Chirurgische Konzepte und Strategien bei Kolonadenomen und Polyposissyndromen / Surgical Approach and Strategies in Colon Adenomas and Polyposis Syndromes

Pistorius, Steffen, Wehrmann, Ursula, Teichert, Eva-Maria, Saeger, Hans-Detlev

17 February 2014

Die Entwicklung moderner minimal-invasiver Diagnose- und Behandlungsverfahren auf dem Gebiet der kolorektalen Adenome und Karzinome ermöglicht eine effektive Überwachung von Risikopersonen, andererseits erfolgt durch die endoskopische Abtragung oder transanale bzw. TEM-technische Resektion von Adenomen bereits eine erhebliche Karzinomprävention. Die Einführung der laparoskopischen Technik bei der Resektion kolorektaler Tumoren könnte nach Evaluierung der bisherigen Ergebnisse zu einer weiteren Verringerung der Hospitalisierung und operationsassoziierten Morbidität der Patienten bei gleicher Prognose führen. Kennzeichnend für familiäre Formen des kolorektalen Karzinoms ist das hohe Risiko für die Entwicklung kolorektaler Tumoren, jedoch auch für weitere extrakolonische Neoplasien. Dies trifft für das hereditäre Nicht-Polyposis-assoziierte kolorektale Karzinom (HNPCC), die familiäre Polyposis (FAP) und die selteneren Formen wie Peutz-Jeghers-Syndrom und juvenile Polyposis zu. Die Anwendung der molekularen Diagnostik in diesen Familien ermöglicht durch die Identifizierung von Mutationsträgern und Nichtmutationsträgern einerseits die gezielte Eingliederung von Hochrisikopersonen (Mutationsträgern) in spezielle, auf das jeweilige Syndrom zugeschnittene Überwachungs- und Vorsorgeprogramme und erspart andererseits Personen mit durchschnittlichem Risiko (Nichtmutationsträgern) unnötige und teilweise invasive Diagnostik. Bezüglich des chirurgischen Vorgehens bei Patienten mit einer Form des hereditären kolorektalen Karzinoms gibt es bereits etablierte Verfahren, wie die Durchführung einer restaurativen Proktokolektomie bei der FAP, bei anderen Formen, wie bei HNPCC, sind diese noch in der Diskussion. Wesentliche Fortschritte bei der Prävention kolorektaler Tumoren sind in den nächsten Jahren möglicherweise auf dem Gebiet der Chemoprävention zu erwarten. / Development of modern, minimally invasive methods for diagnosis and treatment in the field of colorectal tumours enables an effective surveillance for persons at high risk as well as a distinct cancer prevention by endoscopic, transanal or TEM removal of colorectal adenomas. Introduction of laparoscopic techniques in the resection of colorectal tumours could entail, after evaluation of preliminary results, a decreased duration of hospitalisation and procedure-associated morbidity in patients with the same prognosis. The very high risk for development of colorectal tumours as well as for some extracolonic neoplasia is typical for familial colorectal cancer syndromes. This concerns hereditary nonpolyposis colorectal cancer (HNPCC) syndrome, familial polyposis coli, and the infrequent forms like Peutz-Jeghers syndrome and juvenile polyposis. Molecular diagnostics has the power to identify carriers and noncarriers of a mutated gene in these families and therefore may permit clear-cut decisions regarding inclusion in special surveillance programmes, which is recommended for all persons at risk from affected families. Concerning the surgical approach in patients with hereditary colorectal cancer, well-accepted routine procedures like restorative proctocolectomy in familiar polyposis patients have already been established; in other forms like HNPCC the best surgical modality is still under discussion. Remarkable progress in the prevention of colorectal tumours could be expected from chemoprevention trials in the next years. / Dieser Beitrag ist mit Zustimmung des Rechteinhabers aufgrund einer (DFG-geförderten) Allianz- bzw. Nationallizenz frei zugänglich.

Kolorektales Karzinom

hereditäre Formen

Prävention

Überwachung

chirurgisches Vorgehen

Colorectal cancer

hereditary forms

prevention

surveillance

surgical approach

ddc:610

rvk:XA 10000

Hereditäre kolorektale Karzinome – Überlegung zu präventiven chirurgischen Maßnahmen

