A Comparison of Chikungunya Virus Infection, Dissemination, and Cytokine Induction in Human and Murine Macrophages and Characterization of RAG2-/-γc-/- Mice as an Animal Model to Study Neurotropic Chikungunya Disease

Guerrero, Israel

07 April 2020

Chikungunya virus (CHIKV) is classified as an alphavirus in the Togaviridae family. This virus is known to rely on Aedes arthropod vectors for its dissemination. Human infection is characterized by rash, high fever, and severe chronic polyarthritis that can last for years. Recently, efforts in developing animal models have been made in an attempt to better understand CHIKV pathogenesis. CHIKV infection starts with a 7 to 10 day long febrile acute phase, in which most of the symptoms occur (rash, fever, and incapacitating pain in joints and muscle). Once the immune system clears most of the viral infection, a chronic phase starts in as many as 70% of the infected patients. Long term virus-related polyarthralgia is the hallmark of the CHIKV chronic phase. It is believed that CHIKV-infected macrophages infiltrate the joints during the acute phase, and CHIKV infects joint tissue and persists in it. Research into the effects of CHIKV infection in human and murine macrophages revealed that CHIKV-infected human macrophages produce high amounts of virions as well as induce the production of pro-inflammatory cytokines and monocyte recruiting chemokines. This contrasts with murine macrophage infection where low quantities of the virus were detected as well as lower production of pro-inflammatory cytokines. This may contribute to the lack of polyarthritis in murine animal models. Current literature suggests that CHIKV’s viral proteins bind and interact with human host cell machinery promoting viral replication more efficiently in humans than in mice. CHIKV-related neuropathology is not the most common outcome of the disease. However, recent outbreaks suggest that this pathology is becoming more prevalent, affecting as many as 30% of confirmed patients. The role of adaptive and innate immunity in CHIKV disease amelioration has been extensively, yet separately, explored. A RAG2-/-γc-/- Balb/c mouse model was used to study the role of these immune pathways and their associated immune cells in CHIKV infection. The mice in this study developed local arthritis at the site of inoculation as well as showed signs of viral invasion in the brain. This study added to the hypothesis that both innate and adaptive immune responses are necessary to ameliorate the disease and that the lack of adequately matured lymphocytes and STAT6-activation deficient macrophages may result in more severe pathologies.

Chikungunya virus

polyarthralgia

macrophage

cytokine

RAG2-/-γc-/- Balb/c mouse model

neuropathology

Life Sciences

Mapeamento genético e caracterização fenotípica do mutante anêmico induzido por Ethyl-nitroso-urea. / Genetic mapping and phenotypic characterization of an anemic mutant by ethylnitrosourea.

Cruz, Carolina Cavalcante da

24 September 2009

A mutagênese química utilizando o agente mutagênico N-ethyl-N-nitrosourea (ENU) seguida da observação do fenótipo deu origem a um mutante Anêmico. O tipo de herança é autossômica dominante, com morte intra útero dos mutantes homozigotos. O mapeamento genético foi feito utilizando-se marcadores microssatélites, sendo selecionados marcadores polimórficos entre as linhagens BALB/c e C57BL/6 envolvidas no mapeamento. Estabeleceu-se um painel de microssatélites distribuídos por todo o genoma do camundongo, que permitisse a localização do cromossomo portador da mutação. O gene mutante foi localizado no cromossomo 7 entre os marcadores D7Mit301 e D7Mit131 delimitando um intervalo entre 46,5cM e 51cM de 4,5cM. Através das análises fenotípicas do mutante Anêmico e estudo dos genes candidatos neste intervalo, foi selecionado o gene Hbb responsável pela síntese das globinas b-major e b-minor , sendo o gene que mais se identifica com as características do mutante, localizado a 50cM. A deficiência deste gene leva a uma das mais severas anemias humana, a b-Talassemia major. / Chemical mutagenesis, using the mutagenic agent N-ethyl-N-nitrosourea (ENU), and followed by observation of the phenotype, originated in an Anaemic mutant. The inheritance-type is dominant auto-somic, with intra-uterus death of the homozygotic mutants. Genetic mapping was undertaken by means of micro-satellite markers, polymorphic markers being selected from among the BALB/c and C57BL/6 lineages involved in the mapping itself. A panel was established of the micro-satellites distributed throughout the whole mouse genome, thereby permitting localization of the mutation bearing chromosome. The mutant gene was located in chromosome 7 between markers D7Mit301 and D7Mit131, these delimiting an interval between 46,5cM and 51cM of 4,5cM. Selection of the Hbb gene responsible for synthesis of the b-major and b-minor globins came about through phenotypic analysis of the Anaemic mutant and a study of candidate genes within this interval, the selected gene being that which was most identified with the mutants characteristics and located at 50cM. A deficiency in this gene leads to one of the most severe forms of human anaemia, b-Talhassemia major.

