Splenic vein graft for the reconstruction of the mesenteric-portal trunk after gastroduodenopancreatectomy

Resection of the confluence of the superior mesenteric and portal veins has been performed most frequently in the treatment of adenocarcinoma of the pancreas, in view of the reported positive results, but it can also be used in cases of benign pancreatic neolpasias when they are strongly adhered to the mesenteric-portal trunk. Nevertheless, there is no study on the best type of venous grafts for reconstruction of the mesenteric-portal trunk when required. The choice of graft depends on the preference of the surgeon or the institution. This technical note critically discusses the use of the splenic vein as an option for mesenteric-portal trunk reconstruction after gastroduodenopancreatectomy.

Adenocarcinoma de Células Claras de Endocérvice em Menina de 7 anos

O adenocarcinoma de células claras de colo e vagina em adolescentes é uma doença rara e na maioria das vezes associada com o uso do dietilestilbestrol (DES) durante a gestação. A queixa mais freqüente é o sangramento vaginal irregular que pode ser incorretamente interpretado como vaginite nas crianças e como alterações do eixo hipotálamo-hipófise nas adolescentes. Relatamos o caso de adenocarcinoma de células claras de endocérvice em uma menina de 7 anos de idade atendida no Ambulatório de Ginecologia da Infância e Adolescência, e chamamos a atenção para o diagnóstico de câncer genital que, embora raro nesta faixa etária, deve ser cogitado quando deparamos com sangramento genital em crianças.

Freqüência de Adenocarcinoma de Endométrio em Ambulatório de Histeroscopia: Um Estudo Multicêntrico

Objetivo: realizar um censo sobre a freqüência do adenocarcinoma de endométrio em mulheres submetidas a histeroscopia diagnóstica em cinco serviços brasileiros de vídeo-endoscopia ginecológica localizados em São Paulo, Rio de Janeiro, Salvador, Caxias do Sul e Porto Alegre. Métodos: foram utilizados questionários padronizados com o objetivo de obter as informações sobre a presença de adenocarcinoma, acometimento da cavidade uterina e tipo histológico nos exames histeroscópicos de mulheres na pré e pós-menopausa. Resultados: entre os 6.466 procedimentos histeroscópicos realizados, foi diagnosticado adenocarcinoma de endométrio em 92 pacientes (1,4%), sendo este diagnóstico confirmado pela histologia em 79 casos (1,2%). Para o diagnóstico histeroscópico de adenocarcinoma de endométrio, confirmado por exame histológico, obtivemos sensibilidade de 85,9%, especificidade de 100%, valor preditivo positivo de 100% e valor preditivo negativo de 98,6%. No grupo de 3.845 pacientes na pré-menopausa, o carcinoma foi diagnosticado pela histeroscopia em 9 (0,2%) casos e confirmados pela histologia em 8 (0,2%), ao passo que no outro grupo de 2.621 pacientes na pós-menopausa, a histeroscopia diagnosticou adenocarcinoma em 83 (3,2%) pacientes, dos quais 71 casos (2,7%) foram confirmados pela histologia. Conclusões: este estudo alerta para uma maior preocupação em relação ao câncer de endométrio, especialmente na pós-menopausa, revelando a necessidade de haver mais estudos epidemiológicos para que se possam elaborar programas de prevenção e diagnóstico precoce do adenocarcinoma de endométrio.

Adenocarcinoma viloglandular de cérvice uterina

OBJETIVO: o adenocarcinoma viloglandular (AVG) da cérvice foi identificado como uma variante do adenocarcinoma cervical que ocorre em mulheres jovens e traz um excelente prognóstico. Diante da escassez de estudos relacionados ao tema, nós relatamos seis casos de AVG de cérvice. MÉTODOS: acompanhamos a evolução de seis casos de AVG, no período de 1995 a 2006, no Hospital São Lucas da Pontifícia Universidade Católica do Rio Grande do Sul (PUC-RS). Coletamos informações clínicas e histológicas de todas as pacientes e submetemos todas as peças cirúrgicas para revisão histológica. RESULTADOS: a idade média da apresentação foi de 43,5 anos (variando de 27 a 61 anos). Quatro pacientes submeteram-se à histerectomia radical de Wertheim-Meigs e linfadenectomia pélvica bilateral, uma submeteu-se a conização e subseqüente radioterapia e uma a linfadenectomia pélvica seguida de radioterapia. Todas as pacientes estão vivas e bem, sem evidência de recorrência. CONCLUSÕES: as implicações da terapia são discutidas. Propomos aqui a inclusão do estudo do padrão de envolvimento linfovascular na determinação diagnóstica do AVG. Assim, ao referenciarmos este diagnóstico, poderemos optar, com cautela, pela terapia conservadora, salvo particularidades de cada caso.