Pistorius, Steffen, Schackert, Hans K., Saeger, Hans-Detlev

26 February 2014

Hereditary Colorectal Carcinomas – Reflection on Preventive Surgery Hereditary Nonpolyposis Colorectal Cancer (HNPCC) accounts for about 5% of all colorectal cancers and is the most frequent familial form; familial adenomatous polyposis coli accounts for about 1%. Prerequisitive for individually tailored surveillance is the identification of the pathogenic germline mutation. In classical FAP, surgical standard is a restorative proctocolectomy while in HNPCC there is no surgical standard other than standard oncological resection due to missing evidence. In HNPCC, prophylactic colectomy before the onset of the first colorectal cancer is not recommended. Main arguments for the extension of the resection in the case of the first colorectal carcinoma in HNPCC are the rate of metachronous colorectal carcinomas of 40–45% in a 10-year interval and rapid tumor progression. In HNPCC, in the case of first colon cancer a subtotal colectomy seems to be indicated. A proctocolectomy or, if indicated, a restorative proctocolectomy may be considered in the case of carcinomas in the lower rectum. These considerations should be evaluated in a prospective clinical trial. Counselling, molecular diagnosis and surgery in patients with hereditary colorectal cancers should only be performed in interdisciplinary centers. / Das «Hereditary Nonpolyposis Colorectal Cancer» (HNPCC)-Syndrom bildet mit zirka 5% aller kolorektalen Karzinome die größte Gruppe der familiären Formen; die familiäre adenomatöse Polyposis coli (FAP) macht zirka 1% aus. Voraussetzung für die Indikationsstellung zu individuellen Vorsorgeprogrammen ist die Identifizierung der pathogenen Keimbahnmutation. Bei der klassischen FAP ist die Durchführung einer restaurativen Proktokolektomie die Therapie der Wahl, beim HNPCC-Syndrom gibt es aufgrund fehlender Daten klinischer Studien noch keinen Operationsstandard, der über eine Resektion entsprechend den onkologischen Resektionsprinzipien hinausgeht. Eine prophylaktische Kolektomie vor Manifestation eines kolorektalen Karzinoms bei HNPCC kann bei der gegenwärtigen Datenlage nicht empfohlen werden. Hauptargumente für die Erweiterung des Eingriffs bei manifestem kolorektalem Karzinom bei HNPCC-Patienten sind das Risiko metachroner kolorektaler Karzinome von 40–45% in einem Zeitraum von 10 Jahren und die rasche Tumorprogression. Bei Erstmanifestation eines Kolonkarzinoms erscheint die Durchführung einer subtotalen Kolektomie indiziert. Bei Erstmanifestation des Karzinoms im unteren Rektumdrittel ist die Durchführung einer Proktokolektomie bzw. unter entsprechenden onkologischen und funktionellen Voraussetzungen eine Kolektomie mit Proktomukosektomie und Ileum-Pouch zu erwägen. Die Evaluierung dieser Überlegungen sollte im Rahmen einer prospektiven klinischen Studie erfolgen. Die Beratung, molekulare Diagnostik und chirurgische Therapie von Patienten mit hereditären kolorektalen Karzinomen sollte zunächst nur entsprechenden interdisziplinären Zentren vorbehalten bleiben. / Dieser Beitrag ist mit Zustimmung des Rechteinhabers aufgrund einer (DFG-geförderten) Allianz- bzw. Nationallizenz frei zugänglich.

Hereditäre kolorektale Karzinome

Molekulare Diagnostik

Präventive Chirurgie

Hereditary colorectal carcinomas

Molecular diagnosis

Preventive surgery

ddc:610

rvk:XA 10000

Hand function in children and in persons with neurological disorders : aspects of movement control and evaluation of measurements

Svensson, Elisabeth

January 2009

Hand function is of great importance in the many daily activities that require well-coordinated hand and arm movements. Measurement of hand function is an essential element in the rehabilitation process, in order to facilitate medical diagnosis and determine developmental stages, functional levels, and the efficacy of treatment interventions. Basic requirements for any measurement used in clinics are that they are easy to use, relevant to the function being assessed, and valid and reliable. When scrutinizing the literature on hand function, important gaps were found with regard to measurement. For example, the reliability of grip strength with the Grippit in children has yet to be determined, and there are few evaluations of hand function measurements in Charcot-Marie-Tooth disease (CMT). Furthermore, laboratory measurements of hand function, which have the potential to provide more detailed information and insight into hand control, such as the role of the cerebellum in reactive grip control – have not been fully explored. The overall aim of the thesis was to achieve more knowledge on hand function; on the evaluation of measurements in different target populations; and on movement control of the hand. In the first study, the aim was to evaluate the test-retest reliability of the peak and sustained grip strength with Grippit in a sample of healthy children (n=58, 6-, 10- and 14-y-olds). This was followed by two studies examining hand function in an adult sample (n=20) diagnosed with CMT. The test-retest reliability of grip and pinch strength using Grippit, sensation with the Shape Texture Identification test (STI) and dexterity with the Box and Block Test (BBT) and Nine-Hole Peg test (NHP) were studied. The impact of the disease on daily life, measured with the Disability of the Arm, Shoulder and Hand questionnaire (DASH), and correlations between disability and various aspects of hand function, were also explored in this condition. The aim of the fourth study was to examine grip force response to unpredictable loadings of an object held in a pinch grip in subjects (n=9, 22-48 yrs) who had been diagnosed with a cerebellar lesion, compared with a healthy control group (n=11). The first study showed that test-retest reliability was good for both peak and sustained grip strength in healthy children. The mean and best of three trials were equally reliable, but differences in reliability were detected within different age groups. For example, the peak grip strength, best of three trials, was more reliable for the 6-y-olds (intraclass correlation coefficient (ICC)=0.96, standard error of measurement in percentage (SEM%)=6.3) and 14-y-olds (ICC=0.96, SEM%=5.2) compared with the 10-y-olds (ICC=0.78, SEM%=12.5). In the second study, evaluating measurements of hand function in subjects with CMT, grip strength proved to be reliable (ICC=0.99, coefficient of repeatability (CR)=26.7 N, coefficient of variation (CV)=6.6 %), but pinch strength was less reliable. The reliability was also good for the BBT (ICC=0.95, CR=11.5 blocks/min, CV=8.4%) and the NHP (ICC=0.99, CR=4.3 s, CV=3.9 %). However, a bias towards higher values was noted on the second test occasion with the BBT. The reliability of the STI test (kappa=0.87) was also very good in subjects with CMT. A limitation in this latter test was noted in terms of its ability to describe subjects either performing very well or very poorly. The results of the third study showed that hand function in CMT was reduced (p<0.001) to about 60% of that in healthy controls in each of the separate outcome measures, as well as by a constructed summary index of hand function. The median DASH score was 38.8 (range 0-66.7) and was clearly related to hand function (r=0.64-0.83). The results of the final study in subjects with cerebellar lesions showed that the ipsilateral hand had delayed and more variable response latencies e.g. 278±166 ms for loads delivered at 2 N/s, compared with healthy subjects (HS) 80±53 ms (p=0.005). The cerebellar subjects also used a higher pre-load grip force with the ipsilateral hand (1.6±0.8 N) than the HS (1.3±0.6 N (p=0.017)). Even the contralateral hand in subjects with unilateral cerebellar stroke showed a delayed onset of the grip response. In conclusion: Grip strength assessment in children with Grippit results in good reliability for peak and sustained grip strength, although the 10-y-olds were less reliable. In CMT the tested instruments can all be used to evaluate hand function, but certain factors, such as the number of trials used should be taken into consideration. The CMT subjects’ hand function was reduced and correlated with their self-experienced disability. However, clinicians should be aware that patients might score lower than expected on DASH, possibly due to a long process of adaptation. Cerebellar lesions can impair the reactive grip control in both the ipsilateral and the contralateral hand. These investigations have thus, as intended increased the knowledge of hand function. The studies have evaluated some measurements in different samples, which will help clinicians testing hand function.

