Human X-chromosome inactivation pattern distributions fit a model of genetically influenced choice better than models of completely random choice

Renault, Nicolas; Pritchett, Sonja; Howell, Robin E.; Greer, Wenda L.; Sapienza, Carmen; Ørstavik, Karen Helene; Hamilton, David C.

doi:10.1038/ejhg.2013.84

Cited by 21 publications

(15 citation statements)

References 34 publications

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“…The absence of a consistent pattern of X inactivation between mothers and daughters supports a generational resetting of X inactivation. 21 In previous studies of X-linked diseases, large deletions were more likely to cause skewing than point mutations. 22 Although this might be true in CGD carriers as well, we analyzed only granulocytes, and therefore differences in other tissues might show different patterns.…”

Section: Discussionmentioning

confidence: 90%

X-linked carriers of chronic granulomatous disease: Illness, lyonization, and stability

Marciano

Zerbe

Falcone

et al. 2018

Journal of Allergy and Clinical Immunology

152

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Section: Discussionmentioning

confidence: 90%

X-linked carriers of chronic granulomatous disease: Illness, lyonization, and stability

Marciano

Zerbe

Falcone

et al. 2018

Journal of Allergy and Clinical Immunology

152

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“…X chromosome inactivation likely has profound but somewhat unpredictable effects on tumorigenesis in women compared with in men. The inactivation process is not entirely understood and until recently was thought to be a random process; however, recent studies suggest otherwise [109,110]. Approximately 15% of X chromosomes escape inactivation and another 10% show variable patterns of inactivation [111].…”

Section: Inactivation Processmentioning

confidence: 97%

“…Decreased B cell activation, differentiation and survival [64] Low CD 3 + T lymphocytes [53] Increased T cell apoptosis [151] Low IL2 and TH1 responses and thus suppression of T and B-lymphocytes development [53] Oxidative processes -Decreased oxidative damage to mitochondrial DNA [82] -Estrogen protects cells against oxidative stress and acts as a direct antioxidant [82] -High level of anti-oxidant enzymes [86] -High oxidative damage to mitochondrial DNA (4-fold higher compared with women) [82] -Androgens diminish protection against oxidative stress [85] -Decreased number of anti-oxidants and anti-oxidant enzymes [86] -Elevated ROS cellular environment promote tumor metastasis [75,86,87] Sex chromosomes -X chromosome inactivation process: [55,108,109] Decreased tissue X chromosome oncogenes expression [mi-RNAs, cancer/testis antigens (CT-X)] [117][118][119][120][121] Tissue mosaicism in X chromosome associated oncogenes -Lack of Y chromosome associated oncogenes -No X chromosome inactivation process: [55,108,109] Monosomic expression of X chromosome specific oncogenes Increased tissue expression of X chromosome oncogenes -Y chromosome associated oncogene expression [TSPY] [133][134][135][136]139] DNA binding sites to elicit transcriptional regulation of target genes. Studies from androgen receptor knockout mouse models demonstrate that androgens influence the promotion of tumorigenesis in liver and prostate cancer and promote both tumorigenesis and metastasis in bladder, lung, kidney cancers [43], which have sex disparities in outcome favoring women (Table 1, Supplemental Fig.…”

Section: Male Sex Hormonesmentioning

confidence: 99%

Sex disparities in melanoma outcomes: The role of biology

Nosrati¹,

Wei²

2014

Archives of Biochemistry and Biophysics

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“…In this study, we denote this phenomenon of skewed XCI as XCI-S. The skewness of XCI has been defined using an arbitrary threshold as inactivation of one of the alleles in more than 75% of cells [Abkowitz et al, 1998;Chabchoub et al, 2009;Minks et al, 2008;Naumova et al, 1998;Renault et al, 2013;Sharp et al, 2000;Wong et al, 2011]. Extreme or severe skewness, which is defined as inactivation of one of the alleles in more than 90% of cells, has also been observed [Amos-Landgraf et al, 2006;Busque et al, 1996;Champion et al, 1997;Gale et al, 1997;Hatakeyama et al, 2004;Minks et al, 2008;Sharp et al, 2000;Tonon et al, 1998;Willard, 2000;Wong et al, 2011].…”

Section: Introductionmentioning

confidence: 99%

X-Chromosome Genetic Association Test Accounting for X-Inactivation, Skewed X-Inactivation, and Escape from X-Inactivation

2014

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X-chromosome inactivation (XCI) is the process in which one of the two copies of the X-chromosome in females is randomly inactivated to achieve the dosage compensation of X-linked genes between males and females. That is, 50% of the cells have one allele inactive and the other 50% of the cells have the other allele inactive. However, studies have shown that skewed or non-random XCI is a biological plausibility wherein more than 75% of cells have the same allele inactive. Also, some of the X-chromosome genes escape XCI, i.e., both alleles are active in all cells. Current statistical tests for X-chromosome association studies can either account for random XCI (e.g., Clayton’s approach) or escape from XCI (e.g., PLINK software). Because the true XCI process is unknown and differs across different regions on the X-chromosome, we proposed a unified approach of maximizing likelihood ratio over all biological possibilities: random XCI, skewed XCI, and escape from XCI. A permutation-based procedure was developed to assess the significance of the approach. We conducted simulation studies to compare the performance of the proposed approach with Clayton’s approach and PLINK regression. The results showed that the proposed approach has higher powers in the scenarios where XCI is skewed while losing some power in scenarios where XCI is random or XCI is escaped, with well-controlled type I errors. We also applied the approach to the X-chromosomal genetic association study of head and neck cancer.

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Human X-chromosome inactivation pattern distributions fit a model of genetically influenced choice better than models of completely random choice

Cited by 21 publications

References 34 publications

X-linked carriers of chronic granulomatous disease: Illness, lyonization, and stability

X-linked carriers of chronic granulomatous disease: Illness, lyonization, and stability

Sex disparities in melanoma outcomes: The role of biology

X-Chromosome Genetic Association Test Accounting for X-Inactivation, Skewed X-Inactivation, and Escape from X-Inactivation

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