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World Journal of Cardiology logoLink to World Journal of Cardiology
. 2025 Jul 26;17(7):109787. doi: 10.4330/wjc.v17.i7.109787

Acute myocardial infarction with ventricular septal rupture: Clinical characteristics, prognosis factors, and treatment strategies

Jian Zu 1, Lu Cheng 2, Jing-Jing Lu 3, Hui Xu, Rong Zhang 4, Xue-Rui Ye 5, Qian Qiao 6, Li-Hong Zhang 7, Hao-Ling Zhang 8, Jing-Jing Zhang 9
PMCID: PMC12304829  PMID: 40741022

Abstract

This review comprehensively examines acute myocardial infarction with ventricular septal rupture (VSR), a rare yet lethal complication. We analyze its epidemiological, pathophysiological, clinical, and therapeutic aspects, emphasizing innovative strategies like bioabsorbable occluders and tissue engineering to reduce complications and improve prognosis. The integration of artificial intelligence and big data analytics for treatment decision-making and personalized surgical timing models is highlighted as transformative. Our analysis underscores the need for early diagnosis and tailored interventions, proposing future research directions in molecular mechanisms, multidisciplinary collaboration, and technology integration. These innovations promise to enhance VSR management and extend to other cardiovascular diseases, heralding a new era of precision and regenerative cardiovascular medicine.

Keywords: Acute myocardial infarction with ventricular septal rupture, Clinical characteristics, Prognostic factors, Surgical repair, Closure of ventricular septal defect through vascular or hybrid surgery, Mechanical cycle support

Core Tip: This study provides a comprehensive analysis of acute myocardial infarction complicated by ventricular septal rupture (AMI-VSR), focusing on its rare occurrence, clinical characteristics, diagnostic challenges, and treatment strategies. By evaluating epidemiology, pathophysiology, prognostic factors, and therapeutic options, it offers crucial insights into improving patient outcomes through timely surgical interventions and optimized management. This research highlights the importance of early diagnosis and balanced treatment to enhance long-term survival in AMI-VSR patients.

INTRODUCTION

Acute myocardial infarction (AMI) is one of the most common critical and severe conditions in cardiovascular diseases, and its complications pose a serious threat to patients. Ventricular septal rupture (VSR) is one of the most dangerous complications of AMI. Although the incidence rate is low (0.2%-2%), the related mortality rate is as high as 40%-90%[1]. VSR mostly occurs 2-8 days after AMI. Its pathological essence is the full-layer rupture of the interventricular septum caused by transmural myocardial necrosis. The acute left-to-right shunt thus produced can rapidly induce acute heart failure, cardiogenic shock (CS), and even multi - organ dysfunction[2]. It should be noted that, despite the popularization of reperfusion techniques that has led to a decrease in the incidence rate of VSR, its mortality rate remains at a high level. In terms of pathogenesis, VSR involves the complex interplay of multiple factors, including myocardial cell necrosis, inflammatory response, oxidative stress, and mechanical stress. The clinical manifestations are characterized by sudden hemodynamic deterioration, often presenting as chest pain, dyspnea, and refractory hypotension. Although early diagnosis and timely intervention are crucial for improving prognosis, the rarity of this complication and the nonspecificity of its symptoms often lead to diagnostic delays in clinical practice. At present, with the advancement of interventional techniques and surgical operations, the treatment strategies for VSR are constantly being optimized. However, how to balance early intervention with surgical risks, how to select the best treatment plan, and how to improve long-term prognosis are still the key and difficult points in clinical research. Distinguishing itself from previous studies, this review places particular emphasis on exploring three cutting-edge directions: The potential of bioabsorbable occluders to reduce long-term complications, the delayed surgical strategy supported by venoarterial extracorporeal membrane oxygenation (VA-ECMO) combined with include Intra-aortic balloon pump (IABP), and the predictive value of inflammatory markers for prognosis. This review aims to comprehensively summarize the clinical features, pathological mechanism and prognostic factors of AMI with VSR (AMI-VSR), and analyze the blank areas in the current treatment evidence, so as to provide scientific basis for clinical practice.

CLINICAL CHARACTERISTICS OF AMI-VSR

Epidemiological characteristics

AMI-VSR is a clinically rare yet highly fatal severe complication. Global data indicate an overall VSR incidence of 0.2%-2% among AMI patients[1], with significant heterogeneity across populations and regions (Table 1).

Table 1.

Epidemiological characteristics of acute myocardial infarction complicated by ventricular septal rupture before and after the implementation of emergency percutaneous coronary intervention, n (%)

Research object
Research center/country
Type of study population
AMI cases (n)
VSR incidence
Gender (male:female)
Implementation status of acute PCI
Year
Ref.
GUSTO Trial International multicenter (Europe and United States) AMI patients primarily receiving thrombolytic therapy 36303 798 (2.2) 1:1.2 Thrombolysis as the primary approach 1993 [84]
PAMI-1 and PAMI-2 Multicenter (America) AMI patients 1295 4 (0.31) - PCI 1995 [85-87]
SHOCK Research International multicenter (Europe and United States) Patients with cardiogenic shock complicated by VSR after MI 939 55 (5.86) - Thrombolysis combined with IABP, partial PCI 1999-2006 [88]
MOODY Registered Study China (multicenter) AMI 9265 52 (0.56) 0.625:1 Thrombolysis combined with IABP, partial PCI 1999-2016 [89]
- International multicenter STEMI, NSTEMI 9126362 10344 (0.11) 0.71:1 Thrombolysis combined with IABP, partial PCI 2003-2015 [9]
Huazhong Fuwai Cardiovascular Hospital China (single centre) VSR with percutaneous closure - 81 0.72:1 PCI and Percutaneous Septal Closure 2013-2020 [90]
Huazhong Fuwai Cardiovascular Hospital China (single centre) PIVSR patients - 213 0.95:1 PCI 2018-2023 [91]
CAUTION study(NCT03848429) International multicenter Post-infarction MCs - 720 1.46:1 Thrombolysis combined with IABP, partial PCI 2001-2019 [92]
Narayana Institute of Cardiac Sciences, India India (single centre) Patients diagnosed with post-AMI VSR and who underwent surgical closure of VSR by double patch technique - 77 2.67:1 Thrombolysis combined with IABP, partial PCI 2002-2022 [93]
Karachi Tabba Heart Institute, Department of Clinical Research in Cardiology Pakistan (multicenter) AMI-VSR 11428 67 (0.6) 1.68:1 PCI 2011-2020 [94]
First Affiliated Hospital of Xi'an Jiaotong University China (single centre) AMI-VSR 5395 42 (0.78) - PCI 2016-2020 [95]
Beijing Anzhen Hospital, Capital Medical University China (single centre) AMI-VSR - 180 0.94:1 PCI 2016-2023 [25]
Coronary Heart Disease Center, Fu Wai Hospital, National Center for Cardiovascular Diseases, Chinese Academy of Medical Science and Peking Union Medical College China (single centre) AMI-VSR 12354 70 (0.57) 0.89:1 Thrombolysis combined with IABP, partial PCI 2002-2010 [96]
Peking University People's Hospital Research China (single centre) STEMI 2057 16 (0.7) 1:1 11 cases of coronary angiography 1990-2004 [97]
- China (multicenter) AMI-VSR - 127 1.12:1 61.4% drug therapy, 24.4% TCC, 14.2% surgical intervention 2012-2019 [98]
Shenyang Northern Theater General Hospital China (single centre) AMI-VSR - 45 1.25:1 Surgery, IABP/ECMO 2012-2021 [99]
Cairo University Egypt (single centre) PIVSR - 32 1:1 PCI 2015-2023 [100]
Nanjing First Hospital Affiliated with Nanjing Medical University China (single centre) AMI-VSR - 50 0.63:1 PCI 2012-2021 [101]
National University of Singapore research Singapore (single centre) Analysis of Pathological Characteristics of VSR in Asian Populations - 40 1.2:1 Histopathology combined with immunohistochemistry 2010-2020 [102]
A tertiary care center in South India South India (single centre) Patients undergoing TCC - 21 2.5:1 PCI + TCC 2000-2014 [103]
Cleveland clinic United States (single centre) AMI-VSR - 38 1.375:1 PCI + Ventricular septal repair 1976-2023 [104]
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AMI-VSR: Acute myocardial infarction complicated by ventricular septal rupture; PCI: Percutaneous coronary intervention; IABP: Intra-aortic balloon pump; STEMI: ST - elevation myocardial infarction; NSTEMI: Non ST - elevation myocardial infarction; TCC: Transcatheter Closure; ECMO: Extraciroireal membrane oxygenation.

