Association between non-coding polymorphisms of HOPX gene and syncope in hypertrophic cardiomyopathy

Güleç, Çağrı; Abacı, Neslihan; Bayrak, Fatih; Kömürcü-Bayrak, Evrim; Kahveci, Gökhan; Güven, Cengiz; Erginel-Unaltuna, Nihan

doi:10.5152/akd.2014.4972

Cited by 7 publications

(2 citation statements)

References 47 publications

(45 reference statements)

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“…During HOPX-induced hypertrophy in rats, inhibition of histone deacetylase (HDACi) is critical for atrial fibrosis and arrhythmic inducibility [ 50 ]. Two variants in the HOPX gene have been shown to cause syncope, which is defined as a loss of consciousness and muscle strength in patients with hypertrophic cardiomyopathy (HCM) [ 51 ].…”

Section: Hopx Regulation Of Molecular Signaling Networkmentioning

confidence: 99%

HOPX: A Unique Homeodomain Protein in Development and Tumor Suppression

Gokulan

Yap

Paterson

2022

Cancers

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Homeobox genes are master regulators of morphogenesis and differentiation by acting at the top of genetic hierarchies and their deregulation is associated with a variety of human diseases. They usually contain a highly conserved sequence that codes for the homeodomain of the protein, a specialized motif with three α helices and an N-terminal arm that aids in DNA binding. However, one homeodomain protein, HOPX, is unique among its family members in that it lacks the capacity to bind DNA and instead functions by interacting with transcriptional regulators. HOPX plays crucial roles in organogenesis and is expressed in both embryonic and adult stem cells. Loss of HOPX expression is common in cancer, where it functions primarily as a tumor suppressor gene. In this review, we describe the function of HOPX in development and discuss its role in carcinogenesis.

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Section: Hopx Regulation Of Molecular Signaling Networkmentioning

confidence: 99%

HOPX: A Unique Homeodomain Protein in Development and Tumor Suppression

Gokulan

Yap

Paterson

2022

Cancers

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“…A single point mutation of a nucleotide may affect many regulatory steps involved in protein synthesis. From previous studies, SNPs in the 5'-UTR have been found to cause some diseases, such as the GDF5 gene associated with osteoarthritis (Mu et al, 2014) and the HOPX gene related to syncope in hypertrophic cardiomyopathy patients (Gulec et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

Genetic variant screening of MC3R and MC4R genes in early-onset obese children and their relatives among a Thai population: family-based study

et al. 2015

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ABSTRACT. MC3R (melanocortin-3 receptor) and MC4R (melanocortin-4 receptor) play important roles in energy homeostasis. Severe early-onset obesity, known as monogenic obesity when it is the consequence of a mutation in a single-gene product, may result when energy homeostasis is disrupted. The purpose of our study was to screen for variations of the MC3R and MC4R genes and observe the mode of inheritance of variations in affected families. We used polymerase chain reaction and direct sequencing to analyze the 11 early-onset obese children (probands) with their 71 family members, together with DNA from 100 healthy subjects used as controls. No novel mutations were found in the MC3R gene. Two previously described polymorphisms, rs3746619 and rs3827103, were detected in the MC3R gene. It was not associated with any obesity-related phenotypes. Three heterozygous variations of the MC4R gene were detected in 3 of 11 probands. The rs34114122 and rs61741819 variations have previously been reported, but rs182455344 was novel. Moreover, each MC4R variant was also found in a number of family members, indicating that this molecular analysis of a family-based study showed an autosomal dominant pattern. Our study indicated that MC4R variations in early-onset obese Thai children were found, and transmission of these variations in each family is in the dominant pattern. These variants could possibly contribute to a genetic influence of early-onset obesity in Thais. There is no evidence of any association between MC3R variations and obesity.

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