MEN 2A-related cutaneous lichen amyloidosis: report of three kindred and systematic literature review of clinical, biochemical and molecular characteristics.

Multiple endocrine neoplasia type 2A (MEN2A) may be rarely associated with cutaneous lichen amyloidosis (CLA), a skin lesion located in the interescapular region. Here, we describe 3 MEN2A-related CLA kindred and perform a systematic review (SR) of the literature on clinical, biochemical and molecular characteristics of MEN2A-related CLA patients. Thirty-eight patients with MEN2A-related CLA followed at our institution were evaluated. The median age at MEN2A diagnosis in our cohort was 25 (13-41) years, 68 % were women and all harbored codon 634 RET mutations. The literature search resulted in 20 publications that contributed with 25 MEN2A families and 214 individuals. The mean age of MEN2A diagnosis was 31 ± 17 years, with 77 % women. The mean age reported by patients to initial skin lesion suggestive to CLA was 20 ± 13 years. All but two kindred harbored mutations at codon 634: C634R 7 kindred (35 %), C634Y 5 kindred (25 %), C634W 3 kindred (15 %), C634G 1 kindred (5 %), V804M 1 kindred (5 %) and S891A 1 kindred (5 %). Most interesting, the standardized CLA prevalence was higher in women (2.3/1.0, P < 0.005). The overall reported prevalence of medullary thyroid carcinoma, CLA, pheochromocytoma and hyperparathyroidism was 94, 51, 30 and 16 %, respectively. SR of literature indicates that MEN2A-related CLA is more frequent in women and presents a high penetrance, being the second most frequent manifestation of the syndrome, preceded only by MTC.

Endothelial dysfunction is related to poor glycemic control in adolescents with type 1 diabetes under 5 years of disease: evidence of metabolic memory.

CONTEXT: The relation between endothelial dysfunction (ED), glycemic control, and early type I diabetes mellitus (T1DM) is unclear. OBJECTIVE: The objective of the study was to evaluate the association of ED, glycemic control, and the duration of diabetes in T1DM. DESIGN: This was a cross-sectional study. SETTING: The study was conducted at a public outpatient clinic. PATIENTS: Fifty-seven T1DM adolescents and 10 healthy age-matched controls participated in the study. INTERVENTION: There were no interventions. METHODS AND OUTCOME MEASURES: Endothelial function (ED) was evaluated by flow-mediated dilation (FMD) in the brachial artery after reactive hyperemia. Biochemical data, including HbA1c (glycohemoglobin), high-sensitivity C-reactive protein, lipids, and urinary albumin excretion were collected. Means of four HbA1c values collected at 3-month intervals in the first and second year before FMD analyses were obtained. RESULTS: Mean FMD was decreased in T1DM compared with controls (P = 0.023), independent of age, smoking, hypertension, or dyslipidemia. Twenty-eight of 57 T1DM patients enrolled (49%) had ED. FMD was decreased in microalbuminuric (4.1%) compared with normoalbuminuric patients (10.1%, P = 0.01) and controls (14.6%, P < 0.001). FMD correlated inversely with mean second-year HbA1c (r = -0.426, P = 0.02), particularly in patients with less than 5 yr of T1DM (r = -0.61, P = 0.004). In these patients, high-sensitivity C-reactive protein was strongly correlated with mean first-year HbA1c (r = -0.66, P = 0.0003). In patients with more than 5 yr of T1DM, we found no significant correlations between ED and glycemic control. CONCLUSIONS: Endothelial dysfunction is common in T1DM adolescents with less than 5 yr of disease. It is associated with duration of disease, microalbuminuria, and mean second-year HbA1c but not with mean first-year HbA1c. These data support the metabolic memory hypothesis.

Identification of occult metastases of medullary thyroid carcinoma by calcitonin measurement in washout fluid from fine needle aspiration of cervical lymph node.

Medullary thyroid carcinoma (MTC) may occur sporadically or as a manifestation of an autosomal-dominant inherited syndrome, the multiple endocrine neoplasia type 2. DNA-based RET genotype analysis gained worldwide acceptance in the identification of asymptomatic gene carrier. MTC synthesize and secrete calcitonin, a well established tumor marker and postoperative level of serum calcitonin, indicates whether residual disease was left behind and whether reintervention is necessary. However, management is difficult when routine imaging studies for MTC are negative. This paper brings a report of an illustrative case of a patient with MTC diagnosed by molecular screening, who persisted with detectable levels of serum calcitonin after surgical procedure. After 48 months, an increase in serum calcitonin impelled us to investigate the disease focus. Cervical-US and calcitonin measurement in washout fluid from fine needle aspiration was successfully used to identify MCT metastasis in a lymph node, allowing appropriated reintervention and illustrating the potential clinical applicability of this method.

