Identifying Mutations of the Tetratricopeptide Repeat Domain 37 (TTC37) Gene in Infants With Intractable Diarrhea and a Comparison of Asian and Non-Asian Phenotype and Genotype: A Global Case-report Study of a Well-Defined Syndrome With Immunodeficiency.

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Identifying Mutations of the Tetratricopeptide Repeat Domain 37 (TTC37) Gene in Infants With Intractable Diarrhea and a Comparison of Asian and Non-Asian Phenotype and Genotype: A Global Case-report Study of a Well-Defined Syndrome With Immunodeficiency.

Medicine (Baltimore). 2016 Mar;95(9):e2918

Authors: Lee WI, Huang JL, Chen CC, Lin JL, Wu RC, Jaing TH, Ou LS

Abstract
Syndromic diarrhea/tricho-hepato-enteric syndrome (SD/THE) is a rare, autosomal recessive and severe bowel disorder mainly caused by mutations in the tetratricopeptide repeat domain 37 (TTC37) gene which act as heterotetrameric cofactors to enhance aberrant mRNAs decay. The phenotype and immune profiles of SD/THE overlap those of primary immunodeficiency diseases (PIDs).Neonates with intractable diarrhea underwent immunologic assessments including immunoglobulin levels, lymphocyte subsets, lymphocyte proliferation, superoxide production, and IL-10 signaling function. Candidate genes for PIDs predisposing to inflammatory bowel disease were sequencing in this study.Two neonates, born to nonconsanguineous parents, suffered from intractable diarrhea, recurrent infections, and massive hematemesis from esopharyngeal varices due to liver cirrhosis or accompanying Trichorrhexis nodosa that developed with age and thus guided the diagnosis of SD/THE compatible to TTC37 mutations (homozygous DelK1155H, Fs*2; heterozygous Y1169Ter and InsA1143, Fs*3). Their immunologic evaluation showed normal mitogen-stimulated lymphocyte proliferation, superoxide production, and IL-10 signaling, but low IgG levels, undetectable antibody to hepatitis B surface antigen and decreased antigen-stimulated lymphocyte proliferation. A PubMed search for bi-allelic TTC37 mutations and phenotypes were recorded in 14 Asian and 12 non-Asian cases. They had similar presentations of infantile onset refractory diarrhea, facial dysmorphism, hair anomalies, low IgG, low birth weight, and consanguinity. A higher incidence of heart anomalies (8/14 vs 2/12; P?=?0.0344, Chi-square), nonsense mutations (19 in 28 alleles), and hot-spot mutations (W936Ter, 2779-2G>A, and Y1169Ter) were found in the Asian compared with the non-Asian patients. Despite immunoglobulin therapy in 20 of the patients, 4 died from liver cirrhosis and 1 died from sepsis.Patients of all ethnicities with SD/THE with the characteristic triad of T nodosa, hepatic cirrhosis, and intractable enteropathy have low IgG, poor vaccine response and/or decreased antigen-stimulated lymphocyte proliferation. This is now better classified into the subgroup of “well-defined syndromes with immunodeficiency” (the update termed as “combined immunodeficiencies with associated or syndromic features”) than “predominantly antibody deficiencies” in the update PIDs classification, and requires optimal interventions.

PMID: 26945392 [PubMed – in process]

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Genetics of allergy and allergic sensitization: common variants, rare mutations.

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Genetics of allergy and allergic sensitization: common variants, rare mutations.

Curr Opin Immunol. 2015 Sep 16;36:115-126

Authors: Bønnelykke K, Sparks R, Waage J, Milner JD

Abstract
Our understanding of the specific genetic lesions in allergy has improved in recent years due to identification of common risk variants from genome-wide association studies (GWAS) and studies of rare, monogenic diseases. Large-scale GWAS have identified novel susceptibility loci and provided information about shared genetics between allergy, related phenotypes and autoimmunity. Studies of monogenic diseases have elucidated critical cellular pathways and protein functions responsible for allergy. These complementary approaches imply genetic mechanisms involved in Th2 immunity, T-cell differentiation, TGF? signaling, regulatory T-cell function and skin/mucosal function as well as yet unknown mechanisms associated with newly identified genes. Future studies, in combination with data on gene expression and epigenetics, are expected to increase our understanding of the pathogenesis of allergy.

PMID: 26386198 [PubMed – as supplied by publisher]

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Air fresheners and scented candles could cause cancerous DNA mutations and asthma – Daily Mail


Daily Mail

Air fresheners and scented candles could cause cancerous DNA mutations and asthma
Daily Mail
A 2007 study also found that using air fresheners as little as once a week can raise the risk of asthma in adults. The same report found that the risk of developing asthma was up to 50 per cent higher in people who had been exposed to air-freshener sprays.

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Investigating mutations of a crucial gene might assist treatment and … – Medical Xpress


Medical Xpress

Investigating mutations of a crucial gene might assist treatment and
Medical Xpress
Allergic asthma affects the lives of millions but new research may help to prevent or suppress an allergic response. Credit: Giorez/iStock/Thinkstock. Mutations in a specific gene are linked with human susceptibility to allergic asthma according to new

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Genetic Mutations in Asthma Come into Question – Genetic Engineering & Biotechnology News

Genetic Mutations in Asthma Come into Question
Genetic Engineering & Biotechnology News
Estimates of heritability for asthma sufferers would suggest that nearly half of the variation in risk can be attributed to some type of genetic factor. However, common genetic variants that have been identified by genome-wide association studies (GWAS
Rare mutations do not explain 'missing heritability' in asthmaMedical Xpress
Rare mutations do not explain "missing heritability" in asthmaHealthCanal.com

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Rare mutations do not explain “missing heritability” in asthma – HealthCanal.com

Rare mutations do not explain "missing heritability" in asthma
HealthCanal.com
Despite a strong suspected link between genetics and asthma, commonly found genetic mutations account for only a small part of the risk for developing the disease — a problem known as missing heritability. Rare and low frequency genetic mutations have …
Rare mutations do not explain 'missing heritability' in asthmaMedical Xpress
Genetic Mutations in Asthma Come into QuestionGenetic Engineering & Biotechnology News

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Gene mutations in primary ciliary dyskinesia related to otitis media.

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Gene mutations in primary ciliary dyskinesia related to otitis media.

Curr Allergy Asthma Rep. 2014 Mar;14(3):420

Authors: Mata M, Milian L, Armengot M, Carda C

Abstract
Otitis media with effusion (OME) is the most common cause of conductive hearing loss in children and is strongly associated with primary ciliary dyskinesia (PCD). Approximately half of the children with PCD require otolaryngology care, posing a major problem in this population. Early diagnosis of PCD is critical in these patients to minimise the collateral damage related to OME. The current gold standard for PCD diagnosis requires determining ciliary structure defects by transmission electron microscopy (TEM) or clearly documenting ciliary dysfunction via digital high-speed video microscopy (DHSV). Although both techniques are useful for PCD diagnosis, they have limitations and need to be supported by new methodologies, including genetic analysis of genes related to PCD. In this article, we review classical and recently associated mutations related to ciliary alterations leading to PCD, which can be useful for early diagnosis of the disease and subsequent early management of OME.

PMID: 24459089 [PubMed – in process]

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