Colpocitologia de mulheres com diagnostico de adenocarcinoma do colo do utero

OBJETIVO: Analisar os achados citológicos de mulheres detectadas com adenocarcinoma do colo do útero, levando em conta o histórico da paciente no ano que antecedeu ao diagnóstico e a histopatologia das lesões. MÉTODOS: Este é um estudo comparativo, retrospectivo conduzido com dados de mulheres com adenocarcinoma ou com carcinoma escamoso do colo do útero detectados entre 2002 e 2008. Os laudos da citologia foram sintetizados de acordo com a terminologia Bethesda revisada em 2001 e foram comparados com a histopatologia de adenocarcinoma e de carcinoma escamoso. Foram verificadas as distribuições dos achados citológicos, a concordância global e corrigida pelo acaso com o uso do coeficiente Kappa de Cohen. Para isso, as alterações citológicas foram agregadas de acordo com a origem epitelial, formando os grupos de células glandulares e de células escamosas, tendo como padrão ouro os grupos de tumor histopatologicamente confirmados (adenocarcinoma versus carcinoma escamoso). RESULTADOS: No período, 284 casos de câncer do colo uterino foram diagnosticados. Os casos efetivamente estudados compreenderam 27 e 54 pacientes com adenocarcinoma e com carcinoma escamoso, respectivamente. O grupo de adenocarcinoma representou 9,5% do total diagnosticado, com 56% das mulheres com idade inferior a 50 anos. A coleta da citologia foi feita em média 92 dias antes do diagnóstico do câncer (variação: 19 dias a 310 dias). Em 41,6% dos casos, a citologia que precedeu o diagnóstico do adenocarcinoma foi indicativa de alterações glandulares do tipo adenocarcinoma e atipias de células glandulares. A concordância simples foi de 73,7% e o coeficiente Kappa de 48,7%, sugerindo moderada concordância. CONCLUSÃO: Nesta população, a citologia teve um importante papel no rastreio de mulheres com adenocarcinoma, embora algumas delas tenham sido referidas para esclarecer sintomas clínicos. A concordância entre os achados da citologia e da histopatologia foi moderada.

Purification of bovine pancreatic glucagon as a by-product of insulin production

A process for purifying bovine pancreatic glucagon as a by-product of insulin production is described. The glucagon-containing supernatant from the alkaline crystallization of insulin was precipitated using ammonium sulfate and isoelectric precipitation. The isoelectric precipitate containing glucagon was then purified by ion-exchange chromatography on Q-Sepharose FF, gel filtration on Sephadex G-25 and ion-exchange chromatography on S-Sepharose FF. A pilot scale test was performed with a recovery of 87.6% and a purification factor of 8.78 for the first chromatographic step, a recovery of 75.1% and a purification factor of 3.90 for the second, and a recovery of 76.2% and a purification factor of 2.36 for the last one. The overall yield was 50%, a purification factor of 80.8 was obtained and the fraction containing active glucagon (suitable for pharmaceutical preparations) was 84% pure as analyzed by HPLC

Development of the insulin secretion mechanism in fetal and neonatal rat pancreatic B-cells: response to glucose, K+, theophylline, and carbamylcholine

We studied the development of the insulin secretion mechanism in the pancreas of fetal (19- and 21-day-old), neonatal (3-day-old), and adult (90-day-old) rats in response to stimulation with 8.3 or 16.7 mM glucose, 30 mM K+, 5 mM theophylline (Theo) and 200 µM carbamylcholine (Cch). No effect of glucose or high K+ was observed on the pancreas from 19-day-old fetuses, whereas Theo and Cch significantly increased insulin secretion at this age (82 and 127% above basal levels, respectively). High K+ also failed to alter the insulin secretion in the pancreas from 21-day-old fetuses, whereas 8.3 mM and 16.7 mM glucose significantly stimulated insulin release by 41 and 54% above basal levels, respectively. Similar results were obtained with Theo and Cch. A more marked effect of glucose on insulin secretion was observed in the pancreas of 3-day-old rats, reaching 84 and 179% above basal levels with 8.3 mM and 16.7 mM glucose, respectively. At this age, both Theo and Cch increased insulin secretion to close to two-times basal levels. In islets from adult rats, 8.3 mM and 16.7 mM glucose, Theo, and Cch increased the insulin release by 104, 193, 318 and 396% above basal levels, respectively. These data indicate that pancreatic B-cells from 19-day-old fetuses were already sensitive to stimuli that use either cAMP or IP3 and DAG as second messengers, but insensitive to stimuli such as glucose and high K+ that induce membrane depolarization. The greater effect of glucose on insulin secretion during the neonatal period indicates that this period is crucial for the maturation of the glucose-sensing mechanism in B-cells.