Age and sex disparities represent core epidemiological features of VSR. Patients ≥ 65 years account for over 70% of cases, correlating with severe coronary artery disease, diminished myocardial self-repair capacity, and multiple comorbidities[3]. Notably, the incidence in individuals ≥ 75 years declined significantly from 11.1% in 1988 to 4.3% in 2008[4], reflecting the positive impact of reperfusion therapy adoption. Regarding sex distribution, females exhibit significantly higher susceptibility (female proportion: 62.5% in VSR group vs 36.4% in controls, P < 0.01)[5]. This discrepancy primarily stems from atypical clinical presentations in females (e.g., fatigue (62%), nausea/vomiting (45%), back or jaw pain (28%) rather than typical chest pain), resulting in a median diagnosis delay of 7.0 hours vs 2.8 hours in males and consequently larger infarct sizes with heightened VSR risk[6,7].

Regional and healthcare disparities profoundly influence VSR burden. Developed regions (e.g., Europe/United States) maintain lower incidence (0.2%-0.3%) due to widespread reperfusion utilization[8,9], while Asian populations (e.g., Yunnan, China) experience higher rates (0.8%-1.57%)[10], attributable to healthcare accessibility limitations and reperfusion delays. Non-reperfused patients demonstrate the highest incidence (1%-3%)[11,12], underscoring timely revascularization’s critical role.

Comorbidity profiles further elucidate VSR susceptibility (Table 2). Non-modifiable risk factors such as advanced age (> 65 years, OR = 4.956) and female gender (OR = 4.263)[13] significantly influence disease incidence. Hypertension (prevalence: 60% in VSR; accelerates myocardial remodeling)[14], diabetes ((46.9% in VSR vs 27.8% in non-VSR, P < 0.05)[15], and chronic kidney disease (baseline creatinine > 138.5 μmol/L; postoperative mortality OR = 1.78)[16] are among the controllable risk factors.

Table 2.

Comparative table of clinical characteristics of acute myocardial infarction complicated by ventricular septal rupture

Clinical factors
Clinical manifestations
Diagnostic methods
Risk factors
Prevalence (%)
Treatment options
Ref.
Gender The proportion of females was significantly higher than that in the control group (62.5% vs 36.4%) Retrospective cohort analysis Female is an independent risk factor 62.5 (VSR group) Gender does not affect treatment selection, but women require closer hemodynamic monitoring [6,105]
Age Average age 66.85 years (VSR group) vs 60.79 years (control group) Analysis of clinical data Advanced age (> 65 years) significantly increases the risk - Elderly patients should be prioritized for interventional or surgical procedures [6,105]
Inflammatory markers CRP, D-dimer levels are significantly elevated Serological testing (CRP, D-dimer) Inflammatory response exacerbates myocardial necrosis - Anti-inflammatory therapy (such as glucocorticoids) may assist in stabilizing the condition [106,107]
Myocardial injury markers TnT significantly elevated Troponin test TnT levels are positively correlated with myocardial necrosis area - Early reperfusion therapy reduces peak TnT levels [108]
Hemoglobin Hb, Hct, and RBC were significantly lower than those in the control group Complete blood count test Anemia may increase the cardiac workload - Blood transfusion support to maintain tissue oxygen supply [14]
Cardiac function classification Killip classification ≥ grade III (78.1% in the deceased group vs 50% in the survival group) Killip classification assessment Deterioration of cardiac function is an independent risk factor for mortality 60 (Killip IV) IABP support therapy [25,34]
Myocardial infarction site Anterior wall myocardial infarction accounts for 75%-84.6% ECG, echocardiogram Anterior wall infarction is prone to involve the blood supply area of the interventricular septum 75-84.6 Patients with anterior wall infarction require early screening for VSR [14,109,110]
Location of ventricular septal perforation Near the cardiac apex (anterior wall infarction) vs posterior interventricular septum (inferior wall infarction) Echocardiography (ventricular septal echo dropout, left-to-right shunt) Posterior perforation carries a worse prognosis 60 near the cardiac apex Interventional closure is suitable for anterior perforations, while surgical repair is indicated for complex locations [58]
Perforation diameter Average 9.8 ± 3.9 mm, large perforation (> 15 mm) are associated with higher mortality rates Echocardiography The perforation diameter is positively correlated with the left-to-right shunt volume - Major perforations require emergency surgical intervention or occlusion [10,110]
Reperfusion therapy The proportion of reperfusion therapy was low (0% in the death group vs 50% in the survival group) Coronary angiography (IRA completely occluded) Failure to receive reperfusion therapy increases the risk of VSR - Emergency PCI or thrombolysis reduces the incidence of VSR [10]
Comorbidity Hypertension (60%); Diabetes (27.8%-46.9%) Medical history collection Hypertension and diabetes accelerate myocardial remodeling 60 (hypertension) Control blood pressure and blood sugar to reduce cardiac workload [14,110]
Hemodynamic status CS (90% mortality group vs 33.9% survival group) Hemodynamic monitoring (mean arterial pressure, heart rate) CS is an independent risk factor for 30-day mortality. (OR = 24.112) 90 (mortality group) VA-ECMO or IABP [14]
Laboratory indicators Elevated white blood cell count and lactate levels (survival group) Complete blood count, lactate test Elevated white blood cell count (OR = 1.619) is associated with mortality - Anti-infection and metabolic support therapy [58]
MELD-XI Score Patients with a score > 15 had a 3-year survival rate of 35.7% vs 85.1% for those with a score ≤ 15 MELD-XI score (Based on creatinine and bilirubin) High score indicates hepatic and renal dysfunction with poor prognosis - Patients with a score > 15 should be prioritized for palliative care [58]
Echocardiography parameters LVEF is normal (66.7% of patients), but cardiac function continues to deteriorate LVEF, LVEDD measurement LVEF is normal but mechanical complications are prone to be missed in diagnosis - Comprehensive evaluation based on clinical symptoms [14,93]
Coronary artery disease Multivessel disease (62.5%), with the left anterior descending artery being the most common infarct-related vessel Coronary angiography Multivessel disease and absence of collateral circulation increase the risk of VSR 62.5 (multivessel disease) CABG combined with VSR repair [14,110]
Time Patients with AMI to VSR time ≤ 4 days have higher mortality rates Medical history review Early perforation (≤ 4 days) presents fragile myocardial tissue and carries high surgical risks - Postpone the surgery for 3-4 weeks (if hemodynamically stable) [94]
Timing of surgical intervention Early surgery (≤ 7 days) mortality rate 43%, delayed surgery (> 4 weeks) mortality rate 65% Analysis of Surgical Records The timing of surgery is correlated with myocardial tissue stability - Hemodynamically stable patients are recommended for delayed surgery [111,112]
Interventional occlusion procedure The 30-day mortality rate after occlusion was 32%, with a 3-year survival rate of 73.8% Percutaneous interventional occlusion (umbrella occluder) Blockage failure is related to the perforation location and diameter - Applicable to patients with hemodynamic stability and suitable perforation site [58]
Conservative treatment The mortality rate of conservative treatment was 61.5% vs surgery/intervention at 14.3% Medications (diuretics, vasodilators, positive inotropic drugs) Conservative treatment is only suitable for those who cannot tolerate surgery - Short-term transitional therapy requires combination with IABP or ECMO [113]
Merged ventricular aneurysm 30% of patients are complicated by ventricular aneurysm Echocardiography or cardiac MRI Ventricular aneurysm increases the risk of cardiac rupture 30 Resection of ventricular wall aneurysm combined with VSR repair [21]
Renal insufficiency Elevated serum creatinine (death group 138.5 μmol/L vs survival group 88.0 μmol/L) Serum creatinine test Renal insufficiency is an independent risk factor for postoperative mortality (OR = 1.78) - Preoperative hemofiltration or postoperative CRRT [14,114]
Arrhythmia The incidence of ventricular fibrillation and atrial fibrillation is relatively high Electrocardiographic monitoring Arrhythmia reflects instability in myocardial electrical activity - Antiarrhythmic drugs or ICDs [115]
Thrombosis risk D-dimer levels were significantly elevated (death group 2.2 μg/mL vs survival group 1.0 μg/mL) D-dimer test Hypercoagulability increases the risk of embolism - Anticoagulation therapy (such as heparin), but the bleeding risk needs to be balanced [109,116]
Pulmonary artery systolic pressure Pulmonary arterial hypertension (> 50 mmHg) is associated with right heart failure Echocardiography (Tricuspid Regurgitation Velocity Method) Pulmonary hypertension indicates increased right heart workload - Reduce pulmonary circulation resistance (such as inhaling NO) [58,117]
Mitral regurgitation Mitral regurgitation area shows no significant correlation with mortality Echocardiography (regurgitant jet area measurement) Mitral regurgitation is mostly secondary and not an independent risk factor - After VSR repair, mitral valve function can be indirectly improved [118]
Hospitalization period The death group had a shorter hospital stay (6 days vs the survival group's 22.5 days) Medical record analysis Short-term hospitalization reflects a sharp deterioration in the condition - Short-term hospitalization reflects a sharp deterioration in the condition [6,109]
Long-term prognosis 3-year survival rate: Interventional closure 738%, surgical procedure 70% Follow-up (survival rate, cardiac function classification) Long-term mortality is often due to heart failure or reinfarction - Long-term anti-heart failure therapy postoperatively (such as ARNI, β-blockers) [6,119]
Case distribution VSR accounts for approximately 0.2%-1.57% of AMI Epidemiological statistics The incidence of VSR has decreased in the PCI era, but mortality rates remain high 0.2 - 1.57 Enhance the popularization rate of early reperfusion therapy to reduce the incidence rate [98,110]
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AMI: Acute myocardial infarction; CRP: C-reactive protein; TnT: Troponin T; Hct: Hematocrit; RBC: Red blood cell count; IABP: Intra-aortic balloon pump; ECG: Electrocardiogram; IRA: Infarct-related artery; PCI: Percutaneous coronary intervention; CS: Cardiogenic shock; VA-ECMO: Venous-arterial extracorporeal membrane oxygenation; LVEF: Left ventricular ejection fraction; LVEDD: Left ventricular end-diastolic diameter; CABG: Coronary artery bypass graft; CRRT: Continuous renal replacement therapy; ICDs: Implantable cardioverter defibrillators; NO: Nitric oxide; ARNI: Angiotensin receptor neprilysin inhibitor; VSR: Ventricular septal rupture.

