Abstract
Endomyocardial biopsy (EMB) is an invasive procedure originally developed for the monitoring of heart transplant rejection. Over the year, this procedure has gained a fundamental complementary role in the diagnostic work-up of several cardiac disorders, including cardiomyopathies, myocarditis, drug-related cardiotoxicity, amyloidosis, other infiltrative and storage disorders, and cardiac tumours. Major advances in EMB equipment and techniques for histological analysis have significantly improved diagnostic accuracy of EMB. In recent years, advanced imaging modalities such as echocardiography with three-dimensional and myocardial strain analysis, cardiac magnetic resonance and bone scintigraphy have transformed the non-invasive approach to diagnosis and prognostic stratification of several cardiac diseases. Therefore, it emerges the need to re-define the current role of EMB for diagnostic work-up and management of cardiovascular diseases. The aim of this review is to summarize current knowledge on EMB in light of the most recent evidences and to discuss current indications, including challenging scenarios encountered in clinical practice.
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Introduction
Endomyocardial biopsy (EMB) is an invasive procedure developed in 1960s initially for the early diagnosis and monitoring of heart transplant (HTx) rejection [1]. Since then, this technique has become an important tool for the diagnosis and evaluation of different cardiac disorders such as cardiomyopathies, myocarditis, infiltrative and storage diseases, and cardiac tumours. EMB incremental diagnostic, prognostic and therapeutic value has led to a wide diffusion of this technique over the years in different settings. Nevertheless, a significant heterogeneity exists in EMB use in clinical practice, probably due to its low sensitivity in specific scenarios, the development of non-invasive diagnostic techniques, the non-negligible risk of major complications especially in non-experienced centres and the limited availability of skilled cardio-pathologists for the interpretation of histological findings, outside referral centres [2].
In recent years, the use of advanced imaging modalities, as echocardiography with three-dimensional (3D) and myocardial strain analysis, cardiac magnetic resonance (CMR) and positron emission tomography (PET), has revolutionized the non-invasive approach to diagnosis and prognostic stratification of several cardiac diseases, resulting in an accurate selection of cases in which EMB may carry important both diagnostic and prognostic information (Table 1). Indeed, along with a full morphological and functional cardiac assessment, CMR imaging can provide a detailed characterization of the cardiac muscle composition, although it may not be feasible in patients with specific features (i.e. arrhythmias, poor breath-holding, non-conditioned cardiac devices) [3]. A remarkable example is the possibility to reach a non-invasive diagnosis of acute myocarditis (AM), according to the Lake Louise Criteria published in 2009 [4], updated in 2018 [5]. Furthermore, another promising tool for clinical practice is the measurement of myocardial strain, which can reveal subtle systolic dysfunction in patients with clinically suspected AM or anthracycline-induced cardiomyopathy presenting with apparently normal left ventricular ejection fraction (LVEF) [6, 7]. In addition, PET with 18F-fluorodeoxyglucose (18F-FDG) uptake could help to identify the involvement of the heart in cardiac sarcoidosis (CS) and to monitor treatment response [8]. Over the years, major technical advances in EMB, tissue processing and analysis, such as molecular diagnostics, proteomics and electron microscopy, increased the accuracy of this procedure and reduced the risk of major complications.
Therefore, it emerges the need to re-define the current role of EMB for diagnostic work-up and management of cardiovascular diseases, a task recently pursued by an international “Position statement on endomyocardial biopsy” [9]. The aim of this review is to summarize current knowledge on EMB in light of the most recent evidences and discuss current indications, including challenging scenarios encountered in clinical practice.
The current role of EMB
Providing essential information on myocardial histology, immunohistochemistry and molecular structure, EMB represents the gold-standard technique to reach a definite and etiological diagnosis in different cardiac disorders, to improve patients’ stratification and guide treatment options (Table 2) [10, 11]. Emerging imaging modalities (3D echocardyography, CMR, PET, electro anatomic voltage mapping) guiding cardiac sampling and the implementation of immunohistochemistry and polymerase chain reaction (PCR) to standard histologic evaluation have enhanced EMB diagnostic accuracy [12]. However, a significant variability in EMB diagnostic yield is conferred by the specific pattern of myocardial involvement (i.e. focal vs diffuse tissue) and centre’s expertise in samples’ collection, processing, analysis and interpretation.
EMB is a cornerstone in the management of patients with unexplained acute heart failure (HF) with haemodynamic compromise or ventricular arrhythmias/conduction disorders of unknown aetiology, clinically suspected AM, CS, storage and infiltrative diseases, cardiac masses and monitoring of HTx rejection status [10, 11].
Aside diagnostic information, viral search by PCR, reverse transcription (RT)-PCR and direct sequencing analysis on cardiac specimens have also therapeutic implications, as in the evaluation of possible candidates to immunosuppressive therapy [13]. While immunosuppression lacks conclusive prognostic evidence in virus-negative lymphocytic myocarditis, it is a recognized effective treatment option for other inflammatory cardiomyopathies, such as giant cell myocarditis (GCM), eosinophilic necrotizing myocarditis (ENM) and CS, which are associated with a poor outcome [13, 14]. Finally, during COVID-19 pandemic, although rarely indicated in suspected AM related to SARS-Cov-2, EMB has been used mainly for research purposes. In this setting, histopathological finings revealed an increased macrophage and lymphocytic tissue infiltration in the heart, without evidence of viral presence within cardiomyocytes [15].
