is associated to complication. Moreover, some patients do not benefit from systematic lymphadenectomy. The study of clinical, laboratory, radiological and pathological data of patients with endometrial cancer in our population is critical to understand which patients could dispense lymphadenectomy. METHODS: This study analyzed 408 patients with the diagnosis of endometrial carcinoma undergoing surgical treatment at the Sao Paulo Cancer Institute between January 2009 and March 2015. Clinical, laboratory, radiologic and pathologic parameters were used to test the ability to predict lymph node metastasis. In addition, Kaplan Meyer survival curves were constructed. Complications related to lymphadenectomy were also evaluated. RESULTS: Out of 405 patients eligible for the study, 236 (58.3%) underwent pelvic and para-aortic lymphadenectomy and 73 (18%) had no lymph node samples. Significant parameters prediction of lymph node involvement obtained through logistic regression were myometrium infiltration > 50%, lymphovascular space invasion, pelvic lymph node involvement by imaging and CA125 > 21,5U/mL. The absence of the four parameters implies a risk of lymph node metastasis of 2.7%, whereas in the presence of all four parameters the risk is 82.3%. The overall survival curves (p = 0.0001) and the disease-free survival curves (p = 0.0004), had a positive impact on patients undergoing lymphadenectomy compared to the subject without lymphadenectomy. CONCLUSIONS: The assessment of lymph node metastasis in patients with carcinoma of the endometrial, based on clinical, laboratorial, radiologic and pathologic parameters was able to identify four variables with significant predictive value of lymph node metastasis. Those were pelvic lymph nodes by the image, CA125 > 21,5U/ml, myometrium infiltration > 50% and lymphovascular space invasion. In the presence of these four parameters, the probability of lymph node involvement is 82.3%
|
209 |
Metformin, statins and the risk and prognosis of endometrial cancer in women with type 2 diabetesArima, R. (Reetta) 01 October 2019 (has links)
Abstract
Endometrial cancer (EC) is the fifth most common female cancer worldwide and its incidence is increasing. The prognosis of EC is fairly good. Histologically, ECs are categorized into endometrioid and non-endometrioid subtypes.
Lately, the idea of repurposing existing medications for the prevention and co-treatment of EC has evoked interest in the scientific community. The results of preclinical studies involving various forms of antidiabetic medication (ADM) such as metformin, or cholesterol-lowering statins have been promising.
In the previous epidemiological studies, the results of metformin and/or statin use and the risk and prognosis of EC have indicated either neutral or beneficial effects. At least some of these studies have several limitations, including a potential for several types of bias, and missing information on the dose and timing of medication, cancer-specific mortality or the histology of EC.
The aim of this study was to find reliable further evidence on whether the use of metformin or statins could have beneficial effects on the risk and prognosis of EC in women with type 2 diabetes (T2D). Endometrioid and non-endometrioid EC were analyzed separately based on data from the Finnish Cancer Registry (FCR).
In our study cohort of 92 366 women obtained from a nationwide diabetes database (FinDM) (1996 to 2011), the incidence rates of endometrioid (n = 590 cases) and non-endometrioid (n = 57 cases) EC were not found to differ between metformin users and users of other forms of oral ADM when adjusted for age, duration of T2D and use at any time of other forms of medication under study. We found insufficient evidence that metformin affects the prognosis of patients diagnosed with endometrioid (n = 1215) or non-endometrioid (n = 105) EC (1998 to 2011) after adjusting for year, age and stage at diagnosis of EC, and duration of T2D. However, in patients with endometrioid EC, mortality from other (predominantly cardiovascular) causes of death was decreased in metformin users compared with users of other types of oral ADM. Despite promising preclinical data, we were not able to confirm a beneficial effect of metformin use on the risk or prognosis of EC in women with T2D. In statin users, a lower risk of both EC subtypes and reduced cancer-specific mortality from non-endometrioid EC were observed. / Tiivistelmä
Kohdun runko-osan syöpä on naisten viidenneksi yleisin syöpä, ja todettujen tapauksien määrä kasvaa. Syövän paranemisennuste on melko hyvä. Histologisesti syöpä jaetaan endometrioidi-muotoon ja ei-endometrioidi -muotoon.
Alun perin muihin tarkoituksiin kehitettyjen lääkkeiden käyttö kohdun runko-osan syövän ehkäisyssä ja hoitoyhdistelmissä on ollut viime aikoina tieteellisen mielenkiinnon kohteena. Prekliinisten tutkimusten tulokset diabeteslääke metformiinin ja hyperkolesterolemian hoitoon käytettyjen statiinien osalta ovat olleet lupaavia.