Contemporary trends in the reperfusion era warrant emphasis: Despite thrombolysis reducing VSR incidence to 0.2%-0.3%[11,12], mortality remains alarmingly high (40%-90%)[1]. This review pioneers the incorporation of Asian epidemiological data, revealing the prognostic impact of healthcare resource disparities and informing optimized prevention strategies in resource-limited settings.

Pathophysiological mechanisms

The pathophysiological mechanisms of VSR mainly includes key links such as myocardial cell necrosis, cascade activation of inflammatory response, and mechanical stress injury, all of which jointly lead to the destruction of the structural integrity of the interventricular septum. Within the first 24 hours after myocardial infarction, the infarcted area is mainly characterized by coagulation necrosis with relatively little neutrophil infiltration. However, extensive intramural hematoma formation in the myocardial wall can already be observed at this time, and such hematomas can penetrate myocardial tissue and cause structural damage to the left ventricular wall. In the following days, a large number of neutrophils infiltrate the infarct area and release lysosomal enzymes, accelerating the dissolution process of necrotic myocardial tissue. It is worth noting that although thrombolytic therapy plays an important role in reducing the infarct area, it may induce hemorrhagic dissection of the left ventricular wall in specific situations, thereby increasing the risk of cardiac rupture[17](Figure 1).

Figure 1.

Figure 1

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Schematic diagram of the pathophysiological mechanism of acute myocardial infarction ventricular septal rupture. Created by Figdraw.

The size of VSR defects varies significantly, ranging from several millimeters to several centimeters. Simple VSR is characterized by the formation of relatively neat channels on both sides of the perforation site. In contrast, complex VSR is often accompanied by large area of intramural hematoma, and the perforation channel is irregular in shape and penetrates necrotic myocardial tissue[18]. The abnormal blood flow caused by VSR is mainly manifested as left - to - right shunt. This pathological change triggers a series of chain reactions: Increased volume load on the right ventricle, increased pulmonary circulation blood flow, and secondary volume load increase in the left atrium and left ventricle. As the left ventricular systolic function progressively deteriorates and forward blood flow decreases, the body compensatory increases systemic vascular resistance through vasoconstriction, which in turn exacerbates the degree of left - to - right shunt. It should be emphasized that the specific amount of shunt mainly depends on multiple factors, including the size of the interventricular septal defect, the ratio of pulmonary to systemic vascular resistance, and the functional state of the left and right ventricles. When the left ventricular function is severely impaired and systolic blood pressure drops significantly, the left - to - right shunt volume will correspondingly decrease[19].

Immunological characteristics of myocardial tissue in AMI-VSR

The intricate pathophysiological mechanisms underlying AMI-VSR are further elucidated by examining the immunological characteristics of myocardial tissue in affected patients. Table 3 presents detailed data on the anatomical locations, pathological features, immunohistochemical findings, complications, and speculated causes of death in cases of AMI-VSR. Examining the immunological signature of myocardial tissue reveals how different regions of the heart respond to infarction and subsequent rupture, offering insights into the local inflammatory processes and tissue damage. For instance, cases with ventricular septal perforation at the apical region of the left ventricle show prominent CD68 + macrophage infiltration, with high expression of IL-1β, often complicated by acute left heart failure and ventricular fibrillation. This indicates an intense local inflammatory reaction and myocardial dysfunction[20,21]. Similarly, perforations near the aortic valve in the basal region of the ventricular septum are marked by neutrophil infiltration and complement deposition (C3d ++), which are closely associated with atrioventricular conduction blockades[22,23]. These findings suggest that the inflammatory response varies with the location of the perforation and the specific affected myocardial structures. Such variations directly influence the types of complications and the ultimate cause of death. Understanding these immunological characteristics is critical for developing targeted anti - inflammatory therapies and individualized treatment strategies. Additionally, the identification of specific biomarkers and inflammatory pathways may pave the way for the development of new therapeutic approaches, such as immunomodulatory agents and tissue repair promoters. Future research should focus on validating these biomarkers in larger cohorts and exploring their potential applications in clinical practice. By integrating this detailed immunological information into clinical decision - making, we can more accurately assess the prognosis of patients with AMI-VSR and design more effective treatment plans to improve patient outcomes.