EMB: the procedural steps in the lab and potential issues
The first technique of EMB using a bioptome designed for transvascular approach (Konno-Sakakibara bioptome) was reported in the early 1960 in Japan [1]. Over the last 60 years, EMB technique has been refined and the procedure has gained worldwide acceptance (Fig. 1). However, safety remains a concern when performing EMB; indeed, although rare, major complications (including cardiac tamponade necessitating pericardiocentesis, thromboembolism, severe arrhythmias/atrioventricular block, valvular trauma) occur in about 1% of cases [16, 17]. Haemodynamically unstable patients and those with large ventricles with thin walls may be at a higher risk of cardiac perforation, which is more frequently observed with right ventricle (RV) than with left ventricle (LV) EMB (Table 3). Of note, LV EMB is associated with a higher risk of stroke or systemic embolism. Therefore, when posing indications to EMB, the risk/benefit balance should be accurately evaluated and the procedure should be performed in high-volume centres with specific expertise to minimize the risk of such complications [2].
Old generation bioptomes for endomyocardial biopsy
RV EMB is performed by jugular, femoral or brachial veins. Transradial artery access is emerging as an alternative access route for LV EMB [18, 19], non‐inferior to transfemoral artery access in terms of major complications [20] and possibly leading to fewer access-site bleedings compared to the femoral access [21]. However, LV EMB is still usually performed by femoral arteries. In LV EMB, intravenous heparin is given to reach an ACT > 200 s to reduce the risk of embolism. From femoral access, long sheath technique is predominantly used for semi-flexible bioptomes also to avoid repeated exposure of the valve leaflets to the bioptome. The long sheath is introduced in the ventricle over a pigtail catheter which advances over a 0.035 wire under fluoroscopy guidance. Then, the mid LV cavity position of the tip of the sheath is confirmed in right and left anterior oblique projection in order to avoid the apex and to be far from valvular apparatus. At this stage, performing a ventriculography (Video 1) can facilitate the positioning of the catheter and additional angiographic views can be used for specific site of sample collection. Pigtail catheter is then removed and the bioptome is advanced into the LV. The forceps should be already in the “opened” position inside the distal segment of the long sheath and have to remain open until contact with the ventricular wall. The bioptome forceps are closed when a slight resistance is sensed by the operator; ventricular beat or non-sustained ventricular tachycardia is common while the bioptome is in contact with the myocardium. The bioptome is then removed from the sheath and the sheath is aspirated and flushed to prevent air or tissue embolism. Once the patient’s hemodynamic stability has been ascertained, heparin is antagonized with protamine sulphate and the introducer removed by closure devices. The general advice about steering the bioptome holds true for both LV and RV EBM. Of note, in RV EMB, samples are usually taken from different sites of the interventricular septum (Videos 2 and 3) to reduce the risk of perforation.
A successful procedure should provide at least ≥ 5 samples for histological evaluation, immunohistochemistry and viral PCR analyses [11, 22]. The diagnostic yield of EMB may be optimized when samples from both ventricles are available [16]; however, LV EMB appears diagnostically more informative than RV EMB [17] in patients with clinically uninvolved RV. The best approach should be identified based on an accurate clinical query: LV biopsy is preferred in suspected AM with primary LV involvement and CS. While the diagnostic accuracy of EMB is high in diffuse cardiac diseases, such as CA, collection of specimens from multiple cardiac sites should be considered in focal diseases as in CS [23]. Of note, increasing the number of collected samples is paralleled by a higher risk of complications [24]. Pre-operative third-level imaging techniques as CMR and 18F-FD PET may identify the sites with myocardial fibrosis (LGE and T1 mapping), cardiac edema (T2 mapping), and inflammation where the probability of an informative EMB result is higher. Moreover, the use of intra-procedural electroanatomic mapping may detect ventricular segments with fragmented or low voltages [5] which may indicate the most diseased area for sample collection [8]. Further studies are needed to evaluate the ability of imaging techniques and electroanatomic mapping to guide EMB and improve the safety and the diagnostic yield of the procedure.
Clinical indications to EMB
Clinical indications to EMB have been based on empirical decisions and expert opinions, often heterogeneous worldwide and dynamic over time, mostly due to the invasive nature of this technique and the lack of specific clinical trials and guidelines (Table 2). Previously published international Scientific Statements [10, 11] did not result in a standardized use of EMB in clinical practice. Currently, in the latest guidelines on the diagnosis and treatment of HF from the European Society of Cardiology (ESC), EMB is indicated with a class IIa recommendation in the context of rapidly progressive HF despite standard therapy, when there is a probability of a specific diagnosis requiring specific treatments, which can be confirmed only in myocardial samples [25].
Furthermore, the recent position Statement by Seferovic et al. [9] identified with a standardized approach 9 specific clinical scenarios in which EMB should be considered to reach the final diagnosis and to guide decision-making (Table 4).
