Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos

Detalhes bibliográficos
Autor(a) principal: Silveira, Helson Freitas
Data de Publicação: 2017
Tipo de documento: Dissertação
Idioma: por
Título da fonte: Repositório Institucional da Universidade Federal do Ceará (UFC)
Texto Completo: http://www.repositorio.ufc.br/handle/riufc/26306
Resumo: Thyroid hormones (HTs) are important mediators of the growth and development of the organism, mainly of the CNS. The lack of HTs decreases neuronal volume, and causes defects in myelination. Hypothyroidism depresses neuronal excitability when associated with chronic peripheral lesion in rats, reduces conduction velocity, with absence of sensory potentials. Considering that hypothyroidism causes changes in the development of the neuronal response, with an increase in the excitability threshold of the peripheral nerve fiber. We investigated and evaluated peripheral and central nociceptive and morphological effects of hypothyroidism in the presence of neuropathic pain. Male Wistar rats, 180 to 220 g, maintained at 24 ° C, day / night cycle - 12/12 h, water ad libitum, free access to balanced feed, housed in groups of 4 per cage were used. The animals were divided into 6 groups of 6 animals: control (C), trigeminal neuralgia (NT), NT Sham, hypothyroidism (H), H + NT, H + NT Sham. Hypothyroidism was induced with 0.05% propylthiuracil (PTU) for 21 days, and confirmed by T4 dosing. Induction of trigeminal neuralgia was performed through infraorbital nerve constriction. The nociceptive threshold was measured by electronic Von Frey test 2 times a week after surgery for 21 days. The caudal trigeminal subnucleus (SCT), trigeminal ganglion (GT), infraorbital nerve (NIO), thyroid and vibrissa skin were collected. Immunofluorescence-labeled material with antibodies, anti-NeuN, anti-c-Fos, anti-PBM, anti-ATF-3 and anti-PGP 9.5 to evidence signs of cellular injury, pain and the integrity of nerve fibers. Thyroid stained in HE for histopathological analysis. Statistical analysis was done by mean ± SEM of the measurements recorded, data normalization by Shapiro-Wilk, analysis of variance (ANOVA one way or two way), with post- test of Turkey or Games-Howell determined by the test of homogeneity of variance of Levene, where values of p <0.05 were considered statistically significant and Spearman's correlation test. Our results showed a reduction in T4 levels, weight loss, increase in thyroid gland size and weight, follicular hyperplasia and thyroid hypertrophy, and negative correlation between T4 levels and thyroid morphometry. There was a reduction in the nociceptive threshold in the NT, but in the H group they showed an increase in the threshold and the threshold of the H + NT group showed at the control levels, suggesting a subclinical manifestation, in addition to a negative correlation with the T4 levels. ATF3 was shown to be elevated in neuropathic groups in GT, but did not express in SCT. C-Fos was elevated in the NT group, reduced in the H + NT in GT, but in the TE the c-Fos in the H + NT group rose above the NT group, which was also increased. PBM and DAPI were increased in the neuropathic groups, there were signs of axonal death and delamination of the myelin sheath. PGP 9.5 showed a decrease in the number of nerve endings in the skin of vibrissae in NT groups. We conclude that the induction model of hypothyroidism with PTU in rats is effective, reproduces the alterations found in humans with hypothyroidism, demonstrated through serological, behavioral, anatomopathological and histopathological studies. There is a negative correlation between T4 levels and thyroid morphometry. Hypothyroidism leads to disturbances in the nociceptive response in rats, and leading the pain signals in neuropathic state to subclinical levels. There is a negative correlation between T4 levels and the nociceptive threshold. The expression of c-Fos reduction in the trigeminal ganglion evidences the predominance of the peripheral effect in the nociception of hypothyroidism. Expression of ATF3 shows that hypothyroidism does not influence the ability of the peripheral neuron to initiate a response. Hypothyroidism decreases axonal repair ability and remyelination of peripheral pathways by reducing the amount of fibers and nerve endings shown in the expression of PBM and PGP 9.5.