Table 3.

Cardiac pathological characteristics and immunohistochemical results

Anatomic location
Pathologic feature
Immunohistochemical result
Perforation site
Complication
Probable cause of death
Ref.
Anterior left ventricle Transmural necrosis, ventricular septal perforation (2.0 cm) CD68 + macrophages densely packed, IL-1β highly expressed Apical interventricular septum Acute left heart failure, ventricular fibrillation Cardiogenic shock [20,21]
Basal part of the ventricular septum Myocardial rupture with hematoma Neutrophil infiltration, C3d complement deposition (++) Near aortic valve at basal part Third-degree atrioventricular block Cardiac arrest [22,23]
Anterior right ventricle Necrosis extends to right ventricle, perforation slit-like CD3 + T cell infiltration, IFN-γ positive Anterior interventricular septum Right heart failure, hepatic congestion Multi - organ failure [120,121]
Lateral left ventricle Old infarct area calcified, fresh perforation (0.8 cm) CD163 + M2 - type macrophages predominant, TGF-β highly expressed Lateral edge of interventricular septum Wall thrombus, cerebral embolism Large - area cerebral infarction [122,123]
Middle of the ventricular septum Necrosis with abscess formation CD15 + neutrophils aggregated, Gram-positive bacteria detected Middle of the ventricular septum Septic shock, infective endocarditis Sepsis with DIC [23,124]
Inferior left ventricle Transmural necrosis with pericarditis CD20 + B lymphocyte infiltration, focal IL-10 expression Posterior - inferior part of interventricular septum Cardiac tamponade, cardiac rupture Acute cardiac tamponade [125,126]
Papillary muscle root Papillary muscle rupture with mitral valve prolapse CD31 + neovessel growth, VEGF highly expressed Posterior papillary muscle attachment area of interventricular septum Acute mitral regurgitation, pulmonary edema Acute pulmonary edema asphyxia [127,128]
Apical left ventricle Ventricular aneurysm formation, thrombus at perforation edge CD68 + /CD206 + M2 - type macrophage polarization Apical interventricular septum Peripheral artery embolism (mesenteric) Intestinal necrosis leading to septic shock [129,130]
Upper part of the ventricular septum Perforation with aortic valve ring tear CD4 + helper T cell infiltration, HLA-DR overexpressed Upper part of interventricular septum near aortic valve Aortic valve regurgitation, coronary artery dissection Acute circulatory collapse [131,132]
Right ventricular outflow tract Necrosis involving pulmonary valve CD8 + cytotoxic T cell infiltration, PD-L1 negative in perforation area Perforation in outflow tract of interventricular septum Pulmonary hypertension, right ventricular failure Acute right heart failure [133,134]
Posterior left ventricle Transmural necrosis extending to AV groove IgG/IgM immune complex deposition, C1q positive Posterior - basal part of interventricular septum Complete atrioventricular block Asystole syndrome [135,136]
Anterior edge of the ventricular septum Multiple small perforations (3 sites) CD66b + NETs formed Anterior 1/3 of interventricular septum DIC, micro thromboembolism Multi - organ microinfarction [135,137]
Basal left ventricle Transmural necrosis with ventricular wall rupture TNF-α/IL-6 double - positive cells diffuse Basal part of interventricular septum Mediastinal hematoma, pericardial effusion Hemorrhagic shock [120,122]
Posterior right ventricle Necrosis with fat infiltration CD34 + microvessel density increased, Ang-2 highly expressed Posterior - inferior part of interventricular septum Pulmonary embolism, right atrial enlargement Acute pulmonary embolism [138,139]
Anterior interventricular septum Ventricular aneurysm with mural thrombus CD47 highly expressed (anti-phagocytosis signal), fibrosis at perforation edge Middle of anterior interventricular septum Thrombus detachment causing renal infarction Acute renal failure [130,140]
Junction of the septum and right ventricle Granulation tissue growth in necrotic area CD45RO + memory T cell infiltration, IL-17A positive in perforation area Right ventricular face of interventricular septum Refractory ventricular tachycardia Electrical storm [141,142]
Posterolateral left ventricle Transmural necrosis involving posterior leaflet of mitral valve Mixed CD68 + macrophage and CD3 + T cell infiltration Posterior papillary muscle area of interventricular septum Acute mitral regurgitation, pulmonary edema Respiratory failure [123,125]
Apical part of the septum Perforation with left ventricular apical thrombus CD14 + monocyte aggregation, MMP - 9 overexpression in perforation area Apical interventricular septum Cerebral embolism, lower limb artery embolism Brainstem infarction [22,143]
Right ventricular septal part Necrosis extending to tricuspid valve ring CD79a + B cell infiltration, IgA deposition Right side of interventricular septum Tricuspid regurgitation, hepatic and renal failure Hepatorenal syndrome [144,145]
Anterolateral left ventricle Transmural necrosis with epicarditis CD123 + plasmacytoid dendritic cell infiltration, IFN-α positive in perforation area Anterolateral edge of interventricular septum Pericarditis, pleural effusion Cardiac tamponade [122,123]
Middle of the septum Necrotic area with eosinophilic infiltration CD117 + mast cell activation, histamine release in perforation area Middle 1/3 of interventricular septum Anaphylactic shock, bronchospasm Asphyxia [124,146]
Posterior basal left ventricle Old calcified lesion with fresh perforation CD68 + macrophages and CD20 + B cell colocalization Posterior - basal part of interventricular septum Splenic infarction, sepsis Septic cardiomyopathy [147,148]
Apical right ventricle Necrosis with fatty degeneration CD36 + foam cell aggregation, ox - LDL positive Apical part of right ventricle Pulmonary infarction, ARDS Respiratory failure with right heart failure [149,150]
Anterior part of the left ventricle interventricular septum Transmural necrosis with coronary artery fistula CD144 + endothelial injury marker, VWF highly expressed in perforation area Anterior interventricular septum near left anterior descending artery Coronary artery - ventricular fistula, myocardial steal Refractory hypotension [151,152]
Junction of the septum and left ventricle Necrosis with lymphatic dilation CD68 + macrophages engulfing hemosiderin Left ventricular face of interventricular septum Chylothorax, protein - losing enteropathy Hypoproteinemia causing multi - organ edema [153,154]
Extensive anterior left ventricle Large - area necrosis (> 40% left ventricle) CD163 + M2 macrophages predominant, IL-10 highly expressed in perforation area Anterior and middle parts of interventricular septum Cardiogenic shock, lactic acidosis Metabolic acidosis causing cardiac arrest [155,156]
Posterior upper part of the septum Perforation with chordae tendineae rupture Mixed CD68 + macrophage and CD15 + neutrophil infiltration Posterior upper part of interventricular septum near mitral valve Acute mitral valve flail, pulmonary edema ARDS [124,157]
Free wall of the right ventricle Necrosis with epicardial hemorrhage CD11b + myeloid cell infiltration, MPO positive in perforation area Free wall of right ventricle Pericardial effusion, cardiac tamponade Acute circulatory failure [158,159]
Posterolateral left ventricle Transmural necrosis involving left atrium CD68 + macrophage polarization (M1 predominant), TNF-α/IL-1β co - expression in perforation area Posterolateral edge of interventricular septum Atrial fibrillation, left atrial thrombus Cerebral embolism with brain herniation [155,160]
Whole layer of the septum Multiple perforations (5 sites) with myocardial dissolution CD4+/CD8+ T cell ratio inverted, Fas/FasL highly expressed in perforation area Anterior, middle, and posterior parts of interventricular septum Whole - heart failure, hyperkalemia Electromechanical dissociation [161,162]
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DIC: Disseminated intravascular coagulation; VEGF: Vascular endothelial growth factor; HLA-DR: Human leukocyte antigen-DR; PD-L1: Programmed death-ligand 1; AV: Atria and ventricles; NETs: Neutrophil extracellular traps; TNF-α: Tumor necrosis factor-α; IL: Interleukin; MMP-9: Matrix metalloproteinase-9; IgA: Immunoglobulin A; ox-LDL: Oxidized low-density lipoprotein; VWF: Von Willebrand factor; ARDS: Acute respiratory distress syndrome; MPO: Myeloperoxidase.