Use of EMB in different clinical settings
EMB covers a fundamental role in suspected AM presenting with cardiogenic shock or acute HF with ventricular dysfunction and/or rhythm disorders. DCM with recent onset and progressive HF, unresponsive to standard treatment, or with new-onset unexplained sustained ventricular arrhythmias as well as high-degree atrioventricular blocks is a setting where EMB is considered useful. These two latter presentations in the context of an autoimmune disorder represent a scenario in which EMB may confirm the presence of an autoimmune myocarditis (i.e. GCM, CS) or vasculitis in patients with unexplained DCM [9]. In these contexts, EMB results have a crucial role in orienting immunosuppressive treatment.
EBM may also be considered in unexplained cardiomyopathies with hypertrophic or restrictive phenotype and inconclusive non-invasive results [26]. In detail, EMB can be useful in patients with a clinical context of high suspicion for HCM phenocopies such as CA. EMB is the gold standard for the diagnosis of CA with nearly 100% sensitivity and specificity if specimens are collected from > 4 multiple sites and tested for amyloid deposits by Congo red staining [27]. In this setting, EMB or extracardiac biopsy is recommended to confirm light chain (AL) CA in patients with suggestive non-invasive findings and evidence of monoclonal proteins [26]. Conversely, a final diagnosis of transthyretin-related (ATTR) CA can be achieved noninvasively in patients with grades 2–3 cardiac uptake at bone tracers scintigraphy and absence of monoclonal proteins on serum and urine tests [28]. Finally, EMB may be considered in the work-up of patients with suspected cancer therapy cardiotoxicity, in particular mediated by immune checkpoint inhibitors (ICI), and for the characterization of cardiac masses without high embolic risk [9]. In all the aforesaid settings, EMB is expected to be highly informative towards ongoing mechanisms of cardiac damage, throughout both the ultrastructural characterization of cardiac tissue and inflammatory infiltrates, and the detection of viral presence, toxic injuries and metabolic disorders [25].
EMB use in selected controversial scenarios
It should be always considered that EMB is an invasive procedure to be used after careful consideration of risks and benefits [24]. EMB has some limitations [2] : (a) its accuracy is not 100% and inconclusive results are possible in clinical practice, (b) it is associated with a modest, but still relevant, risk of potential major procedural complications, (c) the presence of mild myocardial histological changes is not always clinically relevant and does not address a specific therapeutic approach, and (d) it requires cardiac pathologists with experience in the interpretation of histological findings. Finally, some absolute contraindications to EMB should be considered such as the presence of intracardiac thrombus, ventricular aneurysm, severe tricuspid, pulmonary or aortic stenosis and tricuspid or aortic prosthesis [9].
A careful candidate selection with a stepwise and comprehensive approach is recommended in challenging scenarios (Table 5). Of note, this approach to EMB indication is supported by the 2021 guidelines for the diagnosis and treatment of acute and chronic HF from the ESC [25].
Non-ischemic DCM and clinically suspected myocarditis
Non-ischemic DCM represents a particularly complex setting due to polymorphic clinical presentation and evolution [24]. Patients presenting with hemodynamically stable non-ischemic DCM are a challenging scenario where EMB might be essential to make the diagnosis and guide therapy [25] when no clinical improvement is seen after at least 3 months of optimal medical treatment, especially in absence of severe LV remodelling [29]. Among the several causes that may underlie this clinical presentation, AM is a reversible and treatable condition [30]. Accurate multiparametric non-invasive evaluation can strengthen the clinical suspicion. However, the value of EMB lies in the ability to orient diagnosis and immunomodulation strategies based on histopathological and immunohistochemical results, combined with the evaluation of viral presence in the heart via PCR analysis [12, 13]. In detail, histological evaluation provides key information on the presence, type and degree of inflammatory cells (i.e. lymphocytic vs non-lymphocytic myocarditis), presence of viruses, myocardial fibrosis or changes in myocardial architecture consistent with a cardiomyopathy substrate [13, 22]. In lymphocytic myocarditis, viral presence detected by PCR analysis on myocardial samples is a contraindication to immunosuppression, although PVB-19 with a low replicative activity (< 250–500 copies/μg) represents a condition where immunosuppression require further research in controlled clinical trials (Fig. 2) [13, 22].
Possible histopathological findings in cardiac diseases. A and B Lymphocytic myocarditis with intense inflammatory infiltrates in the myocardium; C and D eosinophilic myocarditis with eosinophilic cells during active degranulation; E and F cardiac sarcoidosis with inflammatory infiltrates and modest myocardial fibrosis and the typical non-caseating sarcoid granuloma; G and H cardiac amyloidosis with vascular and interstitial deposition on Congo red staining. Legend: IHC, Immunohistochemistry
Haemodynamically stable patients with normal LVEF and clinically suspected AM are another challenging scenario where EMB should be considered to reach a final diagnosis and guide therapy if persistently or relapsing increased serum troponin values, deterioration of systolic function or frequent ventricular arrhythmias are present.
CS is another challenging scenario where the patchy myocardial involvement makes it difficult to find the pathognomonic non-caseating granulomas. In case of strong clinical suspicion and consistent non-invasive tests (i.e. PET), a negative EMB result should not discourage clinicians to pursue a final diagnosis, also with a repeated EMB [13].