Identification of occult metastases of medullary thyroid carcinoma by calcitonin measurement in washout fluid from fine needle aspiration of cervical lymph node / Identificação de metástase oculta do carcinoma medular de tireoide através da dosagem de calcitonina no lavado da agulha de punção aspirativa de linfonodo cervical

Medullary thyroid carcinoma (MTC) may occur sporadically or as a manifestation of an autosomal-dominant inherited syndrome, the multiple endocrine neoplasia type 2. DNA-based RET genotype analysis gained worldwide acceptance in the identification of asymptomatic gene carrier. MTC synthesize and secrete calcitonin, a well established tumor marker and postoperative level of serum calcitonin, indicates whether residual disease was left behind and whether reintervention is necessary. However, management is difficult when routine imaging studies for MTC are negative. This paper brings a report of an illustrative case of a patient with MTC diagnosed by molecular screening, who persisted with detectable levels of serum calcitonin after surgical procedure. After 48 months, an increase in serum calcitonin impelled us to investigate the disease focus. Cervical-US and calcitonin measurement in washout fluid from fine needle aspiration was successfully used to identify MCT metastasis in a lymph node, allowing appropriated reintervention and illustrating the potential clinical applicability of this method.

O carcinoma medular de tireoide (CMT) pode ocorrer na forma esporádica ou como manifestação da síndrome genética neoplasia endócrina múltipla tipo 2. Mutações de linhagem germinativa do proto-oncogene RET causam a forma hereditária, e o diagnóstico molecular é a base para o manejo adequado. O CMT sintetiza e secreta a calcitonina e os níveis séricos da calcitonina pós-tireoidectomia indicam se o paciente está curado ou se há necessidade de reintervenção. No entanto, o manejo é difícil quando exames de imagem são negativos. Neste estudo mostramos um caso ilustrativo de uma paciente com CMT hereditário diagnosticado por meio de rastreamento genético que persistiu com calcitonina sérica detectável pós-tireoidectomia. Após 48 meses, observou-se aumento da calcitonina sérica, determinando investigação para localizar o foco da doença. A utilização do US-cervical e a dosagem da calcitonina no lavado da agulha da punção aspirativa de linfonodo possibilitaram o diagnóstico e a reintervenção terapêutica, ilustrando a potencial aplicabilidade clínica desse método.

Pancreatitis as the first manifestation of multiple endocrine neoplasia type 2A / Pancreatite como primeira manifestação de neoplasia endócrina múltipla do tipo 2

Multiple endocrine neoplasia type 2A (MEN2A) is an autosomal dominant inherited condition that predisposes to the triad of medullary thyroid cancer (MTC), pheochromocytoma (Pheo), and primary hyperparathyroidism (PHT). Nearly 100 percent of MEN2A are associated with germ line mutation of the RET proto-oncogene (RET), and DNA-based RET genotype analysis is now considered essential for earlier diagnosis. The first manifestation of MEN2A is most often due to MTC, and less frequently to Pheo. Rarely, MEN2A is recognized during the search for PHT associated conditions. Most patients with primary hyperparathyroidism are asymptomatic, and the focus of the presentation may be the side effects of chronic hypercalcemia, osteoporosis, renal lithiasis, peptic ulcer disease, and hypertension. Hypercalcemic pancreatitis is rare, being an uncommon first manifestation of PHT. Here, we report on a patient who presented recurrent pancreatitis as the first manifestation of MEN2A. In the present case, prompt sequential dosage of calcium, diagnosis of PHT, and genetic analysis would have resulted in pancreatitis prevention and early MEN2A management.