cerebellum

disability

hand function

latency

motor control

reactive control

reproducibility

sensation

strength

Physiotherapy

Sjukgymnastik/fysioterapi

DNA nucleotide excision repair gene single nucleotide polymorphisms and hereditary nonpolyposis colorectal cancer.

Zhang, Nianxiang. Frazier, Marsha L. Kapadia, Asha Seth, Hardy, Robert J. Amos, Christopher I. Fu, Yun-Xin.

January 2007

Thesis (M.S.)--University of Texas Health Science Center at Houston, School of Public Health, 2007. / Source: Masters Abstracts International, Volume: 46-01, page: 0238. Adviser: Marsha Frazier. Includes bibliographical references.

CRISPR-Cas9 Mediated Restoration of Dystrophin Expression and Inhibition of Myostatin: A Novel Gene Therapy for Duchenne Muscular Dystrophy

Rangan, Apoorva

01 January 2016

Duchenne Muscular Dystrophy (DMD) is an X-linked recessive genetic disease, caused by a frame-shift mutation in the dystrophin gene. Current gene therapies for DMD target dystrophin transcripts in existing skeletal and cardiac muscle, rather than adipose and fibrotic tissues. These approaches may be unable to repair muscle functionality in DMD patients who have already undergone extensive muscle damage and wasting. Thus, successful DMD therapies must consider the underlying genetic cause and pathology. Inhibition of the gene myostatin, a negative regulator of muscle growth, has been shown to ameliorate muscle loss. Here, the CRISPR-Cas9 gene-editing platform is proposed to restore dystrophin expression and inhibit myostatin as a novel gene therapy in DMD patient derived induced pluripotent stem cells. Successful CRISPR-Cas9 mediated gene editing would be determined using PCR amplification, western blot analysis, immunofluorescence staining, and off target sequence analysis in differentiated skeletal muscle cells.

DMD

Myostatin

CRISPR-Cas9

Gene Therapy

Duchenne Muscular Dystrophy

Dystrophin

Biology

Musculoskeletal Diseases

Estudo da miotonia hereditária em suínos

Araújo, César Erineudo Tavares de.