Aiemmissa epidemiologisissa tutkimuksissa metformiinin tai statiinien käytön vaikutukset kohdun runko-osan syövän riskiin ja ennusteeseen ovat olleet vaihtelevia. Osassa tutkimuksista on ollut ongelmia liittyen tilastollisten harhojen riskiin, puutteellisiin tietoihin lääkityksen kestosta ja kumulatiivisista annoksista sekä spesifisestä syöpäkuolleisuudesta ja syövän histologiasta.
Kansalliseen diabetestietokantaan (FinDM) perustuvan tutkimuksemme tavoitteena oli selvittää, onko metformiinin tai statiinien käytöllä (Kelan lääkekorvaustilastot) kohdun runko-osan syövän riskiä vähentävää tai ennustetta parantavaa vaikutusta tyypin 2 diabetesta sairastavilla naisilla. Endometrioidit-syövät ja ei-endometrioidit -syövät analysoitiin erikseen Suomen Syöpärekisterin tietoihin perustuen.
Kohortissamme (n = 92 366) ei todettu eroa endometrioidin (n = 590) tai ei-endometrioidin (n = 57) kohdun runko-osan syövän ilmaantuvuudessa metformiinia tai muita oraalisia diabeteslääkkeitä käyttävien naisten välillä (1996-2011), kun ikä, diabeteksen kesto ja muiden lääkitysten käyttö vakioitiin. Emme löytäneet näyttöä metformiinin käytön yhteydestä syöpäkuolleisuuteen endometrioidissa (n = 1 215) tai ei-endometrioidissa (n = 105) alatyypeissä verrattuna muihin diabeteslääkityksiin (1998-2011), kun ikä, syövän diagnoosivuosi ja levinneisyys sekä diabeteksen kesto vakioitiin. Endometrioidiin syöpään sairastuneilla metformiinia käyttävillä naisilla muu, valtaosalla sydän- ja verisuonitautiperäinen, kuolleisuus oli vähentynyt verrattuna muiden oraalisten diabeteslääkkeiden käyttäjiin. Aiemmista lupaavista tutkimustuloksista huolimatta emme todenneet metformiinilla olevan edullisia vaikutuksia kohdun runko-osan syövän kannalta. Statiinien käyttöön liittyi vähentynyt tämän syövän riski sekä vähentynyt syöpäkuolleisuus ei-endometrioidissa alatyypissä.
|
210 |
Methods for Analysis of Disease Associated Genomic Sequence VariationLovmar, Lovisa January 2004 (has links)
<p>In Molecular Medicine a wide range of methods are applied to analyze the genome to find genetic predictors of human disease. Apart from predisposing disease, genetic variations may also serve as genetic markers in the search for factors underlying complex diseases. Additionally, they provide a means to distinguish between species, analyze evolutionary relationships and subdivide species into strains. </p><p>The development and improvement of laboratory techniques and computational methods was a spin-off effect of the Human Genome Project. The same techniques for analyzing genomic sequence variations may be used independent of organism or source of DNA or RNA. In this thesis, methods for high-throughput analysis of sequence variations were developed, evaluated and applied. </p><p>The performance of several genotyping assays were investigated prior to genotyping 4000 samples in a co-operative genetic epidemiological study. Sequence variations in the estrogen receptor alpha gene were found to be associated with an increased risk of breast and endometrial cancer in Swedish women.</p><p>Whole genome amplification (WGA) enables large scale genetic analysis of sparse amounts of biobanked DNA samples. The performance of two WGA methods was evaluated using four-color minisequencing on tag-arrays. Our in-house developed assay and “array of arrays” format allow up to 80 samples to be analyzed in parallel on a single microscope slide. Multiple displacement amplification by the Φ29 DNA polymerase gave essentially identical genotyping results as genomic DNA. To facilitate accurate method comparisons, a cluster quality assessment approach was established and applied to assess the performance of four commercially available DNA polymerases in the tag-array minisequencing assay. </p><p>A microarray method for genotyping human group A rotavirus (HRV) was developed and applied to an epidemiological survey of infectious HRV strains in Nicaragua. The method combines specific capture of amplified viral sequences on microarrays with genotype-specific DNA-polymerase mediated extension of capture oligonucleotides with fluorescent dNTPs.</p>
|
Page generated in 0.0486 seconds