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spelling Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratosInfluence of hypothyroidism on peripheral and central nociceptive and morphological changes in trigeminal neuralgia in ratsHipotireoidismoNeuralgia do TrigêmeoNociceptividadeDorThyroid hormones (HTs) are important mediators of the growth and development of the organism, mainly of the CNS. The lack of HTs decreases neuronal volume, and causes defects in myelination. Hypothyroidism depresses neuronal excitability when associated with chronic peripheral lesion in rats, reduces conduction velocity, with absence of sensory potentials. Considering that hypothyroidism causes changes in the development of the neuronal response, with an increase in the excitability threshold of the peripheral nerve fiber. We investigated and evaluated peripheral and central nociceptive and morphological effects of hypothyroidism in the presence of neuropathic pain. Male Wistar rats, 180 to 220 g, maintained at 24 ° C, day / night cycle - 12/12 h, water ad libitum, free access to balanced feed, housed in groups of 4 per cage were used. The animals were divided into 6 groups of 6 animals: control (C), trigeminal neuralgia (NT), NT Sham, hypothyroidism (H), H + NT, H + NT Sham. Hypothyroidism was induced with 0.05% propylthiuracil (PTU) for 21 days, and confirmed by T4 dosing. Induction of trigeminal neuralgia was performed through infraorbital nerve constriction. The nociceptive threshold was measured by electronic Von Frey test 2 times a week after surgery for 21 days. The caudal trigeminal subnucleus (SCT), trigeminal ganglion (GT), infraorbital nerve (NIO), thyroid and vibrissa skin were collected. Immunofluorescence-labeled material with antibodies, anti-NeuN, anti-c-Fos, anti-PBM, anti-ATF-3 and anti-PGP 9.5 to evidence signs of cellular injury, pain and the integrity of nerve fibers. Thyroid stained in HE for histopathological analysis. Statistical analysis was done by mean ± SEM of the measurements recorded, data normalization by Shapiro-Wilk, analysis of variance (ANOVA one way or two way), with post- test of Turkey or Games-Howell determined by the test of homogeneity of variance of Levene, where values of p <0.05 were considered statistically significant and Spearman's correlation test. Our results showed a reduction in T4 levels, weight loss, increase in thyroid gland size and weight, follicular hyperplasia and thyroid hypertrophy, and negative correlation between T4 levels and thyroid morphometry. There was a reduction in the nociceptive threshold in the NT, but in the H group they showed an increase in the threshold and the threshold of the H + NT group showed at the control levels, suggesting a subclinical manifestation, in addition to a negative correlation with the T4 levels. ATF3 was shown to be elevated in neuropathic groups in GT, but did not express in SCT. C-Fos was elevated in the NT group, reduced in the H + NT in GT, but in the TE the c-Fos in the H + NT group rose above the NT group, which was also increased. PBM and DAPI were increased in the neuropathic groups, there were signs of axonal death and delamination of the myelin sheath. PGP 9.5 showed a decrease in the number of nerve endings in the skin of vibrissae in NT groups. We conclude that the induction model of hypothyroidism with PTU in rats is effective, reproduces the alterations found in humans with hypothyroidism, demonstrated through serological, behavioral, anatomopathological and histopathological studies. There is a negative correlation between T4 levels and thyroid morphometry. Hypothyroidism leads to disturbances in the nociceptive response in rats, and leading the pain signals in neuropathic state to subclinical levels. There is a negative correlation between T4 levels and the nociceptive threshold. The expression of c-Fos reduction in the trigeminal ganglion evidences the predominance of the peripheral effect in the nociception of hypothyroidism. Expression