Whole-Genome Sequencing Reveals Exonic Variation of ASIC5 Gene Results in Recurrent Pregnancy Loss

Qahtani, Nourah Hasan Al; AbdulAzeez, Sayed; Almandil, Noor B.; Alhur, Norah Fahad; Alsuwat, Hind Saleh; Taifi, Hatoon Ahmed Al; Alghamdi, Ahlam; Jermy, B. Rabindran; Abouelhoda, Mohamed; Subhani, Shazia; Asoom, Lubna Ibrahim Al; Borgio, J. Francis

doi:10.3389/fmed.2021.699672

Cited by 10 publications

(7 citation statements)

References 58 publications

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“…One of the fetal tissue reported with homozygous ASIC5 Saudi mutation. 27 As the fetal tissue samples were collected from aborted 9-week fetuses therefore clinical confirmation of the gender of the fetus could not be achieved. Early prenatal diagnosis of gender and identification of disease associated mutations can provide effective decision making in the mother among high-consanguinity population to decide within the allowed time.…”

Section: Discussionmentioning

confidence: 99%

“…Early prenatal diagnosis of gender and identification of disease associated mutations can provide effective decision making in the mother among high-consanguinity population to decide within the allowed time. 27 , 28 The eight pairs of primers designed in the study is highly specific, sensitive, unique and well matched for the simultaneous detection of the male specific Y-biomarkers, SRY, DAZ2 and TSPY1 genes and the internal control, ACTB gene for both conventional PCR and real-time qPCR. The specificity of the primers were confirmed through sequencing.…”

Section: Discussionmentioning

confidence: 99%

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Fetal Nucleated Red Blood Cells Preferable Than Cell-Free Fetal DNA for Early Determination of Gender Among Invasive and Non-Invasive Source Using Novel Four Genes Multiplex PCR

Alhur¹,

Qahtani²,

AlSuhaibani³

et al. 2021

IJGM

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Background Deoxyribonucleic acid from invasive, non-invasive and 9th week embryo can be a resource for the determination of fetal sex using highly sensitive and specific multiplex PCR. Methods A total of 402 DNA samples were used to test the newly developed novel multiplex PCR including male specific (3 genes: SRY, DAZ2 and TSPY1 ) Y-biomarkers and internal control, ACTB . The study isolated cffDNA (Cell-free fetal DNA; n = 73) from mother’s plasma, serum and urine, fetal DNA from 9th week embryo and cord blood, and fetal DNA from CD71 +ve nucleated red blood cells (fNRBC; n = 73). Paternal and maternal DNA from buccal cells (n = 20) and blood (n = 232) used for male and female confirmation. Results The study observed that SRY alone cannot be a suitable Y-biomarker. Confirmation from any two Y-biomarkers is mandatory for male fetus identification. Direct sequencing of the gel eluted multiplex and single amplicons confirmed the specific sequences. Presence of two out of 3 Y-biomarkers OR single Y-biomarker with >1,000,000 intensity is considered positive for male. The multiplex PCR is suitable for determining sex from all source of fetal DNA including highly degraded cffDNA and can detect the sex using 0.5ng DNA. Individual marker-based real-time qPCR followed by combined melt curve analysis showed distinguished melt curve peaks for the markers. Conclusion The multiplex PCR achieved 100% accuracy on fetal DNA from fNRBC for early determinations (<13 weeks) of gender. The developed novel and simple multiplex PCR and individual qPCR can be adopted in all types of laboratories for determining human fetal gender using fetal DNA from fNRBC. Early identification of gender can support to prepare for possible X-linked analysis, reduce anxiety in mother, strengthen a bond between mother and fetus, and effective decision making. Non-invasive source of fetal DNA from fNRBC preferred for identifying gender to reduce the risk of invasive procedures in early (8–13 weeks) pregnancy.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Fetal Nucleated Red Blood Cells Preferable Than Cell-Free Fetal DNA for Early Determination of Gender Among Invasive and Non-Invasive Source Using Novel Four Genes Multiplex PCR

Alhur¹,

Qahtani²,

AlSuhaibani³

et al. 2021

IJGM

Self Cite

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“…Genetic abnormalities such as chromosome abnormalities, submicroscopic chromosome deletion and duplications, and gene sequence variation are the major genetic causes of female infertility [ 22 ]. Whole-genome sequencing revealed that even single gene causes could explain infertility and pregnancy complications [ 23 ]. However, these complications are often challenging due to their multitissue and multiorganism nature.…”

Section: Factors Affecting Female Infertilitymentioning

confidence: 99%

Angiotensin-Converting Enzyme (ACE) Insertion/Deletion (I/D) Polymorphism as a Conjoint Regulator of Coagulation, Fibrinolytic, and RAAS Pathway in Infertility and Associated Pregnancy Complications

Kumar¹,

Sharma

Kaur³

et al. 2022

J Renin Angiotensin Aldosterone Syst

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Despite the increase in assisted reproductive technologies, the high rates of infertility and pregnancy complications are a major concern to infertility specialists worldwide. Infertility may be attributed to pregnancy complications like thrombophilia, preeclampsia and fibrin-induced recurrent pregnancy loss (RPL). Renin-angiotensin-aldosterone system (RAAS) directly or indirectly causes preeclampsia and thrombophilia through the fibrinolytic pathway that ultimately leads to RPL or infertility. The underlying mechanisms of this interaction are still unclear. The present comprehensive review is intended to demonstrate the role and interaction of RAAS and fibrinolytic pathways in pregnancy complications. How this interaction can induce pregnancy complications, and ultimately infertility, is also discussed in the light of current evidence. This study also presents common markers that link RAAS and fibrinolytic processes in developing thrombophilia, preeclampsia and RPL. The common link in these pathways is ACE gene I/D polymorphism. Apart from ACE, PAI-1, VIIa, XIIa, AT1R, AT1AA, and TF are common molecules that can delineate the underlying causes of pregnancy complications and infertility.

