Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos
| Autor(a) principal: | |
|---|---|
| Data de Publicação: | 2014 |
| Tipo de documento: | Tese |
| Idioma: | por |
| Título da fonte: | Repositório Institucional da UFSCAR |
| Texto Completo: | https://repositorio.ufscar.br/handle/ufscar/5170 |
Resumo: | This study investigated the function of cerebellar histaminergic system on emotional memory consolidation. The cerebellar vermis of male mice were implanted with guide cannulae, and after three days of recovery, the animals were submitted to the elevated plus maze (EPM) or the inhibitory avoidance test (IA) on two consecutive days. Immediately after the first day, animals received a microinjection of histaminergic drugs into the cerebellar vermis: experiment 1, animals received microinjections of saline (SAL) or histamine (HA) (0.54, 1.36, 2.72, and 4.07 nmol/0.1 microliter); experiment 2, animals received a microinjection of SAL or the H1 antagonist chlorpheniramine (CPA, 0.016, 0.052 or 0.16 nmol/0.1 μl); experiment 3, SAL or the H2 antagonist ranitidine (RA, 0.57, 2.85 or 5.7 nmol/0.1 μl); experiment 4, SAL or HA 5 minutes after a pretreatment with 0.16 nmol CPA or SAL; and experiment 5, SAL or HA 5 minutes after a pretreatment with 2.85 nmol ranitidine (RA) or SAL. In the EPM, the decrease of open arm exploration (% entries and % time spent in the open arms) in Trial 2 relative to Trial 1 was used as a measure of learning and memory; while in the IA, latency to cross to the dark compartment was used to evaluate memory retention. Data were analyzed using ANOVA and Duncan‟s test. The results of experiment 1 showed that animals microinjected SAL and 0.54 and 1.36 nmol HA reduced percentage of open arm entries and time, while mice microinjected with HA 2.72 and 4.07 nmol did not decrease open arm exploration on trial 2; which indicates that histamine induced a dose-dependent inhibitory effect on memory consolidation. In the IA task, results showed that 1.36 nmol histamine facilitated memory consolidation, suggesting a different action of HA in a memory model that uses punishment. In the experiment 2, microinjections with CPA did not present behavioral effects in the EPM or in the IA at the doses used (0.016, 0.052 and 0.16 nmol). The results of experiment 3 showed that 5.7 nmol RA impaired memory consolidation on both protocols. The experiment 4 demonstrated that animals treated with HA did not reduce the avoidance to the open arms on retesting, and indicated that CPA did not altered behavioral parameters by itself, but the pretreatment with CPA reverted histamine-induced impairment on memory consolidation, which suggests that histamine effect on the EPM was mediated by H1 receptors. In the IA test, the results showed that the groups that received CPA+HA and SAL+HA showed a significant difference in latency on the second day of testing in relation to group SAL+SAL , while the group treated with CPA + SAL showed no difference with the control group. These results show that microinjection of histamine in the cerebellar vermis increased latency time and that pretreatment with CPA did not reverse this effect. For the fifth experiment, the results showed that animals microinjected with SAL+SAL and RA+SAL reduced the percentage of entries and time spent in open arms in the EPM while the groups treated with RA+HA and SAL+HA showed no difference between test days. These results show that RA did not alter memory consolidation and was unable to reverse the effect of histamine. In the IA, there was significant difference between SAL+SAL and SAL+HA groups, showing the facilitatory effect of histamine on memory consolidation of IA. The groups that received combined injection of RA+SAL and RA+HA showed no significant difference compared to control, which shows that the RA had no effect by itself, but when applied before histamine was able to reverse its effect. Our results suggest different histamine effects in tasks involving anxiety or fear. |