Hypertrophic cardiomyopathies and phenocopies
EMB might be indicated to reach a final diagnosis in patients presenting with HF and ventricular hypertrophy. Patients’ age at clinical onset is relevant as the incidence of phenocopies (i.e. CA) increases with ageing [31], while HCM, Danon disease and Anderson-Fabry disease are more frequently encountered in young adults [32]. Specific extracardiac findings such as renal insufficiency and neurological issues might be found in Anderson-Fabry disease, while bilateral carpal tunnel syndrome (CTS) [33] and macroglossia should raise the suspicion of CA [28]. Extreme ventricular thickening (i.e. > 30 mm) with significantly increased QRS voltages in very young patients might suggest the presence of Danon disease [34]. Infiltrative diseases (i.e. CA) expand the extracellular space and can present with low QRS voltages, while storage diseases (i.e. Pompe disease, PRKAG2 disease) are characterized by normal to high QRS voltages [35]. The presence of discrepancies between the degree of ventricular hypertrophy at echocardiography and the QRS voltage on surface ECG might suggest an infiltrative disease [35]. Conversely, a family history of HCM or sudden death at a young age, significant cardiac hypertrophy with an asymmetrical pattern, especially involving the interventricular septum or the apex, and the identification of a genetic mutation in sarcomeric proteins suggest the presence of HCM. CMR can provide important information to differentiate HCM from phenocopies [3], but a final diagnosis can be made only by histological analysis in specific settings.
Restrictive cardiomyopathies
EMB might be required in patients presenting with restrictive cardiomyopathy with controversial non-invasive findings to reach a final diagnosis (i.e. endomyocardial fibrosis, CA, hemochromatosis). Patients with iron overload cardiomyopathy (IOC) might present with restrictive phenotype on a background of acquired anaemia requiring multiple transfusions or development of diabetes mellitus with typical skin pigmentation. The diagnosis is supported by the presence of serum ferritin > 300 ng/mL with transferrin saturation > 55% and cardiac siderosis (cardiac T2* < 20 ms on CMR scan) [36]. However, in case of inconclusive non-invasive tests, cardiac samples analysis with Perls’ Prussian blue stain can provide histological confirmation of myocardial iron deposition [36].
Cardiac masses
Patients with incidental detection of cardiac masses require accurate differential diagnosis between tumour, vegetation, calcification and thrombus [37]. The presence of fever, increased white blood cells count and PCR serum levels, signs of organ infection (i.e. pneumonia), cardiac devices, native or prosthetic valve disease and known neoplasia increase the risk of infective or non-infective endocarditis. Fatigue, anaemia and progressive weight loss might suggest the presence of a neoplasm. Contrast CT and CMR play a key role in characterization of the cardiac mass (i.e. CMR in lipomas) and in pre-procedural planning, while scintigraphy with 99-Tc-labelled leukocytes can reveal sites of active inflammation and infection [37]. Size and location of the mass in the heart are relevant: myxomas are found predominantly in the left atrium, lipomas tend to occur in right atrium or in the left ventricle, and fibroma and rhabdomyomas are mostly located in the ventricle. Some masses might show peculiar features such as myxomas, which can cause dynamic mitral valve obstruction leading to syncope, pulmonary edema and embolic manifestations [37]. Of note, EMB, particularly LV EMB, is not indicated in case of intracardiac friable masses with high embolic potential such as left-sided tumours or typical cardiac myxomas [9]. In those cases, a patient’s tailored approach is essential and surgical removal can be preferred over EMB, according to patients’ overall conditions.
HTx rejection
EMB remains the gold standard for the diagnosis and monitoring of HTx rejection status. An International Society for Heart and Lung Transplantation (ISHLT) classification of postcardiac transplant cellular rejection was developed in 1990 and revised in 2004 [38], facilitating the standardization and management of graft rejection. However, poor inter-pathologists agreement in grading rejection has been a concern, as demonstrated by the data from the CARGO II study [39]. Standardization in diagnosis is still a challenge. Automated computational-image analysis and molecular diagnostics are promising tools to improve the precision and accuracy in the disease pathological grading and classification [10].
Another debated issue is the optimal timing and frequency of routine surveillance EMB (rsEMB) after HTx, which can be scheduled according to a protocol in asymptomatic patients and in patients with worsening clinical status (symptom triggered EMB). In recent years, novel non-invasive tests have been developed such as gene-expression profiling and donor-derived cell-free DNA for screening in stable patients [40, 41]. Nevertheless, the limited access to these tests together with a low accuracy in the early period following HTx has limited their clinical use. The reduction in rsEMB has resulted from the recognition that the occurrence of clinically relevant cardiac rejection is very uncommon in the absence of symptoms or left ventricular systolic dysfunction [42]. Thus, a revised schedule for HTx rejection surveillance has been recently proposed, suggesting three different rsEMB protocols (low-, moderate- and high-frequencies) [9].
Future perspectives and conclusion
Although a consensus exists about the clinical indications to EMB, this exam gains particular relevance (a) in acute cardiac syndromes, refractory to standard therapies, (b) when non-invasive assessment is not feasible (i.e. CMR not feasible because of frequent arrhythmias, etc..) or yields inconclusive results, (c) for surveillance indications (i.e. reject after HTx) and (d) in selected cases of chronic hemodynamically stable patients with inconclusive non-invasive tests and suspicion of inflammatory disease (i.e. persistently or relapsing increased serum troponin values, ventricular arrhythmias, development of severe LV dysfunction) or underlying cardiomyopathies (i.e. HCM “phenocopies”) (Fig. 3).
