Modified chordal sparing mitral valve replacement as effective technique for both stenotic and insufficient mitral valves.

BACKGROUND: Chordal apparatus preservation is important for preserving left ventricular (LV) function in the long-term perspective. We present results of originally modified chordal-sparing mitral valve replacement (MVR) successfully used in patients with mitral stenosis and mitral insufficiency. METHODS: The modified surgical method involves preserving only four strut chords with portions of the mitral valve leaflets, which are later fixed to the fibrous ring. The rest of the leaflets and marginal chords are removed. RESULTS: Starting from 1998, 484 modified universal chordal-sparing MVR were performed including 270 (55.79%) in patients with rheumatic mitral stenosis and 214 (44.21%) in patients with mitral valve insufficiency. Overall, 116 patients underwent isolated MVR, and 368 patients underwent MRV with concomitant surgical procedures. The overall in-hospital mortality was 2.5% (12 patients). Long-term efficiency was assessed in patients discharged after isolated MVR (114 patients), average follow-up period was 3.1±0.6 years. Preservation of strut chords ensured normalization of intraventricular anatomy and prevented LV dilatation; the LV Sphericity Index is maintained at 0.44-0.63. Heart failure functional class (NYHA) was improved in all patients. Non-fatal prosthesis-related complications were observed in 11 patients (9.65%). Three patients (2.63%) died due to extracardiac causes. CONCLUSIONS: The proposed modification of the strut chordal-sparing mitral valve replacement technique allows preserving functionally complete annulo-papillary apparatus, regardless of the nature of valvular dysfunction, and provides parallel movement to the mechanical prosthesis. This modified surgical technique is safe and effective and eliminates the risk of jamming of the prosthesis disk and left ventricular outflow tract obstruction.

Atrial appendage transcriptional profile in patients with atrial fibrillation with structural heart diseases.

During the last few years DNA microarray studies of gene expression changes in human atrial tissues from patients with and without atrial fibrillation (AF) have been performed. For this purpose, tissue samples are usually collected from AF patients undergoing open heart surgery. These investigations have limitations associated with the unavoidable heterogeneity of compared groups which is due to the presence of various structural changes accompanying different sets of underlying heart diseases in both groups. It is thus reasonable to compare the atrial tissue samples from AF patients with those from individuals without signs of cardiovascular disease. To address this, we selected the atrial tissue samples from 12 AF patients (who underwent open heart surgery) and compared them with control atrial tissue samples from 10 individuals with no signs of cardiovascular diseases (those who died due to street accident). cDNA microarray method and reverse transcription-polymerase chain reaction (RT-PCR) analysis were used to identify genes which can discriminate between control and pathologically altered atrial tissues. Thirty-nine genes were found to be differentially expressed in pathologically altered tissues samples independently of the type of the underlying structural heart disease. These genes are involved in signal transduction, gene transcription regulation, cell proliferation, and apoptosis. The greatest alterations were observed for NOR1, DEC1, MSF, and Bcl2A1 genes (5 to 28-fold decrease, P < 0.05). Additional studies are needed to determine the specific role of each selected gene in pathophysiological changes leading to AF.