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Gianlorenço, Anna Carolyna LepesteurMattioli, Rosanahttp://genos.cnpq.br:12010/dwlattes/owa/prc_imp_cv_int?f_cod=K4797764Z6http://lattes.cnpq.br/38610504596716902016-06-02T20:18:22Z2014-02-242016-06-02T20:18:22Z2014-02-10GIANLORENÇO, Anna Carolyna Lepesteur. Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos. 2014. 164 f. Tese (Doutorado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2014.https://repositorio.ufscar.br/handle/ufscar/5170This study investigated the function of cerebellar histaminergic system on emotional memory consolidation. The cerebellar vermis of male mice were implanted with guide cannulae, and after three days of recovery, the animals were submitted to the elevated plus maze (EPM) or the inhibitory avoidance test (IA) on two consecutive days. Immediately after the first day, animals received a microinjection of histaminergic drugs into the cerebellar vermis: experiment 1, animals received microinjections of saline (SAL) or histamine (HA) (0.54, 1.36, 2.72, and 4.07 nmol/0.1 microliter); experiment 2, animals received a microinjection of SAL or the H1 antagonist chlorpheniramine (CPA, 0.016, 0.052 or 0.16 nmol/0.1 μl); experiment 3, SAL or the H2 antagonist ranitidine (RA, 0.57, 2.85 or 5.7 nmol/0.1 μl); experiment 4, SAL or HA 5 minutes after a pretreatment with 0.16 nmol CPA or SAL; and experiment 5, SAL or HA 5 minutes after a pretreatment with 2.85 nmol ranitidine (RA) or SAL. In the EPM, the decrease of open arm exploration (% entries and % time spent in the open arms) in Trial 2 relative to Trial 1 was used as a measure of learning and memory; while in the IA, latency to cross to the dark compartment was used to evaluate memory retention. Data were analyzed using ANOVA and Duncan‟s test. The results of experiment 1 showed that animals microinjected SAL and 0.54 and 1.36 nmol HA reduced percentage of open arm entries and time, while mice microinjected with HA 2.72 and 4.07 nmol did not decrease open arm exploration on trial 2; which indicates that histamine induced a dose-dependent inhibitory effect on memory consolidation. In the IA task, results showed that 1.36 nmol histamine facilitated memory consolidation, suggesting a different action of HA in a memory model that uses punishment. In the experiment 2, microinjections with CPA did not present behavioral effects in the EPM or in the IA at the doses used (0.016, 0.052 and 0.16 nmol). The results of experiment 3 showed that 5.7 nmol RA impaired memory consolidation on both protocols. The experiment 4 demonstrated that animals treated with HA did not reduce the avoidance to the open arms on retesting, and indicated that CPA did not altered behavioral parameters by itself, but the pretreatment with CPA reverted histamine-induced impairment on memory consolidation, which suggests that histamine effect on the EPM was mediated by H1 receptors. In the IA test, the results showed that the groups that received CPA+HA and SAL+HA showed a significant difference in latency on the second day of testing in relation to group SAL+SAL , while the group treated with CPA + SAL showed no difference with the control group. These results show that microinjection of histamine in the cerebellar vermis increased latency time and that pretreatment with CPA did not reverse this effect. For the fifth experiment, the results showed that animals microinjected with SAL+SAL and RA+SAL reduced the percentage of entries and time spent in open arms in the EPM while the groups treated with RA+HA and SAL+HA showed no difference between test days. These results show that RA did not alter memory consolidation and was unable to reverse the effect of histamine. In the IA, there was significant difference between SAL+SAL and SAL+HA groups, showing the facilitatory effect of histamine on memory consolidation of IA. The groups that received combined injection of RA+SAL and RA+HA showed no significant difference compared to control, which shows that the RA had no effect by itself, but when applied before histamine was able to reverse its effect. Our results suggest different histamine effects in tasks involving anxiety or fear.Esse trabalho teve como objetivo investigar a atuação do sistema neural histaminérgico na consolidação da memória emocional de camundongos. Foi realizada cirurgia esterotáxica para implantação da cânula no vérmis cerebelar de camundongos machos. No terceiro dia de recuperação, foram realizados os testes comportamentais Labirinto em Cruz Elevado (LCE) e Esquiva Inibitória (EI) em dois dias consecutivos. Imediatamente após o primeiro dia de teste, os animais receberam o tratamento farmacológico com a microinjeção de drogas histaminérgicas no vérmis cerebelar. No experimento 1, foi verificado o efeito da histamina (HA) microinjetada nas