Galectin-3 as a Predictor for Left Ventricular Remodeling After Anterior Wall Myocardial Infarction Treated by Primary Percutaneous Coronary Intervention | ||||
Benha Journal of Applied Sciences | ||||
Article 10, Volume 6, Issue 5, September 2021, Page 55-62 PDF (494.91 K) | ||||
Document Type: Original Research Papers | ||||
DOI: 10.21608/bjas.2021.198231 | ||||
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Authors | ||||
A.A. Elheet1; A.M. Bendary2; S.A. Moustafa2; H. M.Kabil3 | ||||
1Mahala Cardiac Center, Specialized Medical Councils, Ministry of Health and Population, Egypt | ||||
2Cardiovascular Medicine Dept., Faculty of Medicine, Benha Univ., Benha, Egypt | ||||
3Cardiovascular Medicine Dept., Faculty of Medicine, Damietta Univ., Damietta, Egypt | ||||
Abstract | ||||
Background: This is a single center, observational prospective study that aimed primarily to study role of Galectin-3 (as a simple marker of inflammation and fibrosis) in prediction of the occurrence of LV remodeling after anterior ST-elevation myocardial infarction (STEMI) treated by primary percutaneous coronary intervention (pPCI) for Left anterior descending artery (LAD) or left main (LM) as infarct related artery. Patients and methods: The present study protocol yielded 2 groups of patients: First group, consists of patients found to have LVR with high galectin 3 levels at baseline and 6 months follow up after anterior STEMI treated with primary PCI to LAD or LM. Second group consists of patients found to have no LVR with low levels of galectin 3 levels at baseline and 6 months follow up after anterior STEMI treated with primary PCI to LAD or LM. Results: Baseline and 6 months EF were significantly higher in the no LVR (57±8 &55 ±8 respectively) group than the LVR group (44 ±7&37 ±8 respectively), P values were <0.001 for each. At 6-month ESV was significantly higher in the LVR group (94 ml) than the no LVR group (42 ml), P-value was <0.001. The median percent change was significantly higher in the LVR group (88.89 %) than the no LVR (5 %). EDV, the mean at 6 months was significantly higher in the LVR group (150 ml) than the no LVR group (94 ml), P-value was <0. 001.The median percent change was significantly higher in the LVR group (77.78%) than the no LVR (0.94%), P-value was <0.00. As regards gelactin-3, the median at baseline was significantly higher in the LVR group (21.8 ng/ml) than the no LVR group (9.6 ng/ml), P-value was <0.001 Table (8). The median percent change was significantly higher in the no LVR group (8.49%) than the LVR group (-31.4%). Conclusion: Gal-3 serum levels after pPCI were independently associated with LVR in patients with anterior STEMI and inversely related to LVEF after a STEMI. Therefore, this study opens the door for a hard question: could we use Gal-3 as part of a screening strategy to identify patients with anterior STEMI who are at higher risk of developing HF after STEMI. | ||||
Keywords | ||||
Galectin-3; Left Ventricular Remodeling; Anterior Wall Myocardial Infarction | ||||
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