January 2018

Orientador: Alexandre Secorun Borges / Resumo: A principal causa de miotonia não distrófica hereditária ocorre devido à mutações no gene CLCN1, codificante para a proteína CLC1 que forma o canal iônico seletivo para o íon cloreto predominante no tecido muscular esquelético. Mutações no gene CLCN1 foram descritas como causadoras de miotomia hereditária em humanos e em várias espécies animais. Não existe descrição de miotonia hereditária na espécie suína. O objetivo deste estudo foi realizar a caracterização clínica e molecular de uma forma de miotonia hereditária em suínos. A hipótese desse estudo foi que animais com sinais clínicos compatíveis apresentavam a miotonia hereditária. Esses animais foram avaliados sob aspectos clínicos, eletromiográficos, histopatológicos e moleculares. Os sinais clínicos verificados foram hipertrofia e rigidez musculares, miotonia com startle response formação de dimples e fenômeno warm-up evidentes. Não foi constatada distrofia muscular ao exame histopatológico. Ao exame eletromiográfico foram demonstradas descargas miotônicas clássicas com formação de som característico diver bomb. A nível molecular foi verificada a ausência dos nucleotídeos referentes aos éxons 15 e 16 utilizando amostras de cDNA dos animais afetados. No DNA genômico foi encontrada uma grande deleção de 4165pb (g. NC_010460.4 del 6912538_6916702) na região do gene CLCN1. Análises de expressão relativa demonstraram níveis de expressão em tecido muscular de animais wild type para um transcrito associado a miotonia hereditári... (Resumo completo, clicar acesso eletrônico abaixo) / Abstract: The major cause of hereditary non-dystrophic myotonia occurs due to mutations in the CLCN1 gene, coding for the CLC1 protein that forms the ionic channel selective for the predominant chloride ion in skeletal muscle tissue. The resulting hereditary disease is called congenital myotonia in human medicine. Mutations in the CLCN1 gene have been described as causing hereditary myotomy in several animal species, but in the swine species, no mutation in this gene has been described. The objective of this study was to perform the clinical and molecular characterization of hereditary myotonia in swine. The hypothesis of this study was that animals with compatible clinical signs had hereditary myotonia. These animals were evaluated under clinical, electromyographic, histopathological and molecular aspects. The clinical signs verifed were muscular hypertrophy and stifness, myotonia with startle response and formation of dimples. The phenomenon warm-up was evident. No muscular dystrophy was observed at the histopathological examination. Electromyographic examination showed classic myotonic discharges with characteristic sound. At the molecular level, the absence of nucleotides from exons 15 and 16 was verifed using cDNA samples of afected animals. In genomic DNA a large deletion of 4165bp (g NC_010460.4 del 6912538_6916702) was found in the region of the CLCN1 gene. Relative expression analyzes demonstrated expression levels of wild type animals for a transcript associated with heredita... (Complete abstract click electronic access below) / Doutor

Doença muscular

Canalopatia

Canal de cloro

Doença hereditária

Deleção

voluntary muscle disorder

channelopathy

chloride channel

hereditary disease

deletion

Avaliação estrutural e diagnóstica de três lesões fibrosas da cavidade bucal

Badauy, Cristiano Macabú

January 2008

O objetivo do presente trabalho é analisar os componentes celulares e de fibras do tecido conjuntivo nas hiperplasias inflamatórias (HI), nos fibromas (F) e na fibromatose gengival hereditária (FGH), além de investigar a imunocompetência e efetuar análises moleculares de pacientes com FGH. Para atingir os objetivos foram desenvolvidos 4 artigos, com diferentes metodologias e universos amostrais. No 1º artigo, pretendeu-se estabelecer critérios microscópicos válidos para diferenciar F e HI. Foram avaliadas em microscópio óptico 136 lesões coradas pela Hematoxilina-eosina (HE) e pelo Tricrômico de Masson quanto às características microscópicas. Os resultados mostraram que uma área central de fibras colágenas dispostas de forma enovelada e mais densa, circundada por uma camada de fibras dispostas de forma paralela são características dos F, enquanto a presença de hiperplasia epitelial, infiltrado inflamatório e fibras colágenas organizadas de forma paralela são características das HI. Tais resultados motivaram o 2º artigo, no qual estudamos 18 lesões de F e 13 de HI, que foram preparadas histologicamente e coradas pelo picrosírius red e pelo direct blue para avaliação quantitativa das fibras colágenas e de fibras do sistema elástico, respectivamente, em microscopia a laser confocal. Os resultados confirmaram a