Low levels of sex hormone-binding globulin and hyperproinsulinemia as markers of increased pancreatic ß-cell demand in men

Low levels of sex hormone-binding globulin (SHBG) are considered to be an indirect index of hyperinsulinemia, predicting the later onset of diabetes mellitus type 2. In the insulin resistance state and in the presence of an increased pancreatic ß-cell demand (e.g. obesity) both absolute and relative increases in proinsulin secretion occur. In the present study we investigated the correlation between SHBG and pancreatic ß-cell secretion in men with different body compositions. Eighteen young men (30.0 ± 2.4 years) with normal glucose tolerance and body mass indexes (BMI) ranging from 22.6 to 43.2 kg/m2 were submitted to an oral glucose tolerance test (75 g) and baseline and 120-min blood samples were used to determine insulin, proinsulin and C-peptide by specific immunoassays. Baseline SHBG values were significantly correlated with baseline insulin (r = -0.58, P<0.05), proinsulin (r = -0.47, P<0.05), C-peptide (r = -0.55, P<0.05) and also with proinsulin at 120 min after glucose load (r = -0.58, P<0.05). Stepwise regression analysis revealed that proinsulin values at 120 min were the strongest predictor of SHBG (r = -0.58, P<0.05). When subjects were divided into obese (BMI >28 kg/m2, N = 8) and nonobese (BMI £25 kg/m2, N = 10) groups, significantly lower levels of SHBG were found in the obese subjects. The obese group had significantly higher baseline proinsulin, C-peptide and 120-min proinsulin and insulin levels. For the first time using a specific assay for insulin determination, a strong inverse correlation between insulinemia and SHBG levels was confirmed. The finding of a strong negative correlation between SHBG levels and pancreatic ß-cell secretion, mainly for the 120-min post-glucose load proinsulin levels, reinforces the concept that low SHBG levels are a suitable marker of increased pancreatic ß-cell demand.

Bradykinin enhances membrane electrical activity of pancreatic beta cells in the presence of low glucose concentrations

In most of cells bradykinin (BK) induces intracellular calcium mobilization. In pancreatic beta cells intracellular calcium is a major signal for insulin secretion. In these cells, glucose metabolism yields intracellular ATP which blocks membrane potassium channels. The membrane depolarizes, voltage-dependent Ca2+ channels are activated and the intracellular calcium load allows insulin secretion. Repolarization occurs due to activation of the Ca2+-dependent K+ channel. The insulin secretion depends on the integrity of this oscillatory process (bursts). Therefore, we decided to determine whether BK (100 nM) induces bursts in the presence of a non-stimulatory glucose concentration (5.6 mM). During continuous membrane voltage recording, our results showed that bursts were obtained with 11 mM glucose, blocked with 5.6 mM glucose and recovered with 5.6 mM glucose plus 100 nM BK. Thus, the stimulatory process obtained in the presence of BK and of a non-stimulatory concentration of glucose in the present study suggests that BK may facilitate the action of glucose on beta cell secretion.

Pancreatic nitric oxide and oxygen free radicals in the early stages of streptozotocin-induced diabetes mellitus in the rat

The objective of the present study was to explore the regulatory mechanisms of free radicals during streptozotocin (STZ)-induced pancreatic damage, which may involve nitric oxide (NO) production as a modulator of cellular oxidative stress. Removal of oxygen species by incubating pancreatic tissues in the presence of polyethylene glycol-conjugated superoxide dismutase (PEG-SOD) (1 U/ml) produced a decrease in nitrite levels (42%) and NO synthase (NOS) activity (50%) in diabetic but not in control samples. When NO production was blocked by N G-monomethyl-L-arginine (L-NMMA) (600 µM), SOD activity increased (15.21 ± 1.23 vs 24.40 ± 2.01 U/mg dry weight). The increase was abolished when the NO donor, spermine nonoate, was added to the incubating medium (13.2 ± 1.32). Lipid peroxidation was lower in diabetic tissues when PEG-SOD was added (0.40 ± 0.02 vs 0.20 ± 0.03 nmol/mg protein), and when L-NMMA blocked NOS activity in the incubating medium (0.28 ± 0.05); spermine nonoate (100 µM) abolished the decrease in lipoperoxide level (0.70 ± 0.02). We conclude that removal of oxygen species produces a decrease in pancreatic NO and NOS levels in STZ-treated rats. Moreover, inhibition of NOS activity produces an increase in SOD activity and a decrease in lipoperoxidation in diabetic pancreatic tissues. Oxidative stress and NO pathway are related and seem to modulate each other in acute STZ-induced diabetic pancreas in the rat.