of ATF3 shows that hypothyroidism does not influence the ability of the peripheral neuron to initiate a response. Hypothyroidism decreases axonal repair ability and remyelination of peripheral pathways by reducing the amount of fibers and nerve endings shown in the expression of PBM and PGP 9.5.Os hormônios tireoidianos (HTs) são importantes mediadores do crescimento e desenvolvimento do organismo, principalmente do SNC. A falta dos HTs diminui o volume neuronal, e provoca defeitos na mielinização, deprindo a excitabilidade e reduzindo a velocidade de condução. O hipotireoidismo provoca alterações no desenvolvimento da resposta neuronal, com aumento do limiar de excitabilidade da fibra nervosa periférica. Investigamos e avaliamos os efeitos nociceptivos e morfológicos periféricos e centrais do hipotireoidismo na presença da dor neuropática. Foram utilizados ratos Wistar machos, 180 a 220 g, mantidos a 24°C, ciclo dia/noite - 12/12 h, água ad libitum, livre acesso a ração balanceada, alojados em grupos de 4 por gaiola. Os animais foram divididos em 6 grupos de 6 animais: controle (C), neuralgia do trigêmeo (NT), NT Sham, hipotireoidismo (H), H+NT, H+ NT Sham. O hipotireoidismo foi induzido com propiltiuracil (PTU) 0,05% por 21 dias, e confirmado por dosagem de T4. Foi realizada indução da neuralgia trigeminal através da constrição do nervo infraorbital. O limiar nociceptivo foi aferido por teste de Von Frey eletrônico 2 vezes por semana após a cirurgia por 21 dias. Foram coletados o subnúcleo caudal do trigêmeo (SCT), gânglio trigeminal (GT), nervo infraorbital (NIO), tireoide e pele da vibrissa. O material marcado por imunofluorescência com os anticorpos, anti-NeuN, anti-c-Fos, anti-PBM, anti ATF-3 e anti-PGP 9.5 para evidenciar sinais de injúria celular, nocicepção e integridade das fibras nervosas e as tireoides coradas em HE para análise histopatológica. A análise estatística foi feita pela média ± EPM das medidas registradas, normalização de dados por Shapiro-Wilk, análise de variância (ANOVA one way ou two way), com pós-teste de Turkey ou Games- Howell determinado pelo teste de homogeneidade de variância de Levene, onde valores de p<0,05 foram considerados estatisticamente significativos e teste de correlação de Spearman. Os resultados mostraram nos grupos com hipotireoidismo redução dos níveis de T4, perda ponderal, aumento nas dimensões e peso das glândulas tireoides, hiperplasia folicular e hipertrofia da tireoide, e houve correlação negativa entre os níveis de T4 e a morfometria da Tireoide. Houve redução do limiar nociceptivo no NT, contudo no grupo H mostraram aumento do limiar e o limiar do grupo H+NT mostrou a níveis do controle, sugerindo uma manifestação subclínica, além de correlação negativa com os níveis de T4. ATF3 mostrou-se elevado nos grupos neuropáticos no GT, mas não expressou no SCT. C-Fos elevou-se no grupo NT, reduzido no H+NT em GT, contudo no TE o c-Fos no grupo H+NT elevou-se acima do grupo NT, que também se apresentava aumentado. PBM e DAPI apresentaram-se aumentados nos grupos neuropáticos, houve sinais de morte axonal e delaminação da bainha de mielina. PGP 9.5 mostrou diminuição do número de terminações nervosas na pele das vibrissas nos grupos com NT. Concluímos que o modelo de indução do hipotireoidismo com PTU em ratos é eficaz, reproduz as alterações encontradas em humanos com hipotireoidismo, demonstrado através de estudos sorológicos, comportamentais, anatomopatológicos e histopatológicos. Há uma correlação negativa entre os níveis de T4 e a morfometria da tireoide. O hipotireoidismo leva a distúrbios na resposta nociceptiva em ratos, e levando os sinais de dor em estado neuropático a níveis subclínicos. Há uma correlação negativa entre os níveis de T4 e o limiar nociceptivo. A expressão de redução de c-Fos do gânglio trigeminal evidencia a predominância do efeito periférico na nocicepção do hipotireoidismo. A expressão de ATF3 mostra que o hipotireoidismo não influencia na capacidade do neurônio periférico de iniciar uma resposta. O hipotireoidismo diminui da capacidade de reparo axonal e remielinização das vias periféricas reduzindo a quantidade de fibras e terminações nervosas mostrados na expressão de PBM e PGP 9.5.Vale, Mariana LimaGondim, Delane VianaSilveira, Helson Freitas2017-10-04T11:16:33Z2017-10-04T11:16:33Z2017-09-26info:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/masterThesisapplication/pdfSILVEIRA, H. F. Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos. 2017. 150 f. Dissertação (Mestrado em Ciências Morfofuncionais) - Faculdade de Medicina, Universidade Federal do Ceará, Fortaleza, 2017.http://www.repositorio.ufc.br/handle/riufc/26306porreponame:Repositório Institucional da Universidade Federal do Ceará (UFC)instname:Universidade Federal do Ceará (UFC)instacron:UFCinfo:eu-repo/semantics/openAccess2018-12-13T17:46:48Zoai:repositorio.ufc.br:riufc/26306Repositório InstitucionalPUBhttp://www.repositorio.ufc.br/ri-oai/requestbu@ufc.br || repositorio@ufc.bropendoar:2024-09-11T18:38:52.655388Repositório Institucional da Universidade Federal do Ceará (UFC) - Universidade Federal do Ceará (UFC)false
dc.title.none.fl_str_mv Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
Influence of hypothyroidism on peripheral and central nociceptive and morphological changes in trigeminal neuralgia in rats
title Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
spellingShingle Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
Silveira, Helson Freitas
Hipotireoidismo
Neuralgia do Trigêmeo
Nociceptividade
Dor
title_short Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
title_full Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
title_fullStr Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
title_full_unstemmed Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
title_sort Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos
author Silveira, Helson Freitas
author_facet Silveira, Helson Freitas
author_role author
dc.contributor.none.fl_str_mv Vale, Mariana Lima
Gondim, Delane Viana
dc.contributor.author.fl_str_mv Silveira, Helson Freitas
dc.subject.por.fl_str_mv Hipotireoidismo
Neuralgia do Trigêmeo
Nociceptividade
Dor
topic Hipotireoidismo
Neuralgia do Trigêmeo
Nociceptividade
Dor
description Thyroid hormones (HTs) are important mediators of the growth and development of the organism, mainly of the CNS. The lack of HTs decreases neuronal volume, and causes defects in myelination. Hypothyroidism depresses neuronal excitability when associated with chronic peripheral lesion in rats, reduces conduction velocity, with absence of sensory potentials. Considering that hypothyroidism causes changes in the development of the neuronal response, with an increase in the excitability threshold of the peripheral nerve fiber. We investigated and evaluated peripheral and central nociceptive and morphological effects of hypothyroidism in the presence of neuropathic pain. Male Wistar rats, 180 to 220 g, maintained at 24 ° C, day / night cycle - 12/12 h, water ad libitum, free access to balanced feed, housed in groups of 4 per cage were used. The animals were divided into 6 groups of 6 animals: control (C), trigeminal neuralgia (NT), NT Sham, hypothyroidism (H), H + NT, H + NT Sham. Hypothyroidism was induced with 0.05% propylthiuracil (PTU) for 21 days, and confirmed by T4 dosing. Induction of trigeminal neuralgia was performed through infraorbital nerve constriction. The nociceptive threshold was measured by electronic Von Frey test 2 times a week after surgery for 21 days. The caudal trigeminal subnucleus (SCT), trigeminal ganglion (GT), infraorbital nerve (NIO), thyroid and vibrissa skin were collected. Immunofluorescence-labeled material with antibodies, anti-NeuN, anti-c-Fos, anti-PBM, anti-ATF-3 and anti-PGP 9.5 to evidence signs of cellular injury, pain and the integrity of nerve fibers. Thyroid stained in HE for histopathological analysis. Statistical analysis was done by mean ± SEM of the measurements