Marshall S. Stanton scite author profile

Background-DNA variants appearing to predispose to drug-associated "acquired" long-QT syndrome (aLQTS) have been reported in congenital long-QT disease genes. However, the incidence of these genetic risk factors has not been systematically evaluated in a large set of patients with aLQTS. We have previously identified functionally important DNA variants in genes encoding K ϩ channel ancillary subunits in 11% of an aLQTS cohort. Methods and Results-The coding regions of the genes encoding the pore-forming channel proteins KvLQT1, HERG, and SCN5A were screened in (1) the same aLQTS cohort (nϭ92) and (2) controls, drawn from patients tolerating QT-prolonging drugs (nϭ67) and cross sections of the Middle Tennessee (nϭ71) and US populations (nϭ90). The frequency of three common nonsynonymous coding region polymorphisms was no different between aLQTS and control subjects, as follows: 24% versus 19% for H558R (SCN5A), 3% versus 3% for R34C (SCN5A), and 14% versus 14% for K897T (HERG). Missense mutations (absent in controls) were identified in 5 of 92 patients. KvLQT1 and HERG mutations (one each) reduced K ϩ currents in vitro, consistent with the idea that they augment risk for aLQTS. However, three SCN5A variants did not alter I Na , which argues that they played no role in the aLQTS phenotype. Conclusions-DNA variants in the coding regions of congenital long-QT disease genes predisposing to aLQTS can be identified in Ϸ10% to 15% of affected subjects, predominantly in genes encoding ancillary subunits. (Circulation. 2002; 105:1943-1948.)

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Atrial Arrhythmias after Cardiothoracic Surgery

Ommen

1997

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Current Clinical Issues for MRI Scanning of Pacemaker and Defibrillator Patients

Kälin

Stanton

2005

Pacing Clinical Electrophis

340

205

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Dramatic increases in both magnetic resonance imaging (MRI) usage and cardiac device-based therapy have resulted in an estimated 50-75% probability of a patient being indicated for an MRI over the lifetime of their device. Some recent studies have demonstrated "safe procedures" and "no adverse events" in the limited populations, clinical situations, and specific devices and lead orientations tested. While these investigations are useful to help ascertain the hazards for patients with cardiac devices, they do not demonstrate clear freedom from risk. All components of active implantable systems must be engineered during the design stage to provide safety in current and evolving MR environments. Device manufacturers need to secure regulatory approval to confirm their products' safety under multiple clinical and technical variables.

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