Future perspectives on endomyocardial biopsy. Legend: Ab, antibodies; AM, acute myocarditis; CMR, cardiac magnetic resonance; EMB, endomyocardial biopsy; LGE, late gadolinium enhancement; PET, positron emission tomography
Of note, EMB should be performed in centres with specific expertise in evaluating patients with cardiomyopathies and interpreting the immunohistopathological and bio-molecular histological findings. In this perspective, the organization of a “hub-spoke” network should be fully supported in the near future. This approach would allow an accurate selection of best candidates to EMB after consideration of the risk–benefit balance, avoiding taking unnecessary procedural risks. CMR findings such as LGE or increased T values/ECV, the analysis of the genetic background [43] and knowledge of the disease-specific mechanisms of cardiac injury [44] are promising fields of future investigation to refine patients selection.
Change history
04 September 2022
The original version of this paper was updated to add funding note.
References
Sakakibara S, Konno S (1962) Endomyocardial biopsy. Jpn Heart J 3:537–543
Sinagra G, Porcari A, Fabris E, Merlo M (2021) Standardizing the role of endomyocardial biopsy in current clinical practice worldwide. Eur J Heart Fail 23:1995–1998
Porcari A, De LA, Grigoratos C, Biondi F, Faganello G, Vitrella G, Nucifora G, Aquaro GD, Merlo M, Sinagra G (2022) Arrhythmic risk stratification by cardiac magnetic resonance tissue characterization: disclosing the arrhythmic substrate within the heart muscle. Heart Fail Rev 27:49–69
Friedrich MG, Sechtem U, Schulz-Menger J, Holmvang G, Alakija P, Cooper LT, White JA, Abdel-Aty H, Gutberlet M, Prasad S, Aletras A, Laissy J-P, Paterson I, Filipchuk NG, Kumar A, Pauschinger M, Liu P (2009) Cardiovascular magnetic resonance in myocarditis: a JACC white paper. J Am Coll Cardiol 53:1475–1487
Ferreira VM, Schulz-Menger J, Holmvang G, Kramer CM, Carbone I, Sechtem U, Kindermann I, Gutberlet M, Cooper LT, Liu P, Friedrich MG (2018) Cardiovascular magnetic resonance in nonischemic myocardial inflammation: expert recommendations. J Am Coll Cardiol 72:3158–3176
Fischer K, Obrist SJ, Erne SA, Stark AW, Marggraf M, Kaneko K, Guensch DP, Huber AT, Greulich S, Aghayev A, Steigner M, Blankstein R, Kwong RY, Gräni C (2020) Feature tracking myocardial strain incrementally improves prognostication in myocarditis beyond traditional CMR imaging features. JACC Cardiovasc Imaging 13:1891–1901
Porcari A, Merlo M, Crosera L, Stolfo D, Barbati G, Biondi F, Angelis G De, Paldino A, Pagnan L, Belgrano M, Cova MA, Pinamonti B, Vitrella G, Sinagra G (2020) Strain analysis reveals subtle systolic dysfunction in confirmed and suspected myocarditis with normal LVEF. A cardiac magnetic resonance study. Clin Res Cardiol 109:869–880
Tschöpe C, Ammirati E, Bozkurt B, Caforio ALP, Cooper LT, Felix SB, Hare JM, Heidecker B, Heymans S, Hübner N, Kelle S, Klingel K, Maatz H, Parwani AS, Spillmann F, Starling RC, Tsutsui H, Seferovic P, Van LS (2021) Myocarditis and inflammatory cardiomyopathy: current evidence and future directions. Nat Rev Cardiol 18:169–193
Seferović PM, Tsutsui H, McNamara DM, Ristić AD, Basso C, Bozkurt B, Cooper LTJ, Filippatos G, Ide T, Inomata T, Klingel K, Linhart A, Lyon AR, Mehra MR, Polovina M, Milinković I, Nakamura K, Anker SD, Veljić I, Ohtani T, Okumura T, Thum T, Tschöpe C, Rosano G, Coats AJS, Starling RC (2021) Heart failure association of the ESC, heart failure society of America and japanese heart failure society position statement on endomyocardial biopsy. Eur J Heart Fail 23:854–871
Leone O, Veinot JP, Angelini A, Baandrup UT, Basso C, Berry G, Bruneval P, Burke M, Butany J, Calabrese F, D’Amati G, Edwards WD, Fallon JT, Fishbein MC, Gallagher PJ, Halushka MK, McManus B, Pucci A, Rodriguez ER, Saffitz JE, Sheppard MN, Steenbergen C, Stone JR, Tan C, Thiene G, van der Wal AC, Winters GL (2012) 2011 Consensus statement on endomyocardial biopsy from the association for european cardiovascular pathology and the society for cardiovascular pathology. Cardiovasc Pathol 21:245–274