disposição estrutural das fibras colágenas observada no 1º artigo, além de apontarem diferenças nas áreas ocupadas pelas fibras colágenas em todas as regiões estudadas. A fim de proceder a uma avaliação dos componentes fibroso e celular das 3 lesões fibrosas, foi desenvolvido o 3º artigo. Espécimes das 3 lesões foram estudados em microscopia ótica, a fim de avaliar suas populações de fibroblastos e de células inflamatórias e os seguintes componentes fibrosos do tecido conjuntivo: fibras colágenas, sistema de fibras elásticas, fibras reticulares e fibras oxitalânicas. Os resultados mostraram disposição e concentração diferente das fibras colágenas nas 3 lesões e uma maior concentração de fibras reticulares na FGH. A análise dos componentes celulares mostrou um maior número de fibroblastos no F e uma maior contagem de células inflamatórias na HI. A partir do encaminhamento de uma família com FGH, optouse por inclui-la no estudo, tendo em vista serem lesões do mesmo grupo. Com isso, foi desenvolvido um 4º estudo, que utilizou uma avaliação morfológica semelhante à dos 2 artigos anteriormente descritos. Dos pacientes com FGH foi obtido sangue periférico para avaliação da proliferação celular de linfócitos através do teste do MTT e para o sequenciamento do gene SOS-1. Os resultados mostraram hiperplasia epitelial na porção externa da gengiva dos pacientes com FGH, maior concentração de fibras colágenas e poucas células inflamatórias. Os 3 pacientes com FGH não mostraram diferenças no seu índice de proliferação de linfócitos em relação aos controles e não apresentaram a mutação descrita no gene SOS-1 de outras famílias com FGH. Pode se concluir que as 3 lesões apresentam estrutura conjuntiva diferente tanto no aspecto quantitativo quanto na disposição estrutural de seus componentes. / The objective of this study was to analyze the cellular and fibrous components of connective tissue in inflammatory hyperplasia (IH), oral fibroma (OF) and hereditary gingival fibromatosis (HGF), and to investigate the immunocompetence and to perform molecular analysis in HGF patients. To achieve the goals were developed 4 articles, with different methodologies and sample universes. In the 1st article, we intended to establish microscopic criteria to differentiate F and IH. The microscopic characteristics of the lesions (n=136) stained by hematoxylin-eosin (HE) and Masson trichrome were evaluated in an optical microscope. The results showed that a central area of wound collagen fibers and arranged in a higher density, surrounded by a layer of parallel fibers are characteristic of F, while the presence of epithelial hyperplasia, inflammatory infiltrate and parallel collagen fibers are characteristics of HI. These results led the 2nd article, which studied 18 F and 13 and IH, histologically prepared and stained by picrosírius red and direct blue for the direct quantitative assessment of collagen fibers and elastic fibers of the system, respectively, in the confocal laser microscope. The results confirmed the structural arrangement of collagen fibers found in Article 1, and indicate differences in the areas of collagen fibers in all regions studied. In order to evaluate the cellular and fibrous components of the 3 fibrous lesions, was developed the 3rd article. Specimens of the 3 lesions were studied in optical microscopy, to assess their populations of fibroblasts and inflammatory cells and the following components of fibrous connective tissue: collagen fibers, elastic fiber system, reticular fibers and oxytalan fibers. The results showed different arrangement and concentration of collagen fibers in the 3 lesions and a higher concentration of reticular fibers in HGF. The analysis of cellular components showed a greater number of fibroblasts in F and a higher count of inflammatory cells in IH. With the identification of a family with HGF, we chose to include it in the study because the lesions belong to the group of benign fibrous lesions. With that, it developed a 4th study, which used a similar morphologic evaluation of the 2 articles described above. Periferic blood was extracted from the HGF patients in order to determine the proliferative capacity of the peripheral lymphocytes, by the MTT test, and in order to sequence the SOS1 gene. The 3 HGF affected patients did not present the described mutation for the SOS1 gene, and the lymphocyte proliferative capacity in HGF patients was similar to those on controls. The results showed epithelial hyperplasia in the outer portion of the gingiva of patients with HGF, greater concentration of collagen fibers and few inflammatory cells. We can conclude that the 3 lesions present a different connective structure, considering both the quantitative aspect and the architectural disposition of their components.