Neoplasia endócrina múltipla do tipo 2 (NEM2A) é uma síndrome genética com herança autossômica dominante, que predispõe à tríade de carcinoma medular de tireóide (CMT), feocromocitoma (Feo) e hiperparatireoidismo primário (HPP). Aproximadamente 100 por cento dos casos de NEM2A estão associados a mutações germinativas do protooncogene RET (RET), e a análise molecular do RET é atualmente considerada essencial para diagnóstico precoce. A primeira manifestação da NEM2A é geralmente em decorrência de CMT, e menos freqüentemente devido ao Feo. Raramente, a NEM2A é descoberta durante investigação para condições associadas ao HPP. A maioria dos pacientes com HPP é oligossintomática e a apresentação ocorre devido a sintomas relacionados à hipercalcemia, à osteoporose, à dispepsia, à hipertensão ou à litíase renal. A pancreatite hipercalcêmica é rara, sendo uma manifestação incomum do HPP. Este artigo relata um caso de paciente que apresentou pancreatite recorrente como primeira manifestação de NEM2A. Neste caso, abordagem seqüencial com determinação do cálcio sérico, diagnóstico de HPP e análise genética poderiam ter resultado prevenção de pancreatite e manejo precoce da NEM2A.

Normal perioperative serum calcitonin levels in patients with advanced medullary thyroid carcinoma: case report and review of the literature.

CONTEXT: Medullary thyroid carcinoma (MTC), a tumor of the parafollicular C cells of the gland, comprises 3-5% of all malignant thyroid neoplasms. Calcitonin, a polypeptidic hormone secreted by the neoplastic cells, is considered a very sensitive and specific MTC tumor marker. Patients with MTC usually present elevated serum calcitonin levels, which correlate with tumor burden and prognosis. OBJECTIVES: To describe a case of advanced MTC with normal serum calcitonin and review the literature on this subject. DESIGN: A case study was performed. INTERVENTION: There were no interventions. PATIENTS: A case of advanced MTC with normal serum calcitonin was studied. RESULTS: Serum calcitonin was measured by two distinct assays, a chemiluminescent immunometric and an in-house two-site monoclonal antibody-based immunofluorometric assay. To rule out a "hook effect," or posttranslational modifications of calcitonin molecule, serum dilutions and tumor immunohistochemistry for calcitonin with the same antibodies used for serum calcitonin measurements were performed. Serum calcitonin levels were within the normal range in both assays, whereas the tumor stained strongly positive for calcitonin. These findings suggest that the tumor was able to produce but not to secrete the calcitonin protein. Five other cases of advanced MTC with normal serum calcitonin levels had been previously reported. CONCLUSIONS: We present an unusual case of advanced MTC with normal serum calcitonin levels. Awareness of MTC cases presenting with normal serum calcitonin levels is important in clinical practice and is particularly relevant to centers that use this test for screening.

Pancreatitis as the first manifestation of multiple endocrine neoplasia type 2A.

Multiple endocrine neoplasia type 2A (MEN2A) is an autosomal dominant inherited condition that predisposes to the triad of medullary thyroid cancer (MTC), pheochromocytoma (Pheo), and primary hyperparathyroidism (PHT). Nearly 100% of MEN2A are associated with germ line mutation of the RET proto-oncogene (RET), and DNA-based RET genotype analysis is now considered essential for earlier diagnosis. The first manifestation of MEN2A is most often due to MTC, and less frequently to Pheo. Rarely, MEN2A is recognized during the search for PHT associated conditions. Most patients with primary hyperparathyroidism are asymptomatic, and the focus of the presentation may be the side effects of chronic hypercalcemia, osteoporosis, renal lithiasis, peptic ulcer disease, and hypertension. Hypercalcemic pancreatitis is rare, being an uncommon first manifestation of PHT. Here, we report on a patient who presented recurrent pancreatitis as the first manifestation of MEN2A. In the present case, prompt sequential dosage of calcium, diagnosis of PHT, and genetic analysis would have resulted in pancreatitis prevention and early MEN2A management.