Cooper LT, Baughman KL, Feldman AM, Frustaci A, Jessup M, Kuhl U, Levine GN, Narula J, Starling RC, Towbin J, Virmani R (2007) The role of endomyocardial biopsy in the management of cardiovascular disease: a scientific statement from the american heart association, the american college of cardiology, and the european society of cardiology. Endorsed by the heart failure society o. J Am Coll Cardiol 50:1914–1931
Caforio ALP, Calabrese F, Angelini A, Tona F, Vinci A, Bottaro S, Ramondo A, Carturan E, Iliceto S, Thiene G, Daliento L (2007) A prospective study of biopsy-proven myocarditis: prognostic relevance of clinical and aetiopathogenetic features at diagnosis. Eur Heart J 28:1326–1333
Sinagra G, Porcari A, Gentile P, Artico J, Fabris E, Bussani R, Merlo M (2021) Viral presence-guided immunomodulation in lymphocytic myocarditis: an update. Eur J Heart Fail 23:211–216
Ammirati E, Cipriani M, Moro C, Raineri C, Pini D, Sormani P, Mantovani R, Varrenti M, Pedrotti P, Conca C, Mafrici A, Grosu A, Briguglia D, Guglielmetto S, Perego GB, Colombo S, Caico SI, Giannattasio C, Maestroni A, Carubelli V, Metra M, Lombardi C, Campodonico J, Agostoni P, Peretto G, Scelsi L, Turco A, Di TG, Campana C, Belloni A et al (2018) Clinical presentation and outcome in a contemporary cohort of patients with acute myocarditis. Circulation 138:1088–1099
Tavazzi G, Pellegrini C, Maurelli M, Belliato M, Sciutti F, Bottazzi A, Sepe PA, Resasco T, Camporotondo R, Bruno R, Baldanti F, Paolucci S, Pelenghi S, Iotti GA, Mojoli F, Arbustini E (2020) Myocardial localization of coronavirus in COVID-19 cardiogenic shock. Eur J Heart Fail 22:911–915
Yilmaz A, Kindermann I, Kindermann M, Mahfoud F, Ukena C, Athanasiadis A, Hill S, Mahrholdt H, Voehringer M, Schieber M, Klingel K, Kandolf R, Böhm M, Sechtem U (2010) Comparative evaluation of left and right ventricular endomyocardial biopsy. Circulation 122:900–909
Chimenti C, Frustaci A (2013) Contribution and risks of left ventricular endomyocardial biopsy in patients with cardiomyopathies: a retrospective study over a 28-year period. Circulation 128:1531–1541
Schulz E, Jabs A, Gori T, Hink U, Sotiriou E, Tschöpe C, Schultheiss H-P, Münzel T, Wenzel P (2015) Feasibility and safety of left ventricular endomyocardial biopsy via transradial access: technique and initial experience. Catheter Cardiovasc Interv Off J Soc Card Angiogr Interv 86:761–765
Schäufele TG, Spittler R, Karagianni A, Ong P, Klingel K, Kandolf R, Mahrholdt H, Sechtem U (2015) Transradial left ventricular endomyocardial biopsy: assessment of safety and efficacy. Clin Res Cardiol 104:773–781
Göbel S, Schwuchow-Thonke S, Jansen T, Karbach S, Emrich T, Gori T, Knies F, Schulz E, Münzel T, Keller K, Wenzel P (2020) Safety of transradial and transfemoral left ventricular compared with transfemoral right ventricular endomyocardial biopsy. ESC Hear Fail 7:4015–4023
Choudhury T, Lurz P, Schäufele TG, Menezes MN, Lavi S, Tzemos N, Hartung P, Stiermaier T, Makino K, Bertrand OF, Gilchrist IC, Mamas MA, Bagur R (2019) Radial versus femoral approach for left ventricular endomyocardial biopsy. EuroIntervention J Eur Collab with Work Gr Interv Cardiol Eur Soc Cardiol 15:678–684
Caforio ALP, Pankuweit S, Arbustini E, Basso C, Gimeno-Blanes J, Felix SB, Fu M, Helio T, Heymans S, Jahns R, Klingel K, Linhart A, Maisch B, McKenna W, Mogensen J, Pinto YM, Ristic A, Schultheiss H-P, Seggewiss H, Tavazzi L, Thiene G, Yilmaz A, Charron P, Elliott PM (2013) Current state of knowledge on aetiology, diagnosis, management, and therapy of myocarditis: a position statement of the european society of cardiology working group on myocardial and pericardial diseases. Eur Heart J 34(2636–2648):2648a–2648d
Bennett MK, Gilotra NA, Harrington C, Rao S, Dunn JM, Freitag TB, Halushka MK, Russell SD (2013) Evaluation of the role of endomyocardial biopsy in 851 patients with unexplained heart failure from 2000–2009. Circ Hear Fail 6:676–684
Sinagra G, Anzini M, Pereira NL, Bussani R, Finocchiaro G, Bartunek J, Merlo M (2016) Myocarditis in clinical practice. Mayo Clin Proc 91:1256–1266
McDonagh TA, Metra M, Adamo M, Gardner RS, Baumbach A, Böhm M, Burri H, Butler J, Čelutkienė J, Chioncel O, Cleland JGF, Coats AJS, Crespo-Leiro MG, Farmakis D, Gilard M, Heymans S, Hoes AW, Jaarsma T, Jankowska EA, Lainscak M, Lam CSP, Lyon AR, McMurray JJV, Mebazaa A, Mindham R, Muneretto C, Francesco Piepoli M, Price S, Rosano GMC, Ruschitzka F et al (2021) 2021 ESC Guidelines for the diagnosis and treatment of acute and chronic heart failure. Eur Heart J 42:3599–3726