Patologia bucal

Mucosa bucal : Doencas

Inflammatory hyperplasia

Oral fibroma

Hereditary gingival fibromatosis

Collagen fibers

Reticular fibers

Fibroblasts

Lymphocytes

Cellular proliferation

Caracterização de pacientes com diagnóstico de retinoblastoma identificados nos Serviços de Oncologia Pediátrica, Oftalmologia e Genética no Hospital de Clínicas de Porto Alegre/RS

Selistre, Simone Geiger de Almeida

January 2013

Retinoblastoma (Rb) é o tumor ocular mais frequente na infância e cada grande Centro deve conhecer o perfil dos seus pacientes. Foi realizado um estudo do tipo coorte retrospectivo e incluiu pacientes com Rb atendidos entre 1983 e 2012 nos Serviços de Oncologia Pediátrica, Oftalmologia e Genética Médica do Hospital de Clínicas de Porto Alegre (HCPA). De um total de 165 registros no período foram efetivamente incluídos 140 pacientes, sendo 95,0% destes provenientes de municípios do Rio Grande do Sul. Os sinais mais frequentes ao diagnóstico foram: leucocoria (73,6%) e estrabismo (20,7%). Identificamos a seguinte distribuição: doença unilateral (65,0%), bilateral (32,9%) sendo 80,4% com doença multifocal (p=0,015), trilateral (2,1%). A idade média dos pacientes por ocasião dos primeiros sinais e sintomas foi de 18,1 meses [mediana=12,0] e a idade média ao diagnóstico foi 23,5 meses [mediana=16,5]. Cinquenta pacientes (35,7%) foram diagnosticados no 1º ano de vida. O tempo de diagnóstico médio da coorte foi 5,4 meses [mediana=3,0], (amplitude=0-77,0). A idade média aos primeiros sinais e sintomas do grupo com critérios de hereditariedade foi de 12,3 meses enquanto a do grupo não hereditário foi de 21,6 meses (p=0,001), enquanto a idade média ao diagnóstico foi de 15,9 meses vs. 28 meses, respectivamente (p<0,001). Entretanto não houve diferença na sobrevida entre esses subgrupos. O estadiamento ocular dos pacientes ao diagnóstico na sua maioria foi avançado (classificação de Reese V em 76,5%, Internacional D ou E em 78,1%), sendo que 35,2% dos unilaterais e 34,8% dos bilaterais já apresentavam doença extraocular em pelo menos um olho ao diagnóstico. Quinze pacientes (10,7%) tinham doença metastática ao diagnóstico. Em relação ao tratamento, diferentes modalidades foram utilizadas, sendo a maioria dos pacientes submetidos à cirurgia, sendo esta enucleação em 88,1% e exenteração em 11,9%. Uma parcela significativa dos pacientes foi tratada com quimioterapia sistêmica (57,1%) e/ou radioterapia (37,1%). Do total de pacientes recrutados, 131 (93,6%) permaneceram vinculados ao hospital até 2012 ou até o óbito. Destes, 32 (22,9%) recidivaram, resultando em 19 óbitos com 84,2% por progressão do Rb. Uma segunda neoplasia primária esteve presente em 4,3% (N=6) e dentre esses, um paciente teve uma terceira neoplasia primária. O tempo de seguimento médio foi 323,2 meses [300,3; 346,1]. As sobrevidas nos diferentes subgrupos foram as seguintes: sobrevida global 86,4%; no não metastático 92,0%; no metastático 40,0%; entre os intraoculares 94,0%; entre os extraoculares 68,5%; entre os unilaterais e bilaterais ambos com cerca de 88,0%; entre os trilaterais (N=3) todos foram a óbito; entre os unilaterais intraoculares 94,9% e extraoculares 75,0% e entre os bilaterais intraoculares 94,5% e extraoculares 68,4%. No nosso meio, o diagnóstico de Rb ainda é feito predominantemente em estadios avançados o que reduz a sobrevida dos pacientes e o índice de preservação do olho e da visão, além de aumentar a intensidade dos tratamentos realizados e consequentemente, toxicidade e efeitos tardios destes. Avaliações clínicas e oftalmológicas periódicas nos primeiros anos de vida da criança oferecem maior oportunidade de um diagnóstico precoce e o encaminhamento rápido à um Centro de Referência multidisciplinar que contemple cuidados terciários em Oftalmologia e Oncologia Pediátrica é fundamental. Existe grande necessidade de investimentos regionais que facilitem o acesso ao diagnóstico e tratamento do Rb, o tumor ocular mais frequente na infância. / Retinoblastoma (Rb) is the most frequent ocular tumor diagnosed in children and every pediatric hospital must be familiar with its clinical presentation and patient characteristics. A retrospective cohort study was undertaken, with patients diagnosed with retinoblastoma from 1983 until 2012, treated at the Pediatric Oncology Unit, Ophthalmology Unit, and Medical Genetics Unit of the Hospital de Clínicas de Porto Alegre (HCPA). Of a total of 165 registries during this time frame, 140 patients were included in this study, with 95% of them from the state of Rio Grande do Sul. The most frequent signs and symptoms at diagnosis were: leukocoria (73.6%) and strabismus (20.7%). The following distribution was identified: unilateral disease (65.0%), bilateral disease (32.9%), being 80.4% with multifocal disease, (P=0,015), and trilateral disease (2.1%). The average age of patients at the appearance of the first sign or symptom was 18.1 months [median=12.0] and the average age at diagnosis was 23.5 months [median=16.5]. Fifty patients (35.7%) were diagnosed during their first year of age. The average time to diagnosis was of 5.4 months [median=3.0], (amplitude=0-77.0). In the hereditary retinoblastoma group, the average age at the appearance of the first sign or symptom was 12.3 months, whereas the non-hereditary group presented the first sign or symptom on average at 21.6 months (P=0,001). The average age at diagnosis was 15.9 months vs. 28 months for the hereditary and non-hereditary patients, respectively (P<0.001). However, no significant difference in overall survival was found when both groups were compared. Ocular staging at diagnosis was, for the most part, advanced disease, (Reese V classification: 76.5%, Internacional Classification of Retinoblastoma D or E in 78.1% patients), being that 35.2% of cases were comprised of unilateral disease and 34.8% of patients with bilateral disease already presented with extraocular lesions in at least one eye at diagnosis. Fifteen patients (10.7%) presented with metastasis at diagnosis. With regards to treatment, differnet modalities were employed, being that most patients underwent surgery with enucleation in 88.1% and e exenteration in 11.9%. A significant number of patients received systemic chemotherapy (57.1%) and/or radiotherapy (37.1%). Of all patients included, 131 (93.6%) remained in follow up at the hospital until 2012 or until their demise. Of these patients, 32 (22.9%) relapsed, leading to 19 deaths, 84.2% of them due to disease progression. Secondary malignancies were present in 6 patients (4.3%) and, of these, one patient presented with two different secondary malignancies. The average time of patient follow up was 323.2 months [300.3; 346.1]. Overall survival was of 86.4%, with the following time frames among the different patient subgroups: 92.0% for non-metastatic patients, 40.0% for metastatic patients, intraoculares 94.0% for patients with intraocular disease, and 68.5% for patients with extraocular lesions. With regards to unilateral or bilateral disease, overall survival was of 88.0%; for patients with trilateral disease, (N=3) all patients expired. Survival of patients with unilateral and intraocular disease was of 94.9%; patients with unilateral and extraocular disease presented a overall survival of 75.0%. Patients with bilateral intraocular lesions overall survival was of 94.5%, whereas patients with bilateral and extraocular disease had an overall survival of 68.4%. In our setting, Rb diagnosis still occurs when the patients already manifest advanced disease, which reduces considerably their overall survival and preservation of the ocular globe and vision. Moreover, late diagnosis requires more agressive treatments, and consequently leads to more frequent toxicities and late side effects. Periodic clinical and ophthalmologic evaluations during the first years of a child's life offer a greater chance of early diagnosis and referral to a multidisciplinary pediatric oncology center, which is crucial for the patient’s well being. There is much need of further investments which facilitate patient access to diagnosis and treatment for Rb, which is the most common ocular tumor in children.

