Moysés Sadigursky scite author profile

The indeterminate phase of Chagas' disease is defined as the prolonged period of clinically silent infection that follows the phase of acute primary infection with Trypanosoma cruzi. The dog is the only experimental animal model in which the indeterminate phase progresses to the late phase of severe, chronic myocarditis. This report describes the cardiac histologic and ultrastructural findings in dogs that survived the acute phase of infection with T. cruzi, becoming clinically and electrocardiographically normal for up to 3.5 years, while maintaining positive serologic test results during this period of time. Most of the myocardium appeared morphologically normal; however, small foci of mild, chronic myocarditis were present, with interstitial edema, mild fibrosis, and infiltration by lymphocytes, macrophages, and plasma cells. No microvascular lesions and no areas of close contact between immune effector cells and endothelial cells or cardiac myocytes were present. These findings were in sharp contrast to those observed in the canine model during the acute infection with T. cruzi. In this model, acute myocyte damage and lesions in the microcirculation, including fibrin microthrombi, were associated with close contacts between immune effector cells and myocytes or endothelial cells. Focally inflamed interstitial tissue showed increased deposition of amorphous and collagenous extracellular matrix as well as evidence of breakdown of collagen. The features of the inflammatory cells in the indeterminate phase of Chagas' disease were interpreted as indicating a self-limited cycle of focal inflammatory changes, with modulation and suppression of cell-mediated immune responses. Thus, we consider the indeterminate phase of Chagas' disease to be a stage of host-parasite equilibrium rather than a process of progressive damage.

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Natural infection of the opossum Didelphis albiventris (Marsupialia, Didelphidae) with Leishmania donovani, in Brazil

Sherlock¹,

Miranda²,

Sadigursky³

et al. 1984

Mem. Inst. Oswaldo Cruz

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A New Liquid Medium without Blood and Serum for Culture of Hemoflagellates

Sadigursky¹,

Brodskyn²

1986

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Renal Changes in Patients with Hepatosplenic Schistosomiasis *

Andrade¹,

Andrade²,

Sadigursky³

1971

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Subcutaneous Zygomycosis Caused by Basidiobolus Haptosporus: Presentation of a Case Mimicking Burkitt's Lymphoma *

Bittencourt¹,

Serra²,

Sadigursky³

et al. 1982

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Efeito genotóxico do etanol em células da mucosa bucal

Reis

Sadigursky

Andrade³

et al. 2002

Pesqui. Odontol. Bras.

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RESUMO:O etanol é um dos agentes químicos relacionados ao desenvolvimento de neoplasias malignas bucais. Os micronúcleos são porções de cromatina que permanecem próximas ao núcleo, resultantes de mitoses aberrantes após a ação de agentes genotóxicos. Dessa forma, sua ocorrência reflete o grau de exposição celular a carcinógenos. O objetivo deste trabalho foi avaliar a freqüência de micronúcleos em células esfoliadas da língua e da mucosa jugal de indiví-duos dependentes químicos de etanol. A amostra constou de células esfoliadas da língua e da mucosa jugal de 40 indivíduos alcoólatras não fumantes e de 20 abstêmios de álcool e fumo. As células obtidas foram coradas pelo método de Feulgen e contracoradas pelo "Fast Green". Observou-se um aumento estatisticamente significativo da freqüência de micronúcleos em células esfoliadas da língua no grupo de indivíduos expostos ao etanol em relação ao grupo controle (p < 0,01). A freqüência de micronúcleos em células esfoliadas da mucosa jugal apresentou-se maior no grupo de indivíduos alcoólatras quando comparado ao grupo controle, porém não houve diferença estatisticamente significante (p > 0,05). Conclui-se, portanto, que o consumo excessivo de etanol promove alterações efetivas em células da mucosa bucal, mesmo na ausência de exposição ao fumo. Tais alterações apresentam-se mais expressivas no bordo lateral de língua, um sítio mais exposto à ação de carcinógenos quando comparado à mucosa jugal. UNITERMOS: Neoplasias bucais; Etanol; Micronúcleos.ABSTRACT: Ethanol is one of the chemicals related to the development of oral malignant neoplasms. Micronuclei are chromatin fragments which, after aberrant mitoses, do not become included in the main nucleus. They have been used as indicators of genotoxic damage in cells exposed to carcinogens. The aim of this study was to assess the frequency of micronuclei in exfoliated cells from the tongue and buccal mucosa of alcoholic individuals. Samples were taken from the tongue and buccal mucosa of 40 alcoholic individuals who did not smoke, and from 20 alcohol and tobacco abstainers. Cells were stained with the Feulgen reaction and counterstained with Fast Green. A significant increase in the frequency of micronuclei in tongue cells was found in the group of subjects exposed to alcohol, when compared to the control group (p < 0.01). The frequency of micronuclei in buccal mucosa cells was higher in the group of alcoholic individuals, when compared to the control group, although there was no significant difference (p > 0.05). Our results indicate that excessive alcohol consumption may induce effective alterations on oral mucosa cells, even without exposure to tobacco. These alterations are more expressive in the tongue, which is a site more exposed to the action of carcinogens, when compared to the buccal mucosa. UNITERMS: Mouth neoplasms; Ethanol; Micronuclei. INTRODUÇÃODiversos agentes influem de forma genotóxica nas células e estão relacionados aos vários está-gios da carcinogênese. Com relação à cavidade bucal, o fumo tem sido descr...

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Pulmonary Changes in Schistosomal Cor Pulmonale *

Sadigursky¹,

Andrade²

1982

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The subclinical form of experimental visceral leishmaniasis in dogs

Oliveira

Santoro

Sadigursky

1993

Mem. Inst. Oswaldo Cruz

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Pathological aspects of a subclinical form of experimental canine leishmaniasis is reported here for the first time. Fifteen mongrel dogs were used in the present study. Eight dogs were infected and seven were used as control. Four of the control dogs were inoculated with spleen cells from non-infected hamsters. The eight mongrel dogs inoculated intravenously with amastigotes forms of Leishmania chagasi evolved for periods as long as 25 months without any clinical characteristic sign of classical Visceral Leishmaniasis (VL). Most of the laboratory test results were compatible to those of the seven control animals but culture of bone marrow aspirated material and serologic testing (IIF) demonstrated or provided evidence that the animals were infected. The most important and predominant histopathological lesion in infected animals were epithelioid granulomas presented in the liver, spleen, adrenal gland and lung of some animals. Channels containing erythrocytes in some granulomas of the liver suggest that these granulomas are formed inside sinusoidal capillaries. Despite the animals were proved to be infected and presented characteristic histologic lesions, they did not present external signs of disease. The granulomatous aspect of the lesions indicates a good immunologic reactivity and suggest that a host-parasite equilibrium does exist in the dog experimental model.

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