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“…Studies on systemic juvenile idiopathic arthritis (LACC1 gene) [80,81]; recurrent pregnancy loss (ASIC5 gene) [82]; tricho-hepato-enteric syndrome (SKIV2L and TTC37 genes) [83];…”

Section: Other Genetic Diseasesmentioning

confidence: 99%

“…Variants in the Mendeliome in Saudi ancestry – APC-related Cenani-Lenz syndrome, Steel syndrome, syndromic cataract, oral-facial-digital syndrome, CHARGE-like presentation, epileptic encephalopathy, Ehlers-Danlos-like syndrome, and congenital hydrocephalus – were reported either with compatible phenotypes (homozygous variant in 30 genes) or phenotypes different from the original reports (homozygous mutations in 18 candidate genes) [ 79 ]. Studies on systemic juvenile idiopathic arthritis ( LACC1 gene) [ 80 , 81 ]; recurrent pregnancy loss ( ASIC5 gene) [ 82 ]; tricho-hepato-enteric syndrome ( SKIV2L and TTC37 genes) [ 83 ]; STING-associated vasculopathy of infantile-onset ( STING1 gene) [ 84 ]; multiple congenital anomaly syndrome ( SMG9 gene) [ 85 ]; diabetic retinopathy ( NME3 , LOC728699 , and FASTK genes) [ 86 ]; congenital neutropenia with inflammatory bowel disease ( G6PC3 gene) [ 87 ]; skeletal dysplasia ( XYLT1 ) [ 88 , 89 ]; Wolf–Hirschhorn syndrome ( WHSC1 gene) [ 90 ]; lymphatic dysplasia with nonimmune hydrops fetalis ( PIEZO1 ) [ 89 ]; Cohen syndrome ( VPS13B gene) [ 91 ]; severe combined immunodeficiency disease ( AK2 , JAK3 , and MTHFD1 genes) [ 92 ]; celiac disease ( CPED1 gene) [ 93 ]; hereditary spherocytosis type 3 ( SPTA1 gene) [ 89 ]; developmental delay, cerebellar hypoplasia, and myoclonic seizures ( KCNMA1 gene) [ 74 ]; Cenani-Lenz syndrome ( APC gene) [ 74 ]; Sjogren-Larsson syndrome ( ELOVL4 gene) [ 74 ]; autism spectrum disorder (multigene) [ 94 ]; congenital heart disease ( PRKD1 gene) [ 95 ]; ciliopathies [ 96 ]; Parkinsonism ( PLA2G6 gene) [ 97 ]; retinal dystrophies ( CLRN1 , ABCA4 , CERKL , AGBL5 , CDH16 , and DNAJC17 genes) [ 98 – 100 ]; pediatric asthma [ 101 ]; cardiovascular genetic diseases ( LDLR gene) [ 102 ]; enteroendocrine dysfunction ( PCSK1 ) [ 103 ]; tricho-hepato-enteric syndrome ( TTC37 and SKIV2L ) [ 104 ]; Wolcott–Rallison syndrome ( EIF2AK3 ) [ 105 ], Fanconi–Bickel syndrome ( SLC2A2 ) [ ...…”

Section: Other Genetic Diseasesmentioning

confidence: 99%

Heterogeneity in biomarkers, mitogenome and genetic disorders of Arab population with special emphasis on large-scale whole-exome sequencing

Borgio

2021

Arch Med Sci

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More than 25 million DNA variations were discovered as novel including major alleles from Arab population. Exome studies on Arabs discovered >3000 novel nucleotide variants associated with >1200 rare genetic disorders. Reclassification of many pathogenic variant into benign through the Arab database enhance building a detailed and comprehensive map of Arab morbid genome. Intellectual disability stands first with the combined and observed carrier frequency. Genome studies and advanced computational biology discovered interesting novel candidate disease marker variations in many genes from consanguineous families with intellectual disability, neurogenetic disorders, blood and bleeding disorder and rare genetic diseases. Pathogenic variants in C12orf57 gene are prominently associated with the etiology of developmental delay/intellectual impairment. Arab mitogenome exposed hundreds of variations in mtDNA genome and its association with obesity. Further study is needed in genomics to fully comprehend the molecular abnormalities and associated pathogenesis that cause inherited disorders in Arab ancestries.

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Whole-Genome Sequencing Reveals Exonic Variation of ASIC5 Gene Results in Recurrent Pregnancy Loss

Cited by 10 publications

References 58 publications

Fetal Nucleated Red Blood Cells Preferable Than Cell-Free Fetal DNA for Early Determination of Gender Among Invasive and Non-Invasive Source Using Novel Four Genes Multiplex PCR

Fetal Nucleated Red Blood Cells Preferable Than Cell-Free Fetal DNA for Early Determination of Gender Among Invasive and Non-Invasive Source Using Novel Four Genes Multiplex PCR

Angiotensin-Converting Enzyme (ACE) Insertion/Deletion (I/D) Polymorphism as a Conjoint Regulator of Coagulation, Fibrinolytic, and RAAS Pathway in Infertility and Associated Pregnancy Complications

Heterogeneity in biomarkers, mitogenome and genetic disorders of Arab population with special emphasis on large-scale whole-exome sequencing

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