Clinical features

AMI-VSR is mainly characterized by sudden hemodynamic deterioration, with typical symptoms including: (1) Persistent or progressively worsening chest pain, often accompanied by symptoms such as cold sweats and nausea; (2) Dyspnea caused by acute left - heart failure, with severe cases presenting signs of pulmonary edema; (3) Hypotension or even cardiogenic shock due to a sudden drop in cardiac output; and (4) On physical examination, a characteristic holosystolic murmur can be heard along the left sternal border, indicating the presence of a ventricular septal defect. Female patients are more prone to atypical symptoms: Such as fatigue (62%), nausea/vomiting (45%), back or jaw pain (28%) rather than typical chest pain. These manifestations are often misdiagnosed as gastrointestinal disorders or anxiety, resulting in a median delay of 4.2 hours from symptom onset to diagnosis[24-26].

In terms of diagnostic evaluation, echocardiography remains the preferred method for confirming VSR, as it can accurately determine the anatomical location of the perforation, the size of the defect, and the direction of the shunt. Electrocardiogram often shows abnormal changes such as persistent ST - segment elevation or new - onset conduction block. Coronary angiography is mainly used to assess the degree of coronary artery disease and to provide a basis for subsequent revascularization strategies. In recent years, studies comparing the clinical application value of different diagnostic methods have found that invasive diagnostic methods such as left - ventricular angiography and right - heart catheterization can more accurately assess the imaging characteristics and hemodynamic parameters of AMI complicated with ventricular aneurysm and VSR. These are of great significance in guiding the formulation of follow-up treatment plans[27].

In terms of laboratory tests, significant elevation of myocardial injury markers such as troponins I/T (TNI, TNT), creatine kinase isoenzyme (CK-MB), and myoglobin (Myo) indicates severe myocardial injury. Elevated levels of B-type natriuretic peptide (BNP)/NT - proBNP can objectively reflect the severity of heart failure[17]. Parameters such as the oxygenation index and lactate in arterial blood gas analysis can effectively assess the state of tissue ischemia and hypoxia[28]. We comprehensively compared the clinical characteristics of AMI-VSR, as detailed in Table 2.

VSR rarely exists independently in clinical practice. Instead, it is often complicated by acute heart failure, malignant arrhythmias, and multi - organ dysfunction. These complications significantly increase the complexity of clinical treatment and the risk of patient death[29]. Research on VSR not only has direct clinical therapeutic value, but also provides an important theoretical basis for the exploration of myocardial tissue repair mechanisms and the development of cardiac critical care medicine. In terms of pathogenesis, VSR involves a complex interplay of multiple factors, including myocardial cell necrosis, inflammatory cascade reactions, oxidative stress - induced injury, and mechanical stress[30]. Breakthroughs in these basic studies have laid a solid scientific foundation for the development of new therapeutic approaches, including targeted anti - inflammatory therapy, stem cell based regenerative therapy, and myocardial tissue engineering[31]. An in-depth understanding of these pathophysiological mechanisms will help to formulate individualized treatment strategies for VSR, thus providing new treatment ideas for improving the prognosis of patients with complicated myocardial infarction (MI).

PROGNOSTIC FACTORS OF AMI-VSR

There are significant methodological limitations in clinical research on AMI-VSR, which make it difficult to objectively evaluate initial influencing factors. These limitations are mainly reflected in patient selection bias, insufficient control of variables, and limited sample size. In STEMI patients with mechanical complications and CS, age, female, obesity, existence of valvular heart disease or peripheral artery disease, history of coronary artery bypass grafting (CABG), use of percutaneous ventricular assist devices or extracorporeal membrane oxygenation support therapy, and systemic thrombolytic therapy are independent predictors of mortality increase[32]. For NSTEMI patients, aging and the use of percutaneous ventricular assist devices are associated with worse prognosis[33]. In both STEMI and Non - STEMI patients, surgical repair significantly reduces mortality in those who develop CS due to mechanical complications. In particular, percutaneous coronary intervention (PCI) also shows survival benefits in STEMI patients[9]. Despite the widespread use of catheter - based reperfusion techniques in the treatment of MI, the prognosis of patients with mechanical complications has not improved as expected over the past decade. McManus et al[34] conducted a large - scale retrospective study that included nearly 150000 MI patients from 1990 to 2007. After 18 years of follow-up, it was found that the in - hospital mortality rate (41% in 1990-1992 and 44% in 2005-2007) and 1 - year mortality rate (60% in 1990-1992 and 56% in 2005-2007) of patients with VSR did not change significantly. Multivariate analysis further confirmed that increasing age and CS are independent predictors of mortality in patients with VSR. According to data from the GRACE registry, factors such as ST - segment elevation or depression, left bundle - branch block, female sex, history of stroke, significant elevation of myocardial necrosis markers, advanced age, and tachycardia are closely related to the occurrence of ventricular dysfunction after acute coronary syndrome[35]. In patients who received low - molecular - weight heparin and beta - blocker therapy within 24 hours of MI onset, as well as in those with a history of MI, the incidence of mechanical complications is relatively low. It conducted a systematic analysis of 175 circulating biomarkers, revealing the complex interplay between inflammatory response, coagulation system, and metabolic pathways during AMI, and also discovered the potential application value of new prognostic biomarkers[36]. Biomarkers such as white blood cell count, BNP/NT - proBNP, TnI/TnT, and growth differentiation factors-15 (GDF-15) are of great value in predicting poor cardiac function recovery and heart failure development after PCI[37,38]. Among them, GDF-15, lactate levels, and BNP/NT - proBNP are particularly noteworthy. It was found that GDF-15 has a moderate correlation with several parameters, including interventricular septal thickness measured by echocardiography, highlighting its potential role as a prognostic biomarker for patients with AMI-VSR. Specifically, in male patients with AMI under 60 years old with acute kidney injury, changes in left atrial size and segmental wall motion abnormalities have unique value in predicting AMI complications. This emphasizes the importance of fully considering individual characteristics when assessing the risk of AMI complications[39]. The importance of timely identification and management of VSR after AMI for improving prognosis[40,41]. They also stressed the key significance of prognostic modeling for AMI patients in predicting clinical outcomes and guiding therapeutic decisions. A prognostic prediction model for first - time AMI patients based on the Sequential Organ Failure Assessment score[42]. By comprehensively analyzing demographic data and clinical parameters, they aimed to identify key factors that can guide clinical treatment decisions and improve patient prognosis. Multiple studies have confirmed that early surgical intervention can significantly improve patient prognosis[43]. Among them, hybrid surgery and interventional closure have better clinical outcomes than traditional open - heart surgery[44], while postoperative complications such as infection, bleeding, and renal failure significantly increase the risk of death[45-47]. And we comprehensively compared the association between the main prognostic factors of AMI-VSR and clinical outcomes through Table 4.

Table 4.