Neoplasia endócrina múltipla tipo 2 / Multiple endocrine neoplasia type 2

O termo neoplasia endócrina múltipla tipo 2 (NEM 2) foi sugerido em 1968, por Steiner e cols., para diferenciar a síndrome clínica caracterizada pela presença de carcinoma medular de tireóide (CMT), feocromocitoma e hiperparatireoidismo, então denominada síndrome de Sipple, da síndrome de Wermer ou NEM tipo 1, que acomete as glândulas paratireóides, pâncreas e hipófise. Sizemore e cols. (1974) complementaram a diferenciação através da classificação da NEM 2 em 2 subgupos: pacientes com CMT, feocromocitoma, hiperparatireoidismo e aparência normal (NEM 2A) e pacientes sem acometimento das paratireóides e fenótipo caracterizado por ganglioneuromatose intestinal e hábitos marfanóides (NEM 2B). CMT é usualmente o primeiro tumor a ser diagnosticado. O diagnóstico do CMT determina que seja avaliada a extensão da doença e rastreamento do feocromocitoma e hiperparatireoidismo. O diagnóstico de CMT esporádico ou hereditário é realizado através da análise molecular do proto-oncogene RET. Neste artigo são discutidos os aspectos fisiopatológicos, as anormalidades genéticas e os aspectos clínicos da NEM 2. A abordagem diagnóstica e terapêutica nos indivíduos afetados, carreadores assintomáticos e familiares em risco também são discutidos. Os avanços relacionados ao rastreamento genético e intervenção precoce permitiram uma melhoria no prognóstico a longo prazo. No entanto, ainda não dispomos de tratamento eficaz para doença metastática.

[Multiple endocrine neoplasia type 2]. / Neoplasia endócrina múltipla tipo 2.

The term multiple endocrine neoplasia (MEN) was introduced by Steiner et al. in 1968 to describe disorders that include a combination of endocrine tumors. The Wermer syndrome was designed as MEN 1 and the Sipple syndrome as MEN 2. Sizemore et al. (1974) completed that the MEN 2 category included 2 subgroups: patients with medullary thyroid carcinoma (MTC), pheochromocytoma, and parathyroid disease and a normal appearance (MEN 2A) and other without parathyroid disease but with mucosal neuromas and mesodermal abnormalities (MEN 2B). MTC is usually the first tumor diagnosed. The diagnosis of MTC has several implications: disease extent should be evaluated, pheochromocytoma and hyperparathyroidism should be screened and whether the MTC is sporadic or hereditary should be determined by a direct analysis of the RET proto-oncogene. Here, the pathological characteristics, genetic abnormalities, and clinical features of MEN 2 are discussed. The diagnostic and therapeutic approaches used to patients with clinical disease and carriers identified through familiar screening are also described. Progresses related especially to genetic screening and earlier intervention have permitted an improvement in the long-term outcome. However, treatment for disseminated disease is still ineffective.

Rastreamento genético do carcinoma medular de tireóide: identificação de mutações no proto-oncogenese Ret / Genetic screening of medullary thyroid carcinoma: identification of Ret proto-oncogene mutations

O carcinoma medular de tireóide (CMT) pode apresentar-se na forma esporádica (75 por cento) ou hereditária (25 por cento) como componente das síndromes de neoplasia endócrina múltipla (NEM2A e 2B), carcinoma medular de tireóide familiar (CMTF) ou outros. Diferentes mutações no proto-oncogene Ret foram identificadas e estudos recentes sugerem uma correlação entre o genótipo-fenótipo. O presente estudo realizou a análise molecular do Ret em indivíduos com CMT e avaliou a correlação genótipo-fenótipo nos afetados e seus familiares. Foram incluídos 48 indivíduos com diagnóstico histopatológico e imunohistoquímico de CMT, sendo 7 esporádicos e 41 hereditários, provenientes de 14 famílias independentes. DNA genômico foi extraído de leucócitos periféricos e os exons 10, 11, 13, 14 e/ou 16 do Ret amplificados por PCR. As mutações foram identificadas por SSCP, restrição enzimática, e/ou seqüenciamento. Das famílias com CMT hereditário, 7 apresentavam NEM2A, 2 NEM2A associada à líquen amilóide cutâneo (CLA), 2 NEM2B, 2 CMTF e 1 como outros. Em 6 famílias com NEM2A, a mutação estava presente no codon 634, troca de TGC-CGC ou TGC-TAC. Uma família com NEM2A apresentava mutação no codon 618 (TGC-CGC). Ambas famílias com CMTF e nos casos de NEM2A+CLA, a mutação também ocorreu no codon 634 (TGC-CGC). Nos indivíduos afetados com NEM2B foi detectada uma mutação de novo no códon 918 (ATG-ACG). Na família classificada como outros, a mutação localizava-se no códon 634 (TGC-TAC). O diagnóstico molecular identificou mutações em todos os indivíduos com história de doença hereditária, em 8 carreadores sem evidência clínica de neoplasia, e em 2 indivíduos com CMT aparentemente esporádico. Nossos resultados confirmam dados da literatura e demonstram que o rastreamento genético é fundamental na conduta terapêutica.