Hospital de Clínicas de Porto Alegre.

Retinoblastoma

Criança

Epidemiologia

Retinoblastoma

Malignant tumors of the retina

Ocular malignant tumors

Hereditary retinoblastoma

Pediatric tumors

Frequência dos mutantes C282Y e H63D do gene HFE e sua influência no metabolismo do ferro e na expressão da beta talassemia heterozigota

Estevão, Isabeth da Fonseca [UNESP]

27 February 2007

Made available in DSpace on 2014-06-11T19:26:03Z (GMT). No. of bitstreams: 0 Previous issue date: 2007-02-27Bitstream added on 2014-06-13T20:54:00Z : No. of bitstreams: 1 estevao_if_me_sjrp.pdf: 1151592 bytes, checksum: 9e2d3a0a29b1ad6405857d13d891a9f1 (MD5) / Coordenação de Aperfeiçoamento de Pessoal de Nível Superior (CAPES) / A beta talassemia é um dos mais freqüentes distúrbios genéticos no mundo. Estima-se que 1,5% a 3% da população mundial seja portadora do traço talassêmico. Esses portadores geralmente são oligo ou assintomáticos e têm uma expectativa de vida semelhante à dos não portadores. Entretanto, níveis elevados de ferritina sérica têm sido observados em alguns estudos comparativos entre beta talassemia heterozigota e não portadores e, alguns indivíduos, que nunca foram transfundidos, apresentam sinais clínicos e laboratoriais de sobrecarga de ferro. A fisiopatologia dessa complicação continua em discussão. Vários pesquisadores têm sugerido um efeito modulador da mutação do gene da beta globina e mutações em genes codificadores de proteínas relacionadas ao metabolismo do ferro. Mutações no gene HFE são as mais freqüentemente associadas à hemocromatose hereditária. O objetivo do presente trabalho foi avaliar a freqüência das mutações C282Y e H63D no gene HFE em portadores de beta talassemia heterozigota e analisar sua influência no metabolismo do ferro. Foram estudados 162 portadores de beta talassemia heterozigota, residentes na cidade de São Carlos ou região, caucasóides e, acompanhados no serviço de Hematologia. O diagnóstico de traço talassêmico foi confirmado em todos por meio do eritrograma e da quantificação da Hb A2 e Hb fetal por HPLC. O metabolismo do ferro foi avaliado pelas dosagens de ferro sérico, capacidade total de ligação do ferro, ferritina e saturação da transferrina e, a análise molecular das mutações no gene HFE, pela técnica de PCR-RLFP. Foram realizadas análises de correlação linear de Pearson por idade e gênero entre hemoglobina... / Beta thalassemia is one of the most frequent genetic disorder in the world. It is estimated that 1.5% to 3% of the world population is a thalassemia carrier. These individuals are generally slightly symptomatic or asymptomatic and they have a life expectancy similar to those who are non-carriers. However, high levels of serum ferritin have been observed in some comparative studies between heterozygous for beta thalassemia and non-carriers, and some individuals that were never transfused, present clinic and laboratories signs of iron overload. The physiopathology of this disease continues in discussion. Several researchers have suggested a modulator effect from the mutation of the beta globin gene and mutations in genes related with the iron metabolism. Mutations of the gene HFE are the most frequently associated to the hereditary hemochromatosis. The aim of this study was evaluate the frequency of C282Y and H63D mutations in the HFE gene in beta thalassemia carriers, and analyze its influence in the iron metabolism. 162 beta thalassemia carriers, Caucasoid, residing in the city of Sao Carlos or region and accompanied in the Hematology service were studied. The diagnostic of thalassemia trait was confirmed in every one through a complete erythrogram and quantification of Hb A2 and Hb fetal by HPLC. The iron metabolism was evaluated by serum iron, total iron-binding capacity, serum ferritin and percent saturation of transferring. The molecular analysis of the mutations in the HFE gene was made by PCR-RLFP. There were made analysis of linear Pearson’ correlation, by age and gender, among hemoglobin, Hb A2, VCM and among reticulocytes count and the values of saturation of transferrin and serum ferritin.

