RESUMO
The objective of this investigation was to assess the toxicological potential of nasal formulation of erythropoietin with low sialic acid content (Neuro EPO) after 28 days of intra-nasal dosing in rats besides to evaluate the immunogenicity and erythropoietic effect of the test substance. Healthy Wistar rats of both sexes were used for 28 days subacute toxicity and immunogenicity assays. Doses evaluated were 3450, 4830 and 6900 UI/kg/day. The toxicological endpoints examined included animal body weight, food consumption, hematological and biochemical patterns, antibodies determination, selected tissue weights and histopathological examination. Reversibility of toxic effects was evaluated at high dose 14 days after treatment period. Female B6D2F1 mice were used for evaluated erythropoietic effect of the nasal formulation. Hematological endpoints were examined every week during 28 days of intra-nasal dosing of 6900 UI/kg/day. Variations of hematological patterns were not observed after 28 days of intranasal dosing. A slight increase in glucose level of treated animals within the normal range was observed. This effect was not dose related and was reversible. Antibody formation was not observed in any of the test doses. Histopathological examination of organs and tissues did not reveal treatment induced changes. The administration of Neuro EPO in normocythaemic mice did not produce erythropoietic effect. These results suggest that Neuro EPO could be used as a neuroprotective agent, without significant systemic haematological side effects.
Assuntos
Eritropoese/fisiologia , Eritropoetina/administração & dosagem , Ácido N-Acetilneuramínico/administração & dosagem , Testes de Toxicidade Aguda , Administração Intranasal , Animais , Esquema de Medicação , Eritropoese/efeitos dos fármacos , Eritropoetina/toxicidade , Feminino , Masculino , Camundongos , Ácido N-Acetilneuramínico/toxicidade , Ratos , Ratos Wistar , Testes de Toxicidade Aguda/métodosRESUMO
Fundamentación: los extractos de Momordica charantia L. poseen potencial terapéutico avalado científicamente que posibilita el empleo de esta planta en diversas enfermedades, sobre todo en la diabetes, por lo que caracterizar su potencial tóxico es de gran importancia para avalar el empleo de esta planta como agente terapéutico. Objetivos: realizar los estudios de toxicidad aguda oral e irritación ocular y dérmica a extractos acuoso e hidroalcohólico de M. charantia, con la finalidad de caracterizar su potencial toxicológico agudo. Métodos: el ensayo de toxicidad aguda oral se llevó a cabo en ratas Wistar hembras mediante el método de las clases tóxicas agudas, con la dosis máxima de 2 000 mg/kg. Los ensayos de irritación dérmica y ocular se llevaron a cabo en conejos Nueva Zelanda siguiendo los métodos descritos en las normas OECD 404 y 405. Resultados: la evaluación del extracto hidroalcohólico de M. charantia en el ensayo de toxicidad aguda mostró signos tóxicos por causa de la presencia de etanol en el extracto y una ligera disminución del peso corporal que no fue significativa. La administración del extracto acuoso no provocó signos tóxicos ni mortalidad. Ambos extractos se clasificaron en categoría 5 para ubicarse en el rango de toxicidad de una DL50> 2 000 mg/kg. En el ensayo de irritación dérmica y ocular se clasificaron los extractos como no irritantes. Conclusiones: los extractos evaluados mostraron un bajo potencial tóxico agudo tanto por vía oral como tópica.
Rationale: Momordica charantia L. extracts have scientifically-endorsed therapeutical potentialities that make the use of this plant possible in several diseases, mainly for diabetes, so characterizing its toxic potential is of great significance to support this plant as a therapeutical agent. Objectives: to conduct acute oral toxicity and ocular and dermal irritation studies on aqueous hydroalcoholic extracts from M. charantia, with the aim of characterizing its acute toxicological potential. Methods: Acute oral toxicity test was applied to female Wistar rats through acute toxic class method, with maximum dose of 2000 mg/kg. Ocular/dermal irritation tests were made in New Zealand rabbits, following the described methods in OECD standards 404 and 405. Results: the evaluation of M. charantia hydroalcoholic extract in the acute toxicity test showed toxic signs due to ethanol in the extract and a minimum bodyweight reduction that was not significant. The administration of water extract elicited neither toxic signs nor mortality. Both extracts were classified into category 5 within the range of toxicity of DL50> 2 000 mg/kg. The dermal/ocular irritation test indicated that the studied extracts were not irritating. Conclusions: The evaluated extracts showed low acute toxic potential for both oral and topical administration.
Assuntos
Animais , Momordica charantia/toxicidade , Plantas Medicinais , Testes de Irritação da Pele , Testes de Toxicidade CrônicaRESUMO
Fundamentación: los extractos de Momordica charantia L. poseen potencial terapéutico avalado científicamente que posibilita el empleo de esta planta en diversas enfermedades, sobre todo en la diabetes, por lo que caracterizar su potencial tóxico es de gran importancia para avalar el empleo de esta planta como agente terapéutico. Objetivos: realizar los estudios de toxicidad aguda oral e irritación ocular y dérmica a extractos acuoso e hidroalcohólico de M. charantia, con la finalidad de caracterizar su potencial toxicológico agudo. Métodos: el ensayo de toxicidad aguda oral se llevó a cabo en ratas Wistar hembras mediante el método de las clases tóxicas agudas, con la dosis máxima de 2 000 mg/kg. Los ensayos de irritación dérmica y ocular se llevaron a cabo en conejos Nueva Zelanda siguiendo los métodos descritos en las normas OECD 404 y 405. Resultados: la evaluación del extracto hidroalcohólico de M. charantia en el ensayo de toxicidad aguda mostró signos tóxicos por causa de la presencia de etanol en el extracto y una ligera disminución del peso corporal que no fue significativa. La administración del extracto acuoso no provocó signos tóxicos ni mortalidad. Ambos extractos se clasificaron en categoría 5 para ubicarse en el rango de toxicidad de una DL50> 2 000 mg/kg. En el ensayo de irritación dérmica y ocular se clasificaron los extractos como no irritantes. Conclusiones: los extractos evaluados mostraron un bajo potencial tóxico agudo tanto por vía oral como tópica(AU)
Rationale: Momordica charantia L. extracts have scientifically-endorsed therapeutical potentialities that make the use of this plant possible in several diseases, mainly for diabetes, so characterizing its toxic potential is of great significance to support this plant as a therapeutical agent. Objectives: to conduct acute oral toxicity and ocular and dermal irritation studies on aqueous hydroalcoholic extracts from M. charantia, with the aim of characterizing its acute toxicological potential. Methods: Acute oral toxicity test was applied to female Wistar rats through acute toxic class method, with maximum dose of 2000 mg/kg. Ocular/dermal irritation tests were made in New Zealand rabbits, following the described methods in OECD standards 404 and 405. Results: the evaluation of M. charantia hydroalcoholic extract in the acute toxicity test showed toxic signs due to ethanol in the extract and a minimum bodyweight reduction that was not significant. The administration of water extract elicited neither toxic signs nor mortality. Both extracts were classified into category 5 within the range of toxicity of DL50> 2 000 mg/kg. The dermal/ocular irritation test indicated that the studied extracts were not irritating. Conclusions: The evaluated extracts showed low acute toxic potential for both oral and topical administration(AU)