Analysis of the Association between major prognostic factors and clinical outcomes

Prognostic factors
Clinical impact
Evidence-based basis
Severity level
Management strategies
Timeframe of impact
Population specificity
Intervention efficacy (%)
Ref.
Female The 30-day mortality rate among female patients showed a significant increase (OR = 4.263) Multicenter studies indicate that female patients account for 62.5% of VSR cases and represent an independent risk factor High Close hemodynamic monitoring with priority given to surgical intervention Short-term (≤ 30 days) Female, Elderly patients The surgical survival rate has increased to 70% [7,13,163,164]
Age > 65 years old The mortality rate among elderly patients increased significantly (mean age of survival group: 57.4 years vs death group: 72.4 years) Logistic regression analysis showed that age was an independent risk factor for 30-day mortality. (OR = 4.956) High Elderly patients are recommended to delay surgery (if stable) or undergo interventional occlusion Short-term to medium-term (≤ 1 year) Elderly patients Delayed surgery mortality rate drops to 6.5% [13,165-168]
Killip Class ≥ Ⅲ The mortality rate reaches 78.1% in patients with deteriorating cardiac function (death group vs 50% survival group) Killip classification ≥ grade III is significantly associated with 30-day mortality rate. (OR = 24.112) Critical IABP or VA-ECMO support, early surgical intervention Short-term (≤ 30 days) Merge patients with cardiogenic shock IABP support increases survival rate by 20% [13,20,119,165]
Anterior Wall AMI Anterior wall infarction patients account for 75%-84.6% of VSR cases, with a higher mortality rate Anterior wall infarction is prone to involve the blood supply area of the interventricular septum, increasing the risk of perforation. (P = 0.023) High Early screening for VSR, prioritizing PCI or CABG combined with repair surgery Acute phase to short term Patients with anterior wall AMI PCI reduces mortality rate to 14.3% [13,163,169-171]
VSR Diameter > 15 mm The mortality rate of patients with large perforations (> 15mm) significantly increases The diameter of the perforation is positively correlated with the left-to-right shunt volume, and large perforations require emergency surgery Severe Emergency surgical repair or interventional closure Acute phase (≤ 7 days) Hemodynamically unstable patient The success rate of the occlusion procedure is 73.8% [13,105,169,172]
Time to VSR Onset ≤ 4 Days The 30-day mortality rate reaches 77.4% for patients who develop VSR within 4 days after AMI Early perforation (≤ 4 days) presents with fragile myocardial tissue and carries high surgical risks. (OR = 12.646) Critical Postpone surgery until 3-4 weeks later (if stable), supplemented with mechanical circulatory support Short-term (≤ 30 days) Early-stage perforation patients Delayed surgery mortality rate 65% [6,13,163]
Elevated Inflammatory Markers Elevated CRP and D-dimer levels are positively correlated with mortality (CRP 85 mg/L in the deceased group vs 27 mg/L in the survival group) Inflammatory response exacerbates myocardial necrosis, and elevated CRP is associated with mortality (P < 0.05) Moderate to High Anti-inflammatory therapy (such as glucocorticoids), infection control Short-term to medium-term Patients with concurrent infections or systemic inflammation Anti-inflammatory therapy improves prognosis by 30% [13,166,173]
Cardiogenic Shock (CS) The 30-day mortality rate for patients with combined CS reaches 90% CS is an independent risk factor (OR = 4.288), requiring VA-ECMO support Critical VA-ECMO combined with IABP for hemodynamic maintenance Acute phase (≤ 7 days) Patients with hemodynamic collapse ECMO support increases survival rate by 40% [13,21,166,174]
LVEF < 40% Patients with low LVEF showed significantly higher mortality (survivor group LVEF 45% vs deceased group 30%) Left ventricular dysfunction exacerbates shunting, leading to multiple organ failure High Positive inotropic drugs combined with mechanical support to optimize cardiac function before surgery Medium-term (≤ 1 year) Patients with chronic heart failure Postoperative survival rate 70% [13,169,175]
No ventricular aneurysm Patients without ventricular aneurysms have a higher mortality rate (OR = 12.646) Ventricular aneurysm may alleviate perforation tension, while non-aneurysmal myocardium is prone to secondary rupture Moderate Ventricular aneurysm resection combined with VSR repair surgery Long-term (> 1 year) Patients with complex anatomical structures Combined surgery survival rate 85% [163,169,176]
Elevated TnT levels TnT levels were positively correlated with mortality (3.56 ng/mL in the deceased group vs 0.31 ng/mL in the survival group) Elevated TnT indicates extensive myocardial necrosis and poor prognosis (P = 0.011) High Early reperfusion therapy reduces peak TnT levels Acute phase (≤ 72 hours) Patients with extensive myocardial infarction Reperfusion therapy reduces mortality by 50% [13,165,177,178]
Delayed surgical timing Early surgery (≤ 7 days) mortality rate 43% vs delayed surgery (> 4 weeks) 6.5% The success rate of surgery is higher after myocardial tissue edema subsides Moderate to High Hemodynamically stable patients are recommended for delayed surgery, supplemented with temporary mechanical support Mid-term (1-4 weeks) Patients with stable condition Delayed surgery survival rate 935% [179,180]
Multiple coronary artery diseases The mortality rate increased in patients with multivessel disease (62.5% vs single-vessel disease) Multiple vessel disease leads to aggravated myocardial ischemia, making repair more difficult High CABG combined with VSR repair surgery Long-term (> 1 year) Patients with complex coronary artery lesions CABG combined surgery survival rate 80% [13,166,181,182]
Anemia (Hb < 10 g/dL) Anemia increases cardiac workload and elevates mortality rates (survivor group Hb 12 g/dL vs deceased group 9 g/dL) Low Hb reduces tissue oxygen supply and accelerates the progression of heart failure Moderate Blood transfusion support to maintain Hb > 10 g/dL Short-term to medium-term Patients with chronic kidney disease or bleeding tendency Blood transfusion improves oxygen delivery with a 25% increase in survival rate [13,99,183]
Renal insufficiency Postoperative mortality rate increases in patients with renal insufficiency (OR = 1.78) Elevated creatinine levels (> 138.5 μmol/L) are associated with postoperative mortality High Preoperative hemofiltration, postoperative CRRT support Short-term to long-term Patients with chronic kidney disease CRRT support reduces mortality rate by 20% [6,13,16]
Elevated Lactate Levels A lactate level > 4 mmol/L indicates tissue hypoperfusion and is associated with significantly increased mortality Elevated lactate levels reflect systemic hypoperfusion and are associated with multiple organ failure (P < 0.001) Critical Optimize perfusion (e.g., ECMO), correct metabolic acidosis Acute phase (≤ 24 hours) Patients with shock or sepsis ECMO support increases survival rate by 35% [13,166,184,185]
Diabetes Mellitus Mortality rate increased in patients with combined diabetes (46.9% vs non-diabetic 27.8%) Diabetes accelerate myocardial remodeling and impair healing (P < 0.05) Moderate Strictly control blood glucose (target HbA1c < 7%) Long-term (> 1 year) Diabetic patients Blood sugar control reduces complication rates by 30% [13,15,186]
Lack of Reperfusion Therapy The mortality rate reaches 66.7% in patients who did not receive reperfusion therapy Reperfusion therapy reduces the incidence of VSR (50% of the survival group received PCI vs 0% in the deceased group) High Emergency PCI or thrombolysis to restore coronary blood flow Acute phase (≤ 12 hours) AMI patients without contraindications PCI reduces mortality rate to 14.3% [13,169,187,188]
Postoperative CAR ≥ 2.83 Postoperative CAR is associated with increased risk of complications (OR = 5.540) CAR predicts postoperative infections and organ failure (AUC = 0.767) Moderate Postoperative monitoring of CAR, early anti-infection and nutritional support Short-term (≤ 30 days) Postoperative patient The complication rate decreased by 40% after intervention [165,189,190]
Genetic Polymorphisms Specific genotypes (such as IL-6 variants) are associated with exacerbated inflammatory responses Preliminary studies suggest that gene polymorphisms influence the efficacy of anti-inflammatory therapy (further verification required) Low to Moderate Personalized anti-inflammatory regimen Long-term (> 1 year) Genetically susceptible population Research phase, no definitive data available yet [191,192]
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IABP: Intra-aortic balloon pump; VA-ECMO: Venous-arterial extracorporeal membrane oxygenation; CABG: Coronary artery bypass graft; PCI: Percutaneous coronary intervention; CRP: C-reactive protein; CS: Cardiogenic shock; LVEF: Left ventricular ejection fraction; TnT: Troponin T; CRRT: Continuous renal replacement therapy; CAR: C-reactive protein to albumin ratio; IL: Interleukin; Hb: Hemoglobin; AMI: Acute myocardial infarction; VSR: Ventricular septal rupture; OR: Odds ratio.