doses de 0,54 nmol, 1,36 nmol, 2,72 nmol e 4,07 nmol em camundongos submetidos ao LCE (experimento 1a) e ao teste EI (experimento 1b). No experimento 2 foi realizada microinjeção de antagonista H1 (Clorfeniramina, CPA) nas doses de 0,016 nmol, 0,052 nmol e 0,16 nmol em camundongos submetidos ao LCE (experimento 2a) e ao teste EI (experimento 2b). No experimento 3, microinjeção de antagonista H2 (Ranitidina, RA) nas doses de 0,57 nmol, 2,85 nmol e 5,7 nmol em camundongos submetidos ao LCE (experimento 3a) e ao teste EI (experimento 3b). No experimento 4, foi realizada microinjeção combinada de antagonista H1 e HA em camundongos submetidos ao LCE (experimento 4a) e ao teste EI (experimento 4b); e no experimento 5, foi realizada microinjeção combinada de antagonista H2 e HA no LCE (experimento 5a) e EI (experimento 5b). O índice de memória dos animais no LCE foi definido pela redução da exploração dos braços abertos na reexposição (T1/T2). Para o Teste de EI, o aumento ou a redução das latências foi considerado indicativo de facilitação ou prejuízo na retenção da memória. Os resultados do experimento 1a mostraram que no LCE, os animais do grupo controle (SAL) e dos grupos HA nas doses de 0,54 nmol e 1,36 nmol apresentaram redução da exploração dos braços abertos (BA) na reexposição, enquanto os animais que receberam HA nas doses de 2,72 e 4,07 não apresentaram diferença significativa em relação a T2. Esses resultados indicam uma inibição da memória emocional quando a histamina foi injetada no vérmis cerebelar em animais submetidos ao LCE. No experimento 1b, a análise estatística mostrou um aumento significativo na latência no teste de EI para os animais que receberam histamina na dose de 1,36 nmol em relação ao grupo controle. Além disso, houve diferença significativa entre os grupos microinjetados com 1,36 nmol e com 2,72 nmol e 4,07 nmol. Estes resultados indicam que a histamina microinjetada na dose de 1,36 nmol facilitou a consolidação da memória de EI em camundongos, sugerindo um papel diferente da histamina em um modelo que usa punição. No experimento 2a, os resultados mostraram que os grupos microinjetados com salina e CPA nas doses de 0,016 nmol, 0,052 nmol e 0,16 nmol reduziram a exploração dos BA na reexposição, o que sugere a CPA não apresentou efeitos sobre a consolidação da memória emocional. No experimento 2b, a CPA também não apresentou efeito nas doses utilizadas no teste de EI. No experimento 3a, a análise estatística indicou que os animais que receberam RA na dose de 5,7 não apresentaram redução na exploração dos BA, o que sugere prejuízo na consolidação da memória. Os resultados do experimento 3b mostraram que a RA na dose de 5,7 nmol prejudicou a consolidação da memória emocional no teste de EI. Os resultados do estudo 4a com injeção combinada de antagonista H1 e HA em camundongos reexpostos ao LCE mostraram que os animais microinjetados com SAL+SAL, CPA+SAL e CPA+HA reduziram a porcentagem de entradas e de tempo nos braços abertos, enquanto que os animais do grupo SAL+HA não apresentaram diferença significativa na exploração dos BA na reexposição, confirmando os resultados do experimento 1a em que animais injetados com HA (4,07 nmol) apresentam prejuízo na consolidação da memória emocional. Além disso, os resultados mostraram que a CPA não alterou os parâmetros comportamentais quando aplicada por si só, e que foi capaz de reverter o déficit produzido pela histamina na consolidação da memória emocional em camundongos no LCE. No experimento 4b no teste de EI, os resultados mostraram que os grupos que receberam injeção combinada de antagonista H1 e histamina (CPA+HA) e a injeção de SAL+HA apresentaram diferença significativa no tempo de latência no segundo dia de teste em relação ao grupo controle SAL+SAL, enquanto o grupo tratado com CPA+SAL não apresentou diferença com o grupo SAL+SAL. Esses resultados mostram que a microinjeção de histamina no vérmis cerebelar aumentou o tempo de latência, e que o pré-tratamento com CPA não reverteu esse efeito. Para o experimento 5a, com microinjeção combinada de antagonista H2 e HA em camundongos submetidos ao LCE, os resultados mostraram que animais microinjetados com SAL+SAL e RA+SAL reduziram a porcentagem de entrada e de tempo nos braços abertos, enquanto os grupos tratados com RA+HA e SAL+RA não apresentaram diferença entre os dias de teste nesse parâmetros. Estes resultados mostraram que a