OSBPL10, RXRA and lipid metabolism confer African-ancestry protection against dengue haemorrhagic fever in admixed Cubans

Sierra, Beatríz; Tříska, Petr; Soares, Pedro; Garcı́a, Gissel; Pérez, Ana B.; Aguirre, Eglys; Oliveira, Marisa; Cavadas, Bruno; Regnault, Béatrice; Álvarez, Mayling; Ruiz, Didye; Samuels, David C.; Sakuntabhai, Anavaj; Pereira, Luı́sa; Guzmán, María G.

doi:10.1371/journal.ppat.1006220

Cited by 55 publications

(55 citation statements)

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“…Importantly, neither DENV nor CHIKV was clinically suspected or was considered in the clinical differential diagnosis and 64.3% of patients were treated with at least one antibacterial drug, of whom almost one in six (11.7%) received dual or triple antimicrobial therapy. A possible explanation of the apparent absence of clinical and/or severe DENV cases in our study, but also in other African settings, is that African heritage genetically protects against severe DENV, more specifically the lower OSBPL10 expression profile in Africans is protective against viral hemorrhagic fever and dengue shock syndrome (31,32).…”

Section: Resultsmentioning

confidence: 46%

Dengue and Chikungunya among Febrile Outpatients in Kinshasa, Democratic Republic of Congo: a cross-sectional study

Proesmans

Katshongo

Milambu³

et al. 2018

Preprint

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Section: Resultsmentioning

confidence: 46%

Dengue and Chikungunya among Febrile Outpatients in Kinshasa, Democratic Republic of Congo: a cross-sectional study

Proesmans

Katshongo

Milambu³

et al. 2018

Preprint

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“…As there are only hundreds of ancestral blocks, these tests have considerable lower statistical burdens than the traditional GWAS with thousands of SNPs. We took advantage of joined admixture-association studies and conducted work in Cuban [59] and Thai (Oliveira et al submitted) cohorts, mapping new candidate genes: lipid metabolism-related OSBPL10 and RXRA; and the already mentioned four genes involved in xenobiotic metabolism (CHST10, AHRR, GRIP1 and PPP2R5E) and…”

Section: Discussionmentioning

confidence: 99%

“…Lastly, the OAS family presented the lower sample sizes screened so far, and with the exceptions of a few individuals from India [35] and Cuba [59] typed for OAS1-rs10774671-G, the Thai cohorts from Simon-Loriere et al [36] dominate these meta-analyses. Notice that Simon-Loriere et al [36] did not provide controls, and in order to be consistent in our tests we included our Thai population screening as controls to compare with these Thai patient cohorts.…”

Section: Tnfa-rs1800629-mentioning

confidence: 99%

“…In this work, we applied population genetics-informed meta-analyses to evaluate the genetic risk/protection conferred by 10 SNPs across seven genes mostly associated with dengue in the literature (PLCE1, TNFA, DC-SIGN/CD209, OAS1, OAS3, FCGR2A/CD32 and MICB; Table 1). We surveyed the literature for case-control cohorts [25,26,27,29,30,35,36,38,40,42,43,44,48,49,53,54,55,56,57,58], took advantage of available datasets chip-genotyped ( [47,59]and Oliveira et al 2018), and added a few case-control cohorts of our own (mostly Cambodia, Vietnam and few Brazilian individuals).…”

Section: Introductionmentioning

confidence: 99%

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Population genetics-informed meta-analysis in seven genes associated with risk to dengue fever disease

Oliveira

Saraiva

Cavadas

et al. 2018

Infection, Genetics and Evolution

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Population genetics theory predicted that rare frequent markers would be the main contributors for heritability of complex diseases, but meta-analyses of genome-wide association studies are revealing otherwise common markers, present in all population groups, as the identified candidate genes. In this work, we applied a population-genetics informed meta-analysis to 10 markers located in seven genes said to be associated with dengue fever disease. Seven markers (in PLCE1, CD32, CD209, OAS1 and OAS3 genes) have high-frequency and the other three (in MICB and TNFA genes) have intermediate frequency. Most of these markers have high discriminatory power between population groups, but their frequencies follow the rules of genetic drift, and seem to have not been under strong selective pressure. There was a good agreement in directional consistency across trans-ethnic association signals, in East Asian and Latin American cohorts, with heterogeneity generated by randomness between studies and especially by low sample sizes. This led to confirm the following significant associations: with DF, odds ratio of 0.67 for TNFA-rs1800629-A; with DHF, 0.82 for CD32-rs1801274-G; with DSS, 0.55 for OAS3-rs2285933-G, 0.80 for PLCE1-rs2274223-G and 1.32 for MICB-rs3132468-C. The overall genetic risks confirmed sub-Saharan African populations and descendants as the best protected against the severer forms of the disease, while Southeast and Northeast Asians are the least protected ones. European and close neighbours are the best protected against dengue fever, while, again, Southeast and Northeast Asians are the least protected ones. These risk scores provide important predictive information for the largely naïve European and North American regions, as well as for Africa where misdiagnosis with other hemorrhagic diseases is of concern.

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“…For example, migrant Chinese have a higher risk of severe dengue fever than local Chinese in Singapore (Xu et al 2018). Furthermore, African ethnicity has been identified as a protective factor for severe symptoms in Cuban dengue patients (Sierra et al 2017). Using data from the 1000 Genomes project, we screened the frequency of rs1285933 alleles of CLEC5A in the African, European, American, South Asian and East Asian populations.…”

Section: Clec5a Polymorphism and Dengue Fevermentioning

confidence: 99%

CLEC5A: A Promiscuous Pattern Recognition Receptor to Microbes and Beyond

Sung

Chang

Hsieh

2020

Advances in Experimental Medicine and Biology

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CLEC5A is a spleen tyrosine kinase (Syk)-coupled C-type lectin that is highly expressed by monocytes, macrophages, neutrophils, and dendritic cells and interacts with virions directly, via terminal fucose and mannose moieties of viral glycans. CLEC5A also binds to N-acetylglucosamine (GlcNAc) and N-acetylmuramic acid (MurNAc) disaccharides of bacterial cell walls. Compared to other C-type lectins (DC-SIGN and DC-SIGNR) and TLRs, CLEC5A binds its ligands with relatively low affinities. However, CLEC5A forms a multivalent hetero-complex with DC-SIGN and other C-type lectins upon engagement with ligands, and thereby mediates microbe-induced inflammatory responses via activation of Syk. For example, in vivo studies in mouse models have demonstrated that CLEC5A is responsible for flaviviruses-induced hemorrhagic shock and neuroinflammation, and a CLEC5A polymorphism in humans is associated with disease severity following infection with dengue virus. In addition, CLEC5A is co-activated with TLR2 by Listeria and Staphylococcus. Furthermore, CLEC5A-postive myeloid cells are responsible for Concanavilin A-induced aseptic inflammatory reactions. Thus, CLEC5A is a promiscuous pattern recognition receptor in myeloid cells and is a potential therapeutic target for attenuation of both septic and aseptic inflammatory reactions.

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OSBPL10, RXRA and lipid metabolism confer African-ancestry protection against dengue haemorrhagic fever in admixed Cubans

Cited by 55 publications

References 50 publications

Dengue and Chikungunya among Febrile Outpatients in Kinshasa, Democratic Republic of Congo: a cross-sectional study

Dengue and Chikungunya among Febrile Outpatients in Kinshasa, Democratic Republic of Congo: a cross-sectional study

Population genetics-informed meta-analysis in seven genes associated with risk to dengue fever disease

CLEC5A: A Promiscuous Pattern Recognition Receptor to Microbes and Beyond

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