Sex-biased chromatin and regulatory cross-talk between sex chromosomes, autosomes, and mitochondria

Silkaitis, Katherine; Lemos, Bernardo

doi:10.1186/2042-6410-5-2

Cited by 38 publications

(30 citation statements)

References 114 publications

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“…The long arm of murine ChrY encodes several multicopy gene families, which exhibit significant strain-specific copy number variation (CNV), and the physiological roles of which are only beginning to be understood (20,21). Importantly, our studies in EAE and CVB3-induced autoimmune myocarditis revealed a strong association between CNV in multicopy ChrY genes and susceptibility to these autoimmune diseases (27,46).…”

Section: Copy Number Variation In Chry Multicopy Genes Does Not Corrementioning

confidence: 87%

“…Importantly, these data suggest that nonendocrine cell-intrinsic (genetic) sex-specific factors may contribute to disease susceptibility in males. In this regard, the concept that genes on the X and Y chromosomes (ChrX and ChrY) may influence sex differences is being increasingly recognized (18)(19)(20)(21), and it was recently suggested that the widely expressed ancestral singlecopy ChrY genes may function as dosage-sensitive regulators of gene expression, translation, and protein stability, and as such may play essential roles in male viability, development, and sex differences in health and disease (22).…”

mentioning

confidence: 99%

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Genetic variation in chromosome Y regulates susceptibility to influenza A virus infection

Krementsov

Case

Dienz

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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Males of many species, ranging from humans to insects, are more susceptible than females to parasitic, fungal, bacterial, and viral infections. One mechanism that has been proposed to account for this difference is the immunocompetence handicap model, which posits that the greater infectious disease burden in males is due to testosterone, which drives the development of secondary male sex characteristics at the expense of suppressing immunity. However, emerging data suggest that cell-intrinsic (chromosome X and Y) sex-specific factors also may contribute to the sex differences in infectious disease burden. Using a murine model of influenza A virus (IAV) infection and a panel of chromosome Y (ChrY) consomic strains on the C57BL/6J background, we present data showing that genetic variation in ChrY influences IAV pathogenesis in males. Specific ChrY variants increase susceptibility to IAV in males and augment pathogenic immune responses in the lung, including activation of proinflammatory IL-17–producing γδ T cells, without affecting viral replication. In addition, susceptibility to IAV segregates independent of copy number variation in multicopy ChrY gene families that influence susceptibility to other immunopathological phenotypes, including survival after infection with coxsackievirus B3. These results demonstrate a critical role for genetic variation in ChrY in regulating susceptibility to infectious disease.

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Section: Copy Number Variation In Chry Multicopy Genes Does Not Corrementioning

confidence: 87%

mentioning

confidence: 99%

Genetic variation in chromosome Y regulates susceptibility to influenza A virus infection

Krementsov

Case

Dienz

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

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“…While the basis for this sex difference is unclear, it is consistent with recent findings that exposure to the persistent organic pollutant polychlorinated biphenyls (PCB) decreased Bdnf (but not Grin2b ) protein levels and Bdnf -mediated signaling in the adult male rat cerebral cortex [43]. We previously observed a male-specific effect of prenatal BPA exposure on reductions in hippocampal Bdnf and Grin2b gene expression and cognitive performance, and these sexspecific effects were likely the typical response to prenatal adversity [20] and may have been mediated by chromosomal, hormonal and epigenetic differences between males and females during fetal development [44–46]. …”

Section: Discussionmentioning

confidence: 99%

Impact of prenatal polycyclic aromatic hydrocarbon exposure on behavior, cortical gene expression, and DNA methylation of the Bdnf gene

et al. 2016

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Prenatal exposure to polycyclic aromatic hydrocarbons (PAH) has been associated with sustained effects on the brain and behavior in offspring. However, the mechanisms have yet to be determined. We hypothesized that prenatal exposure to ambient PAH in mice would be associated with impaired neurocognition, increased anxiety, altered cortical expression of Bdnf and Grin2b, and greater DNA methylation of Bdnf. Our results indicated that during open-field testing, prenatal PAH exposed offspring spent more time immobile and less time exploring. Females produced more fecal boli. Offspring prenatally exposed to PAH displayed modest reductions in overall exploration of objects. Further, prenatal PAH exposure was associated with lower cortical expression of Grin2b and Bdnf in males, and greater Bdnf IV promoter methylation. Epigenetic differences within the Bdnf IV promoter correlated with Bdnf gene expression, but not with the observed behavioral outcomes, suggesting that additional targets may account for these PAH-associated effects.

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“…Moreover, mitochondrial function varies in adult males and females but the origin of these differences is unknown. [116,117] Acknowledging these gaps should lend strong impetus for bridging them with detailed, mechanistic studies.…”

Section: Caveats and Opportunitiesmentioning

confidence: 99%

Sex Differences in Early Embryogenesis: Inter‐Chromosomal Regulation Sets the Stage for Sex‐Biased Gene Networks

Engel

2018

BioEssays

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Sex-specific transcriptional and epigenomic profiles are detectable in the embryo very soon after fertilization. I propose that in male (XY) and female (XX) pre-implantation embryos sex chromosomes establish sexually dimorphic interactions with the autosomes, before overt differences become apparent and long before gonadogenesis. Lineage determination restricts expression biases between the sexes, but the epigenetic differences are less constrained and can be perpetuated, accounting for dimorphisms that arise later in life. In this way, sexual identity is registered in the epigenome very early in development. As development progresses, sex-specific regulatory modules are harbored within shared transcriptional networks that delineate common traits. In reviewing this field, I propose that analyzing the mechanisms for sexual dimorphisms at the molecular and biochemical level and incorporating developmental and environmental factors will lead to a greater understanding of sex differences in health and disease. Also see the video abstract here: https://youtu.be/9BPlbrHtkHQ.

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Sex-biased chromatin and regulatory cross-talk between sex chromosomes, autosomes, and mitochondria

Cited by 38 publications

References 114 publications

Genetic variation in chromosome Y regulates susceptibility to influenza A virus infection

Genetic variation in chromosome Y regulates susceptibility to influenza A virus infection

Impact of prenatal polycyclic aromatic hydrocarbon exposure on behavior, cortical gene expression, and DNA methylation of the Bdnf gene

Sex Differences in Early Embryogenesis: Inter‐Chromosomal Regulation Sets the Stage for Sex‐Biased Gene Networks

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