Garcia-Pavia P, Rapezzi C, Adler Y, Arad M, Basso C, Brucato A, Burazor I, Caforio ALP, Damy T, Eriksson U, Fontana M, Gillmore JD, Gonzalez-Lopez E, Grogan M, Heymans S, Imazio M, Kindermann I, Kristen AV, Maurer MS, Merlini G, Pantazis A, Pankuweit S, Rigopoulos AG, Linhart A (2021) Diagnosis and treatment of cardiac amyloidosis: a position statement of the ESC working group on myocardial and pericardial diseases. Eur Heart J 42:1554–1568
Ruberg FL, Grogan M, Hanna M, Kelly JW, Maurer MS (2019) Transthyretin amyloid cardiomyopathy. J Am Coll Cardiol 73:2872–2891
Porcari A, Merlo M, Rapezzi C, Sinagra G (2020) Transthyretin amyloid cardiomyopathy: an uncharted territory awaiting discovery. Eur J Intern Med 82:7–15
Pollack A, Kontorovich AR, Fuster V, Dec GW (2015) Viral myocarditis–diagnosis, treatment options, and current controversies. Nat Rev Cardiol 12:670–680
Porcari A, De AG, Romani S, Paldino A, Artico J, Cannatà A, Gentile P, Pinamonti B, Merlo M, Sinagra G (2019) Current diagnostic strategies for dilated cardiomyopathy: a comparison of imaging techniques. Expert Rev Cardiovasc Ther 17:53–63
Porcari A, Bussani R, Merlo M, Varrà GG, Pagura L, Rozze D, Sinagra G (2021) Incidence and characterization of concealed cardiac amyloidosis among unselected elderly patients undergoing post-mortem examination. Front Cardiovasc Med 8:749523
Limongelli G, Monda E, Tramonte S, Gragnano F, Masarone D, Frisso G, Esposito A, Gravino R, Ammendola E, Salerno G, Rubino M, Caiazza M, Russo M, Calabrò P, Elliott PM, Pacileo G (2020) Prevalence and clinical significance of red flags in patients with hypertrophic cardiomyopathy. Int J Cardiol 299:186–191
Porcari A, Pagura L, Longo F, Sfriso E, Barbati G, Murena L, Longo E, Ramella V, Arnež ZM, Rapezzi C, Merlo M, Sinagra G (2022) Prognostic significance of unexplained left ventricular hypertrophy in patients undergoing carpal tunnel surgery. ESC Hear Fail 9:751–760
Arad M, Maron BJ, Gorham JM, Johnson WHJ, Saul JP, Perez-Atayde AR, Spirito P, Wright GB, Kanter RJ, Seidman CE, Seidman JG (2005) Glycogen storage diseases presenting as hypertrophic cardiomyopathy. N Engl J Med 352:362–372
Vergaro G, Aimo A, Barison A, Genovesi D, Buda G, Passino C, Emdin M (2020) Keys to early diagnosis of cardiac amyloidosis: red flags from clinical, laboratory and imaging findings. Eur J Prev Cardiol 27:1806–1815
Kremastinos DT, Farmakis D (2011) Iron overload cardiomyopathy in clinical practice. Circulation 124:2253–2263
Bussani R, Castrichini M, Restivo L, Fabris E, Porcari A, Ferro F, Pivetta A, Korcova R, Cappelletto C, Manca P, Nuzzi V, Bessi R, Pagura L, Massa L, Sinagra G (2020) Cardiac tumors: diagnosis, prognosis, and treatment. Curr Cardiol Rep 22:169
Stewart S, Winters GL, Fishbein MC, Tazelaar HD, Kobashigawa J, Abrams J, Andersen CB, Angelini A, Berry GJ, Burke MM, Demetris AJ, Hammond E, Itescu S, Marboe CC, McManus B, Reed EF, Reinsmoen NL, Rodriguez ER, Rose AG, Rose M, Suciu-Focia N, Zeevi A, Billingham ME (2005) Revision of the 1990 working formulation for the standardization of nomenclature in the diagnosis of heart rejection. J Hear lung Transplant Off Publ Int Soc Hear Transplant 24:1710–1720
Crespo-Leiro MG, Zuckermann A, Bara C, Mohacsi P, Schulz U, Boyle A, Ross HJ, Parameshwar J, Zakliczyński M, Fiocchi R, Stypmann J, Hoefer D, Lehmkuhl H, Deng MC, Leprince P, Berry G, Marboe CC, Stewart S, Tazelaar HD, Baron HM, Coleman I-C, Vanhaecke J (2012) Concordance among pathologists in the second cardiac allograft rejection gene expression observational study (CARGO II). Transplantation 94:1172–1177
Pham MX, Teuteberg JJ, Kfoury AG, Starling RC, Deng MC, Cappola TP, Kao A, Anderson AS, Cotts WG, Ewald GA, Baran DA, Bogaev RC, Elashoff B, Baron H, Yee J, Valantine HA (2010) Gene-expression profiling for rejection surveillance after cardiac transplantation. N Engl J Med 362:1890–1900
Purewal S, Moayedi Y, Runeckles K, Fan C, Gordon J, Henricksen EJ, Oro G, Shudo Y, Khush KK, Teuteberg J (2020) Are two tests better than one? Combining donor derived cell-free DNA and gene expression profiling for non-invasive surveillance after heart transplantation. J Hear Lung Transplant 39:S71