In a word, early identification, accurate diagnosis and individualized treatment for AMI-VSR patients are very important. The combined application of biomarker testing, imaging assessment techniques, and prognostic prediction models provides key evidence for decision - making. However, more research are still needed to achieve the clinical goal of improving the prognosis of AMI-VSR patients.

TREATMENT STRATEGY SLECTION OF AMI-VSR

The treatment of AMI-VSR has evolved significantly with technological advancements and a deeper understanding of the pathophysiology. Current strategies emphasize integrating cutting-edge technologies and personalized decision-making models to optimize outcomes.

Surgical repair

Surgical repair is a mainstay for AMI-VSR. Despite controversy over timing, surgical technique advancements and enhanced perioperative care have improved outcomes. Early surgery can prevent heart failure progression, while delayed surgery allows necrotic tissue stabilization. A major observational study showed that 30 - day mortality in VSR patients correlates negatively with the time from VSR occurrence to surgery. Delayed defect closure with prolonged mechanical support can stabilize patients for surgery. Cardiac surgery under IABP support or with other mechanical cycle support (MCS) is also an option[48-55].

Closure of ventricular septal defect by vascular or hybrid operation

Treatment strategies have shifted from single-modality surgery to a multidisciplinary approach. The hybrid approach, combining surgical and percutaneous techniques, has improved clinical outcomes. Percutaneous closure is valuable but has limitations like occluder displacement and residual shunt. However, bioabsorbable occluders have emerged as a promising innovation, potentially reducing long-term complications. A multicenter study showed a 20% higher 30-day survival rate with hybrid surgery compared to traditional open - heart surgery. Percutaneous closure also reduces surgical trauma and postoperative complications in high-risk patients. Sutureless patch repair technology has also shown promise. These advancements reflect continuous innovation in VSR treatment[4,56-62].

Subsidiary support scheme

Pharmacological treatment initially focuses on reducing cardiac afterload and shunt fraction. However, high mortality with sole pharmacological therapy underscores the preference for surgical repair. New drugs like Entresto have shown potential in improving symptoms and reducing readmissions in AMI and acute heart failure patients[51,63-71].

For refractory cardiogenic shock, multiple catecholamines are often needed. Short-term MCS is recommended for potentially reversible cases. Various short-term MCS types effectively reduce left-ventricular loading, preventing further myocardial injury and supporting left-ventricular functional recovery[66,72-75]. Developing new-generation assist devices with lower complication rates remains a key future direction.

Individualized treatment of complex diseases

We comprehensively compared the advantages and disadvantages of different treatment strategies in the literature, as shown in Table 5. Prognosis for AMI-VSR patients remains poor despite advanced treatments. This has prompted reflection on existing strategies and spurred innovation. Personalized treatment involves comprehensively assessing each patient’s characteristics, including laboratory tests, echocardiographic parameters, and hemodynamic monitoring[48,76,77]. To achieve precision treatment, molecular biological techniques like genomics, transcriptomics, proteomics, and metabolomics can be used for multi-dimensional analysis. Building a dedicated database of patient biological samples and clinical data helps determine the best treatment plan and validate its effectiveness in clinical trials. Multi-level analysis can overcome existing treatment limitations and develop innovative, personalized plans for AMI-VSR patients.

Table 5.

Comparison of advantages and disadvantages among different treatment strategies

Treatment method
Indications
Success rate (%)
Complications incidence (%)
Cost-effectiveness
Ref.
Percutaneous interventional closure procedure (TCC) The condition is stable, the perforation diameter is ≤ 20 mm, and the location is away from the valve structures 73.8 (3-year survival rate) 32 (Residual shunt, mechanical hemolysis) Moderate (requiring high-precision imaging equipment and consumables) [20,82,193-195]
Surgical repair (combining CABG) Perforation diameter > 20mm, multivessel disease, combined with ventricular aneurysm or valvular injury 70 (3-year survival rate) 40-52 (Postoperative infection, cardiogenic shock) Low (The surgical costs are high, requiring long-term monitoring and care) [98,114,165,169]
Medical conservative treatment (medication + IABP/ECMO) Hemodynamically extremely unstable, unable to tolerate surgery or interventional therapy 38.5 (30-day survival rate) 50-60 (multiple organ failure, hemorrhage) Low short-term costs, but high long-term expenses (requires repeated hospitalizations) [25,165,196]
Delayed intervention closure (occurring > 3 weeks after VSR) Myocardial edema subsides, hemodynamics stabilize, and perforated tissue becomes fibrotic 96.3 (30-day survival rate) 10-15 (Residual shunt, arrhythmia) High (reduces the risk of secondary surgery) [58,82,193,197]
Early intervention and occlusion (VSR occurrence ≤ 3 weeks) Emergency rescue, unable to wait for delayed surgery 62.5 (30-day survival rate) 45-50 (Perforation enlargement, occluder displacement) Moderate (urgent resource support required) [193,198,199]
VA-ECMO combined with IABP support CS, hemodynamic collapse 40 (Survival rate improvement) 25-30 (Lower limb ischemia, hemorrhage) Low (equipment and monitoring costs are high) [169,200,201]
Pharmacological treatment alone (diuretics + vasodilators) Hospice care or transitional treatment 14.3 (30-day survival rate) 60-70 (Deterioration of renal function, electrolyte imbalance) Minimum (drug cost only) [165,202,203]
Interventional occlusion combined with PCI procedure Single-vessel disease, late-onset VSR after PCI 91.4 (Surgical success rate) 20-25 (Stent thrombosis, residual shunt) Moderate (requires phased implementation) [58,194,195]
Surgical procedure combined with CABG Multivessel disease requiring revascularization, combined with complex anatomical structures 80 (Long-term survival rate) 35-40 (Postoperative infection, stroke) Low (surgical and rehabilitation costs compounded) [93,169,204]
Staged interventional therapy (occlusion first followed by PCI) Hemodynamically stable but requires revascularization 85 (1-year survival rate) 15-20 (Secondary operational risk) Moderate (phased fee accumulation) [195,203,205]
Palliative care (anti-heart failure medications) Advanced age, severe comorbidities, limited life expectancy - - Minimum (only basic medication costs) [105,119,165]
IABP standalone support Mild cardiogenic shock, transition to definitive treatment 20 (Survival rate improvement) 15-20 (Lower limb ischemia, catheter infection) Moderate (equipment rental and monitoring costs) [118,169,206]
Emergency surgical procedure (≤ 7 days) Hemodynamically unstable, unable to wait for myocardial repair 57 (30-day survival rate) 50-60 (Postoperative heart failure, infection) Low (emergency surgery costs and high risk) [83,111,165]
Delayed surgical procedure (> 4 weeks) Myocardial tissue stabilization, hemodynamic improvement 93.5 (30-day survival rate) 10-15 (Postoperative adhesions, arrhythmia) High (surgical success rate improvement) [112,173,193]
Hybrid surgery (interventional + surgical) Complex perforations (multiple holes or serpentine tracts), residual shunts requiring secondary intervention 75 (Overall success rate) 30-35 (Multi-stage complication risks) Low (high cost of multidisciplinary collaboration) [10,93]
Anticoagulation therapy (heparin/warfarin) Hypercoagulable state, embolism prevention - 20-25 (Bleeding, thrombocytopenia) Low (primarily drug costs) [82,169,202,207]
Anti-inflammatory therapy (glucocorticoids) Systemic inflammatory response, significant elevation of CRP 30 (Prognosis improvement rate) 10-15 (Risk of infection increases) Moderate (requires monitoring of infection indicators) [106,165,169,208]
Transcatheter thrombolytic therapy No PCI conditions, early reperfusion requirements 50 (Recanalization rate) 30-40 (Bleeding, allergic reactions) Low (medication costs are low, but complication treatment expenses are high) [58,169,209]
Pericardiocentesis drainage Massive pericardial effusion leading to cardiac tamponade 90 (Symptom remission rate) 5-10 (Puncture injury, infection) Moderate (requires imaging guidance and aseptic operation) [116,210]
MELD-XI Score-Guided Therapy Risk stratification in patients with hepatic and renal dysfunction - - High (optimizing resource allocation and reducing ineffective treatment) [58,82,83]
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TCC: Transcatheter Closure; CABG: Coronary artery bypass graft; IABP: Intra-aortic balloon pump; ECMO: Extraciroireal membrane oxygenation; CS: Cardiogenic shock; PCI: Percutaneous coronary intervention; VSR: Ventricular septal rupture.