RA não alterou a consolidação da memória e não foi capaz de reverter o efeito da histamina. Já no experimento 5b com a microinjeção combinada de RA e HA no teste de EI, houve diferença significativa entre os grupos SAL+SAL e SAL+HA, mostrando novamente o efeito facilitador da histamina na consolidação da memória de EI. Os grupos que receberam injeção combinada de antagonista H2 e histamina (RA+HA) e o grupo de recebeu RA+SAL não apresentaram diferença significativa em relação ao controle no tempo de latência no segundo dia de teste, o que mostra que a RA não apresentou efeito por si só, mas quando aplicada pré histamina foi capaz de reverter seu efeito. Os resultados dos diversos experimentos realizados parecem indicar efeitos da histamina em circuitos neurais diferentes em tarefas envolvendo medo ou ansiedade.Universidade Federal de Minas Geraisapplication/pdfporUniversidade Federal de São CarlosPrograma de Pós-Graduação em Fisioterapia - PPGFtUFSCarBRPsicofarmacologiaSistema histaminérgicoCerebeloMemória emocionalConsolidação (memória)HistaminaHistaminergic systemEmotional memoryConsolidationCerebellumCIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONALInfluência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongosinfo:eu-repo/semantics/publishedVersioninfo:eu-repo/semantics/doctoralThesisinfo:eu-repo/semantics/openAccessreponame:Repositório Institucional da UFSCARinstname:Universidade Federal de São Carlos (UFSCAR)instacron:UFSCARORIGINAL5721.pdfapplication/pdf10685553https://{{ getenv "DSPACE_HOST" "repositorio.ufscar.br" }}/bitstream/ufscar/5170/1/5721.pdfb8c33e77b08071259076d9ba53ebc334MD51TEXT5721.pdf.txt5721.pdf.txtExtracted texttext/plain0https://{{ getenv "DSPACE_HOST" "repositorio.ufscar.br" }}/bitstream/ufscar/5170/2/5721.pdf.txtd41d8cd98f00b204e9800998ecf8427eMD52THUMBNAIL5721.pdf.jpg5721.pdf.jpgIM Thumbnailimage/jpeg6748https://{{ getenv "DSPACE_HOST" "repositorio.ufscar.br" }}/bitstream/ufscar/5170/3/5721.pdf.jpg2ffff5956039cb16685f2beaa7fb8615MD53ufscar/51702019-09-11 04:16:38.342oai:repositorio.ufscar.br:ufscar/5170Repositório InstitucionalPUBhttps://repositorio.ufscar.br/oai/requestopendoar:43222019-09-11T04:16:38Repositório Institucional da UFSCAR - Universidade Federal de São Carlos (UFSCAR)false |
| dc.title.por.fl_str_mv |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| title |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| spellingShingle |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos Gianlorenço, Anna Carolyna Lepesteur Psicofarmacologia Sistema histaminérgico Cerebelo Memória emocional Consolidação (memória) Histamina Histaminergic system Emotional memory Consolidation Cerebellum CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL |
| title_short |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| title_full |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| title_fullStr |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| title_full_unstemmed |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| title_sort |
Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos |
| author |
Gianlorenço, Anna Carolyna Lepesteur |
| author_facet |
Gianlorenço, Anna Carolyna Lepesteur |
| author_role |
author |
| dc.contributor.authorlattes.por.fl_str_mv |
http://lattes.cnpq.br/3861050459671690 |
| dc.contributor.author.fl_str_mv |
Gianlorenço, Anna Carolyna Lepesteur |
| dc.contributor.advisor1.fl_str_mv |
Mattioli, Rosana |
| dc.contributor.advisor1Lattes.fl_str_mv |
http://genos.cnpq.br:12010/dwlattes/owa/prc_imp_cv_int?f_cod=K4797764Z6 |
| contributor_str_mv |
Mattioli, Rosana |
| dc.subject.por.fl_str_mv |
Psicofarmacologia Sistema histaminérgico Cerebelo Memória emocional Consolidação (memória) Histamina |
| topic |
Psicofarmacologia Sistema histaminérgico Cerebelo Memória emocional Consolidação (memória) Histamina Histaminergic system Emotional memory Consolidation Cerebellum CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL |
| dc.subject.eng.fl_str_mv |
Histaminergic system Emotional memory Consolidation Cerebellum |
| dc.subject.cnpq.fl_str_mv |
CIENCIAS DA SAUDE::FISIOTERAPIA E TERAPIA OCUPACIONAL |
| description |