Curcumin induces human HT-29 colon adenocarcinoma cell apoptosis by activating p53 and regulating apoptosis-related protein expression

Curcumin, a major yellow pigment and active component of turmeric, has multiple anti-cancer properties. However, its molecular targets and mechanisms of action on human colon adenocarcinoma cells are unknown. In the present study, we examined the effects of curcumin on the proliferation of human colon adenocarcinoma HT-29 cells by the 3-[4,5-dimethylthiazol-2-yl]-2,5-diphenyltetrazolium bromide method and confirmed the curcumin-induced apoptosis by morphology and DNA ladder formation. At the same time, p53, phospho-p53 (Ser15), and other apoptosis-related proteins such as Bax, Bcl-2, Bcl-xL, pro-caspase-3, and pro-caspase-9 were determined by Western blot analysis. The colon adenocarcinoma cells were treated with curcumin (0-75 µM) for 0-24 h. We observed that p53 was highly expressed in HT-29 cells and curcumin could up-regulate the serine phosphorylation of p53 in a time- and concentration-dependent manner. An increase in expression of the pro-apoptotic factor Bax and a decrease in expression of the anti-apoptotic factor Bcl-2 were also observed in a time-dependent manner after exposure of 50 µM curcumin, while the expression of the anti-apoptotic factor Bcl-xL was unchanged. Curcumin could also down-regulate the expression of pro-caspase-3 and pro-caspase-9 in a time-dependent manner. These data suggest a possible underlying molecular mechanism whereby curcumin could induce the apoptosis signaling pathway in human HT-29 colon adenocarcinoma cells by p53 activation and by the regulation of apoptosis-related proteins. This property of curcumin suggests that it could have a possible therapeutic potential in colon adenocarcinoma patients.

Ca2+ signaling in pancreatic acinar cells: physiology and pathophysiology

The pancreatic acinar cell is a classical model for studies of secretion and signal transduction mechanisms. Because of the extensive endoplasmic reticulum and the large granular compartment, it has been possible - by direct measurements - to obtain considerable insights into intracellular Ca2+ handling under both normal and pathological conditions. Recent studies have also revealed important characteristics of stimulus-secretion coupling mechanisms in isolated human pancreatic acinar cells. The acinar cells are potentially dangerous because of the high intra-granular concentration of proteases, which become inappropriately activated in the human disease acute pancreatitis. This disease is due to toxic Ca2+ signals generated by excessive liberation of Ca2+ from both the endoplasmic reticulum and the secretory granules.

Reduced pancreatic β-cell mass is associated with decreased FoxO1 and Erk1/2 protein phosphorylation in low-protein malnourished rats

A low-protein diet leads to functional and structural pancreatic islet alterations, including islet hypotrophy. Insulin-signaling pathways are involved in several adaptive responses by pancreatic islets. We determined the levels of some insulin-signaling proteins related to pancreatic islet function and growth in malnourished rats. Adult male Wistar rats (N = 20 per group) were fed a 17% protein (normal-protein diet; NP) or 6% protein (low-protein diet; LP), for 8 weeks. At the end of this period, blood glucose and serum insulin and albumin levels were measured. The morphometric parameters of the endocrine pancreas and the content of some proteins in islet lysates were determined. The β-cell mass was significantly reduced (≅65%) in normoglycemic but hypoinsulinemic LP rats compared to NP rats. Associated with these alterations, a significant 30% reduction in insulin receptor substrate-1 and a 70% increase in insulin receptor substrate-2 protein content were observed in LP islets compared to NP islets. The phosphorylated serine-threonine protein kinase (pAkt)/Akt protein ratio was similar in LP and NP islets. The phosphorylated forkhead-O1 (pFoxO1)/FoxO1 protein ratio was decreased by 43% in LP islets compared to NP islets (P < 0.05). Finally, the ratio of phosphorylated-extracellular signal-related kinase 1/2 (pErk1/2) to total Erk1/2 protein levels was decreased by 71% in LP islets compared to NP islets (P < 0.05). Therefore, the reduced β-cell mass observed in LP rats is associated with the reduction of phosphorylation in mitogenic-related signals, FoxO1 and Erk proteins. The cause/effect basis of this association remains to be determined.