Howlett JG, Crespo-Leiro MG (2021) The international endomyocardial biopsy position paper: a basis for integration into modern clinical practice. J Card Fail S1071–9164(21)00261-X
Baggio C, Gagno G, Porcari A, Paldino A, Artico J, Castrichini M, Dal Ferro M, Bussani R, Merlo M (2021) Myocarditis: which role for genetics? Curr Cardiol Rep 23:58
Blanco-Domínguez R, Sánchez-Díaz R, la Fuente H, de, Jiménez-Borreguero LJ, Matesanz-Marín A, Relaño M, Jiménez-Alejandre R, Linillos-Pradillo B, Tsilingiri K, Martín-Mariscal ML, Alonso-Herranz L, Moreno G, Martín-Asenjo R, García-Guimaraes MM, Bruno KA, Dauden E, González-Álvaro I, Villar-Guimerans LM, Martínez-León A, Salvador-Garicano AM, Michelhaugh SA, Ibrahim NE, Januzzi JL, Kottwitz J, Iliceto S, Plebani M, Basso C, Baritussio A, Seguso M, Marcolongo R et al (2021) A novel circulating microRNA for the detection of acute myocarditis. N Engl J Med 384:2014–2027
Lurz P, Luecke C, Eitel I, Föhrenbach F, Frank C, Grothoff M, de Waha S, Rommel K-P, Lurz JA, Klingel K, Kandolf R, Schuler G, Thiele H, Gutberlet M (2016) Comprehensive cardiac magnetic resonance imaging in patients with suspected myocarditis: the MyoRacer-Trial. J Am Coll Cardiol 67:1800–1811
Zhang J, Li Y, Xu Q, Xu B, Wang H (2018) Cardiac magnetic resonance imaging for diagnosis of cardiac sarcoidosis: a meta-analysis. In: Leroyer C (ed) Can Respir J, vol 2018. p 7457369
Bravo PE, Singh A, Di CMF, Blankstein R (2019) Advanced cardiovascular imaging for the evaluation of cardiac sarcoidosis. J Nucl Cardiol Off Publ Am Soc Nucl Cardiol 26:188–199
Birnie DH, Nery PB, Ha AC, Beanlands RSB (2016) Cardiac sarcoidosis. J Am Coll Cardiol 68:411–421
Brownrigg J, Lorenzini M, Lumley M, Elliott P (2019) Diagnostic performance of imaging investigations in detecting and differentiating cardiac amyloidosis: a systematic review and meta-analysis. ESC Hear Fail 6:1041–1051
Fontana M, Chung R, Hawkins PN, Moon JC (2015) Cardiovascular magnetic resonance for amyloidosis. Heart Fail Rev 20:133–144
Rosengren S, Skibsted Clemmensen T, Tolbod L, Granstam S-O, Eiskjær H, Wikström G, Vedin O, Kero T, Lubberink M, Harms HJ, Flachskampf FA, Baron T, Carlson K, Mikkelsen F, Antoni G, Frost Andersen N, Hvitfeldt Poulsen S, Sörensen J (2020) Diagnostic accuracy of [(11)C]PIB positron emission tomography for detection of cardiac amyloidosis. JACC Cardiovasc Imaging 13:1337–1347
Jessup M, Abraham WT, Casey DE, Feldman AM, Francis GS, Ganiats TG, Konstam MA, Mancini DM, Rahko PS, Silver MA, Stevenson LW, Yancy CW (2009) Focused update: ACCF/AHA guidelines for the diagnosis and management of heart failure in adults: a report of the American College of Cardiology Foundation/American Heart Association Task Force on Practice Guidelines: developed in collaboration with the International Society for Heart and Lung Transplantation. Circulation 119(14):1977–2016. https://doi.org/10.1161/CIRCULATIONAHA.109.192064. Epub 2009 Mar 26. PMID: 19324967
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Made substantial contributions to conception and structure of the review: Aldostefano Porcari, Chiara Baggio, Gianfranco Sinagra; editing and drafting: Aldostefano Porcari, Chiara Baggio, Enrico Fabris; revision, supervision, and final approval: Marco Merlo, Rossana Bussani, Andrea Perkan, Gianfranco Sinagra.
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Supplementary file1 Video 1 Ventriculography in right anterior oblique projection showing the long sheath over a pigtail catheter in the mid-left ventricular cavity position (AVI 1948 KB)
Supplementary file2 Video 2 Ventriculography in right anterior oblique projection showing the long sheath over a pigtail catheter which is positioned in the right ventricle, in the interventricular septum (AVI 2830 KB)
Supplementary file3 Video 3 Ventriculography in left anterior oblique projection showing the long sheath over a pigtail catheter which is positioned in the right ventricle, in the interventricular septum (AVI 2350 KB)
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Porcari, A., Baggio, C., Fabris, E. et al. Endomyocardial biopsy in the clinical context: current indications and challenging scenarios. Heart Fail Rev 28, 123–135 (2023). https://doi.org/10.1007/s10741-022-10247-5
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DOI: https://doi.org/10.1007/s10741-022-10247-5