Anemia hemolítica

BALB/c mouse

Biotechnology

Biotecnologia

Camundongos BALB/c

Fenótipos (características)

Genetic mapping

Hemolytic anemia

Induced gene mutation

Mapeamento genético

Mutação genética induzida

Mutagênese

Mutagenesis

Phenotype (characteristics)

Mapeamento genético e caracterização fenotípica do mutante anêmico induzido por Ethyl-nitroso-urea. / Genetic mapping and phenotypic characterization of an anemic mutant by ethylnitrosourea.

Carolina Cavalcante da Cruz

24 September 2009

A mutagênese química utilizando o agente mutagênico N-ethyl-N-nitrosourea (ENU) seguida da observação do fenótipo deu origem a um mutante Anêmico. O tipo de herança é autossômica dominante, com morte intra útero dos mutantes homozigotos. O mapeamento genético foi feito utilizando-se marcadores microssatélites, sendo selecionados marcadores polimórficos entre as linhagens BALB/c e C57BL/6 envolvidas no mapeamento. Estabeleceu-se um painel de microssatélites distribuídos por todo o genoma do camundongo, que permitisse a localização do cromossomo portador da mutação. O gene mutante foi localizado no cromossomo 7 entre os marcadores D7Mit301 e D7Mit131 delimitando um intervalo entre 46,5cM e 51cM de 4,5cM. Através das análises fenotípicas do mutante Anêmico e estudo dos genes candidatos neste intervalo, foi selecionado o gene Hbb responsável pela síntese das globinas b-major e b-minor , sendo o gene que mais se identifica com as características do mutante, localizado a 50cM. A deficiência deste gene leva a uma das mais severas anemias humana, a b-Talassemia major. / Chemical mutagenesis, using the mutagenic agent N-ethyl-N-nitrosourea (ENU), and followed by observation of the phenotype, originated in an Anaemic mutant. The inheritance-type is dominant auto-somic, with intra-uterus death of the homozygotic mutants. Genetic mapping was undertaken by means of micro-satellite markers, polymorphic markers being selected from among the BALB/c and C57BL/6 lineages involved in the mapping itself. A panel was established of the micro-satellites distributed throughout the whole mouse genome, thereby permitting localization of the mutation bearing chromosome. The mutant gene was located in chromosome 7 between markers D7Mit301 and D7Mit131, these delimiting an interval between 46,5cM and 51cM of 4,5cM. Selection of the Hbb gene responsible for synthesis of the b-major and b-minor globins came about through phenotypic analysis of the Anaemic mutant and a study of candidate genes within this interval, the selected gene being that which was most identified with the mutants characteristics and located at 50cM. A deficiency in this gene leads to one of the most severe forms of human anaemia, b-Talhassemia major.

Anemia hemolítica

Biotecnologia

Camundongos BALB/c

Fenótipos (características)

Mapeamento genético

Mutação genética induzida

Mutagênese

BALB/c mouse

Biotechnology

Genetic mapping

Hemolytic anemia

Induced gene mutation

Mutagenesis

Phenotype (characteristics)