This study investigated the function of cerebellar histaminergic system on emotional memory consolidation. The cerebellar vermis of male mice were implanted with guide cannulae, and after three days of recovery, the animals were submitted to the elevated plus maze (EPM) or the inhibitory avoidance test (IA) on two consecutive days. Immediately after the first day, animals received a microinjection of histaminergic drugs into the cerebellar vermis: experiment 1, animals received microinjections of saline (SAL) or histamine (HA) (0.54, 1.36, 2.72, and 4.07 nmol/0.1 microliter); experiment 2, animals received a microinjection of SAL or the H1 antagonist chlorpheniramine (CPA, 0.016, 0.052 or 0.16 nmol/0.1 μl); experiment 3, SAL or the H2 antagonist ranitidine (RA, 0.57, 2.85 or 5.7 nmol/0.1 μl); experiment 4, SAL or HA 5 minutes after a pretreatment with 0.16 nmol CPA or SAL; and experiment 5, SAL or HA 5 minutes after a pretreatment with 2.85 nmol ranitidine (RA) or SAL. In the EPM, the decrease of open arm exploration (% entries and % time spent in the open arms) in Trial 2 relative to Trial 1 was used as a measure of learning and memory; while in the IA, latency to cross to the dark compartment was used to evaluate memory retention. Data were analyzed using ANOVA and Duncan‟s test. The results of experiment 1 showed that animals microinjected SAL and 0.54 and 1.36 nmol HA reduced percentage of open arm entries and time, while mice microinjected with HA 2.72 and 4.07 nmol did not decrease open arm exploration on trial 2; which indicates that histamine induced a dose-dependent inhibitory effect on memory consolidation. In the IA task, results showed that 1.36 nmol histamine facilitated memory consolidation, suggesting a different action of HA in a memory model that uses punishment. In the experiment 2, microinjections with CPA did not present behavioral effects in the EPM or in the IA at the doses used (0.016, 0.052 and 0.16 nmol). The results of experiment 3 showed that 5.7 nmol RA impaired memory consolidation on both protocols. The experiment 4 demonstrated that animals treated with HA did not reduce the avoidance to the open arms on retesting, and indicated that CPA did not altered behavioral parameters by itself, but the pretreatment with CPA reverted histamine-induced impairment on memory consolidation, which suggests that histamine effect on the EPM was mediated by H1 receptors. In the IA test, the results showed that the groups that received CPA+HA and SAL+HA showed a significant difference in latency on the second day of testing in relation to group SAL+SAL , while the group treated with CPA + SAL showed no difference with the control group. These results show that microinjection of histamine in the cerebellar vermis increased latency time and that pretreatment with CPA did not reverse this effect. For the fifth experiment, the results showed that animals microinjected with SAL+SAL and RA+SAL reduced the percentage of entries and time spent in open arms in the EPM while the groups treated with RA+HA and SAL+HA showed no difference between test days. These results show that RA did not alter memory consolidation and was unable to reverse the effect of histamine. In the IA, there was significant difference between SAL+SAL and SAL+HA groups, showing the facilitatory effect of histamine on memory consolidation of IA. The groups that received combined injection of RA+SAL and RA+HA showed no significant difference compared to control, which shows that the RA had no effect by itself, but when applied before histamine was able to reverse its effect. Our results suggest different histamine effects in tasks involving anxiety or fear. |
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2014 |
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2014-02-24 2016-06-02T20:18:22Z |
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2014-02-10 |
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2016-06-02T20:18:22Z |
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GIANLORENÇO, Anna Carolyna Lepesteur. Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos. 2014. 164 f. Tese (Doutorado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2014. |
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https://repositorio.ufscar.br/handle/ufscar/5170 |
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GIANLORENÇO, Anna Carolyna Lepesteur. Influência do sistema histaminérgico cerebelar na consolidação da memória emocional de camundongos. 2014. 164 f. Tese (Doutorado em Ciências Biológicas) - Universidade Federal de São Carlos, São Carlos, 2014. |
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