Innovative treatment strategies and future directions

Recent studies have explored bioabsorbable occluders in VSR treatment[78,79]. These occluders, absorbable over time, reduce long-term complications like thrombosis and infection. Animal experiments and early clinical trials show promise, with occluders providing adequate closure and allowing tissue healing[80]. Tissue engineering using biomaterials and stem cells to engineer functional myocardial tissue is another promising area, potentially offering a more permanent VSR solution and improving prognosis[81].

Moreover, artificial intelligence (AI) and big data analytics are revolutionizing treatment decision-making. By analyzing large datasets of patient information, AI algorithms can predict optimal treatment strategies, leading to more accurate and personalized decisions. In addition, a novel individualized surgical timing selection model has been proposed[58,82,83]. This model leverages machine learning algorithms to analyze patient data, including hemodynamic parameters, inflammatory markers, and genetic information, helping determine the best surgical timing and improving long-term survival rates.

The integration of bioabsorbable occluders, tissue engineering, AI-driven decision-making, and individualized surgical timing models into clinical practice is expected to transform VSR management. Future research should further explore these innovations and refine them to enhance survival and quality of life for AMI-VSR patients.

In conclusion, these innovations not only advance VSR treatment but also have broad implications for managing other cardiovascular diseases. By establishing early diagnosis systems and optimizing treatment strategies, we can reduce mortality, improve quality of life, and provide a scientific basis for rational medical resource allocation.

Innovations in treatment strategy selection

Personalized treatment model: This model uses multidimensional data analysis to develop individualized treatment plans for patients, considering factors like hemodynamics, inflammation, and genetics. Machine learning algorithms predict optimal treatment strategies and surgical timing, improving the accuracy and personalization of treatment decisions.

Bioabsorbable occluders: These occluders can be absorbed by the body over time, reducing long-term complications such as occluder-related thrombosis and infection. They provide adequate defect closure while allowing surrounding tissue to heal and regenerate.

Tissue engineering technology: Utilizing biomaterials and stem cells to engineer functional myocardial tissue offers a potential permanent solution for VSR repair and improving cardiac function.

AI-driven decision-making: AI algorithms analyze large datasets of patient information to predict optimal treatment strategies, leading to more accurate and personalized treatment decisions.

CONCLUSION

In summary, this review comprehensively explores AMI-VSR from epidemiological, pathophysiological, clinical, and therapeutic perspectives, offering a detailed analysis of current treatment strategies and their outcomes. Our findings underscore the complexity of AMI-VSR management and highlight several innovative approaches with the potential to transform clinical practice. The integration of bioabsorbable occluders and tissue engineering technologies represents a significant advancement, potentially reducing long-term complications and improving patient prognosis. Additionally, the application of AI and big data analytics in treatment decision-making and the development of personalized surgical timing selection models based on risk-benefit assessments are expected to enhance the precision and effectiveness of clinical interventions. Looking to the future, we propose several key directions for further research. At the basic research level, there is a pressing need to further elucidate the molecular mechanisms underlying VSR pathophysiology, which could lead to the development of targeted therapeutic agents. In clinical practice, strengthening the construction of multidisciplinary heart teams and optimizing the integration of advanced technologies such as AI and imaging will be crucial for achieving early and accurate diagnosis. Furthermore, refining treatment strategies through personalized risk-benefit assessments will be essential for improving patient outcomes. These innovations not only hold the promise of advancing the diagnosis and treatment of VSR but also have the potential to be extended to other cardiovascular diseases, thereby broadening their impact. By establishing robust early diagnosis systems and continuously optimizing treatment strategies, we aim to reduce mortality rates, enhance patients' quality of life, and provide a scientific basis for the rational allocation of medical resources. The ongoing innovation in bioabsorbable materials and the refinement of AI algorithms will likely bring about a paradigm shift in managing not only VSR but also other complex cardiovascular conditions, heralding a new era of precision and regenerative cardiovascular medicine.

Footnotes

Conflict-of-interest statement: There is no conflict of interest in this study.

Provenance and peer review: Unsolicited article; Externally peer reviewed.

Peer-review model: Single blind

Specialty type: Cardiac and cardiovascular systems

Country of origin: China

Peer-review report’s classification

Scientific Quality: Grade C, Grade C

Novelty: Grade C, Grade C

Creativity or Innovation: Grade C, Grade C

Scientific Significance: Grade C, Grade C

P-Reviewer: Han JM S-Editor: Liu JH L-Editor: A P-Editor: Wang WB

Contributor Information

Jian Zu, Gansu University of Chinese Medicine, Lanzhou 730000, Gansu Province, China.

Lu Cheng, Department of Cardiovascular Medicine, Fuwai Yunnan Hospital, Chinese Academy Medical Sciences, Kunming 650000, Yunnan Province, China.

Jing-Jing Lu, School of Traditional Chinese and Western Medicine, Gansu University of Chinese Medicine, Lanzhou 730000, Gansu Province, China.

Rong Zhang, School of Traditional Chinese and Western Medicine, Gansu University of Chinese Medicine, Lanzhou 730000, Gansu Province, China.

Xue-Rui Ye, Department of Cardiovascular Medicine, Fuwai Yunnan Hospital, Chinese Academy Medical Sciences, Kunming 650000, Yunnan Province, China.

Qian Qiao, Department of Cardiovascular Medicine, Fuwai Yunnan Hospital, Chinese Academy Medical Sciences, Kunming 650000, Yunnan Province, China.

Li-Hong Zhang, Department of Cardiovascular Medicine, Fuwai Yunnan Hospital, Chinese Academy Medical Sciences, Kunming 650000, Yunnan Province, China.

Hao-Ling Zhang, Department of Biomedical Science, Advanced Medical and Dental Institute, Universiti Sains Malaysia, Pinang 13200, Malaysia.

Jing-Jing Zhang, Department of Cardiovascular Medicine, Fuwai Yunnan Hospital, Chinese Academy Medical Sciences, Kunming 650000, Yunnan Province, China. zhangjingjing1@kmmu.edu.cn.

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