recorded, data normalization by Shapiro-Wilk, analysis of variance (ANOVA one way or two way), with post- test of Turkey or Games-Howell determined by the test of homogeneity of variance of Levene, where values of p <0.05 were considered statistically significant and Spearman's correlation test. Our results showed a reduction in T4 levels, weight loss, increase in thyroid gland size and weight, follicular hyperplasia and thyroid hypertrophy, and negative correlation between T4 levels and thyroid morphometry. There was a reduction in the nociceptive threshold in the NT, but in the H group they showed an increase in the threshold and the threshold of the H + NT group showed at the control levels, suggesting a subclinical manifestation, in addition to a negative correlation with the T4 levels. ATF3 was shown to be elevated in neuropathic groups in GT, but did not express in SCT. C-Fos was elevated in the NT group, reduced in the H + NT in GT, but in the TE the c-Fos in the H + NT group rose above the NT group, which was also increased. PBM and DAPI were increased in the neuropathic groups, there were signs of axonal death and delamination of the myelin sheath. PGP 9.5 showed a decrease in the number of nerve endings in the skin of vibrissae in NT groups. We conclude that the induction model of hypothyroidism with PTU in rats is effective, reproduces the alterations found in humans with hypothyroidism, demonstrated through serological, behavioral, anatomopathological and histopathological studies. There is a negative correlation between T4 levels and thyroid morphometry. Hypothyroidism leads to disturbances in the nociceptive response in rats, and leading the pain signals in neuropathic state to subclinical levels. There is a negative correlation between T4 levels and the nociceptive threshold. The expression of c-Fos reduction in the trigeminal ganglion evidences the predominance of the peripheral effect in the nociception of hypothyroidism. Expression of ATF3 shows that hypothyroidism does not influence the ability of the peripheral neuron to initiate a response. Hypothyroidism decreases axonal repair ability and remyelination of peripheral pathways by reducing the amount of fibers and nerve endings shown in the expression of PBM and PGP 9.5.
publishDate 2017
dc.date.none.fl_str_mv 2017-10-04T11:16:33Z
2017-10-04T11:16:33Z
2017-09-26
dc.type.status.fl_str_mv info:eu-repo/semantics/publishedVersion
dc.type.driver.fl_str_mv info:eu-repo/semantics/masterThesis
format masterThesis
status_str publishedVersion
dc.identifier.uri.fl_str_mv SILVEIRA, H. F. Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos. 2017. 150 f. Dissertação (Mestrado em Ciências Morfofuncionais) - Faculdade de Medicina, Universidade Federal do Ceará, Fortaleza, 2017.
http://www.repositorio.ufc.br/handle/riufc/26306
identifier_str_mv SILVEIRA, H. F. Influência do hipotireoidismo sobre as alterações nociceptivas e morfológicas periféricas e centrais na neuralgia trigeminal em ratos. 2017. 150 f. Dissertação (Mestrado em Ciências Morfofuncionais) - Faculdade de Medicina, Universidade Federal do Ceará, Fortaleza, 2017.
url http://www.repositorio.ufc.br/handle/riufc/26306
dc.language.iso.fl_str_mv por
language por
dc.rights.driver.fl_str_mv info:eu-repo/semantics/openAccess
eu_rights_str_mv openAccess
dc.format.none.fl_str_mv application/pdf
dc.source.none.fl_str_mv reponame:Repositório Institucional da Universidade Federal do Ceará (UFC)
instname:Universidade Federal do Ceará (UFC)
instacron:UFC
instname_str Universidade Federal do Ceará (UFC)
instacron_str UFC
institution UFC
reponame_str Repositório Institucional da Universidade Federal do Ceará (UFC)
collection Repositório Institucional da Universidade Federal do Ceará (UFC)
repository.name.fl_str_mv Repositório Institucional da Universidade Federal do Ceará (UFC) - Universidade Federal do Ceará (UFC)
repository.mail.fl_str_mv bu@ufc.br || repositorio@ufc.br
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