Talassemia

Hematologia

Ferro - Metabolismo

Talassemia beta

Gene HFE - Mutações

Hereditary hemochromatosis

HFE gene

Beta-thalassemia

Ferritin

Saturation of transferrin

Iron overload

Avaliação estrutural e diagnóstica de três lesões fibrosas da cavidade bucal

Badauy, Cristiano Macabú

January 2008

O objetivo do presente trabalho é analisar os componentes celulares e de fibras do tecido conjuntivo nas hiperplasias inflamatórias (HI), nos fibromas (F) e na fibromatose gengival hereditária (FGH), além de investigar a imunocompetência e efetuar análises moleculares de pacientes com FGH. Para atingir os objetivos foram desenvolvidos 4 artigos, com diferentes metodologias e universos amostrais. No 1º artigo, pretendeu-se estabelecer critérios microscópicos válidos para diferenciar F e HI. Foram avaliadas em microscópio óptico 136 lesões coradas pela Hematoxilina-eosina (HE) e pelo Tricrômico de Masson quanto às características microscópicas. Os resultados mostraram que uma área central de fibras colágenas dispostas de forma enovelada e mais densa, circundada por uma camada de fibras dispostas de forma paralela são características dos F, enquanto a presença de hiperplasia epitelial, infiltrado inflamatório e fibras colágenas organizadas de forma paralela são características das HI. Tais resultados motivaram o 2º artigo, no qual estudamos 18 lesões de F e 13 de HI, que foram preparadas histologicamente e coradas pelo picrosírius red e pelo direct blue para avaliação quantitativa das fibras colágenas e de fibras do sistema elástico, respectivamente, em microscopia a laser confocal. Os resultados confirmaram a disposição estrutural das fibras colágenas observada no 1º artigo, além de apontarem diferenças nas áreas ocupadas pelas fibras colágenas em todas as regiões estudadas. A fim de proceder a uma avaliação dos componentes fibroso e celular das 3 lesões fibrosas, foi desenvolvido o 3º artigo. Espécimes das 3 lesões foram estudados em microscopia ótica, a fim de avaliar suas populações de fibroblastos e de células inflamatórias e os seguintes componentes fibrosos do tecido conjuntivo: fibras colágenas, sistema de fibras elásticas, fibras reticulares e fibras oxitalânicas. Os resultados mostraram disposição e concentração diferente das fibras colágenas nas 3 lesões e uma maior concentração de fibras reticulares na FGH. A análise dos componentes celulares mostrou um maior número de fibroblastos no F e uma maior contagem de células inflamatórias na HI. A partir do encaminhamento de uma família com FGH, optouse por inclui-la no estudo, tendo em vista serem lesões do mesmo grupo. Com isso, foi desenvolvido um 4º estudo, que utilizou uma avaliação morfológica semelhante à dos 2 artigos anteriormente descritos. Dos pacientes com FGH foi obtido sangue periférico para avaliação da proliferação celular de linfócitos através do teste do MTT e para o sequenciamento do gene SOS-1. Os resultados mostraram hiperplasia epitelial na porção externa da gengiva dos pacientes com FGH, maior concentração de fibras colágenas e poucas células inflamatórias. Os 3 pacientes com FGH não mostraram diferenças no seu índice de proliferação de linfócitos em relação aos controles e não apresentaram a mutação descrita no gene SOS-1 de outras famílias com FGH. Pode se concluir que as 3 lesões apresentam estrutura conjuntiva diferente tanto no aspecto quantitativo quanto na disposição estrutural de seus componentes. / The objective of this study was to analyze the cellular and fibrous components of connective tissue in inflammatory hyperplasia (IH), oral fibroma (OF) and hereditary gingival fibromatosis (HGF), and to investigate the immunocompetence and to perform molecular analysis in HGF patients. To achieve the goals were developed 4 articles, with different methodologies and sample universes. In the 1st article, we intended to establish microscopic criteria to differentiate F and IH. The microscopic characteristics of the lesions (n=136) stained by hematoxylin-eosin (HE) and Masson trichrome were evaluated in an optical microscope. The results showed that a central area of wound collagen fibers and arranged in a higher density, surrounded by a layer of parallel fibers are characteristic of F, while the presence of epithelial hyperplasia, inflammatory infiltrate and parallel collagen fibers are characteristics of HI. These results led the 2nd article, which studied 18 F and 13 and IH, histologically prepared and stained by picrosírius red and direct blue for the direct quantitative assessment of collagen fibers and elastic fibers of the system, respectively, in the confocal laser microscope. The results confirmed the structural arrangement of collagen fibers found in Article 1, and indicate differences in the areas of collagen fibers in all regions studied. In order to evaluate the cellular and fibrous components of the 3 fibrous lesions, was developed the 3rd article. Specimens of the 3 lesions were studied in optical microscopy, to assess their populations of fibroblasts and inflammatory cells and the following components of fibrous connective tissue: collagen fibers, elastic fiber system, reticular fibers and oxytalan fibers. The results showed different arrangement and concentration of collagen fibers in the 3 lesions and a higher concentration of reticular fibers in HGF. The analysis of cellular components showed a greater number of fibroblasts in F and a higher count of inflammatory cells in IH. With the identification of a family with HGF, we chose to include it in the study because the lesions belong to the group of benign fibrous lesions. With that, it developed a 4th study, which used a similar morphologic evaluation of the 2 articles described above. Periferic blood was extracted from the HGF patients in order to determine the proliferative capacity of the peripheral lymphocytes, by the MTT test, and in order to sequence the SOS1 gene. The 3 HGF affected patients did not present the described mutation for the SOS1 gene, and the lymphocyte proliferative capacity in HGF patients was similar to those on controls. The results showed epithelial hyperplasia in the outer portion of the gingiva of patients with HGF, greater concentration of collagen fibers and few inflammatory cells. We can conclude that the 3 lesions present a different connective structure, considering both the quantitative aspect and the architectural disposition of their components.

Patologia bucal

Mucosa bucal : Doencas

Inflammatory hyperplasia

Oral fibroma

Hereditary gingival fibromatosis

Collagen fibers

Reticular fibers

Fibroblasts

Lymphocytes

Cellular proliferation