LM is typically characterized by patchy infiltration of an array of mononuclear cells, with a majority of T lymphocytes and some macrophages (1, 18). Other immune related cells, such as neutrophils, eosinophils, and plasma cells may be present, but are not the prominent cell type (1). LM is further characterized into acute and chronic LM based on immunopathology (18). In acute LM, there is minimal fibrosis, however chronic LM is characterized by fibrosis given the persistent inflammation (18). Of note, in chronic LM, the lymphocytic infiltration still remains in addition to fibrosis (18). Currently, the timing of transition from acute to chronic LM is not well described and varies at the individual level (18). Thus far, studies have found LM is due to viral (coxsackie B virus and adenovirus being the most common) and autoimmune etiologies (1, 18). The exact pathophysiology of LM is not completely understood; however, current proposed mechanisms have been attributed to an inflammatory response following viral infection (19).

It has been identified that viral infection causes activation of toll-like receptors which leads to an innate immune response and upregulation of immune mediators (19). As the inflammatory cascade continues, the acquired immune system is eventually generated, leading to T cell activation (19). In order for T cell activation to occur, viral antigen must be presented via binding between the T cell receptor and major histocompatibility complex (19, 20). If the viral antigen peptide shares similarity to myosin, or other myocardial antigens, the T cells may attack the myocardium, which is known as molecular mimicry (19, 20). Through damage from T cells, the myocardium exposes more antigens and provokes further activation of toll-like receptors, perpetuating the immune response (19). This continued inflammatory response engenders B cell activation and production of cardiac autoantibodies, leading to further myocardial inflammation and damage (19). Studies have found that this pathologic immune response is regulated by T helper 17 (Th17) cells and regulatory T cells (19). Th17 cells lead to a proinflammatory state while regulatory T cells lead to an immunosuppressive state and are thus responsible for increasing the threshold of immune cells in recognizing self-antigens (19). Demonstrating this effect, research has shown that humans diagnosed with myocarditis have higher ratios of Th17 to regulatory T cells in peripheral blood, leading to proinflammatory cytokines and the recruitment of inflammatory cells to the myocardium (19). Also, in animal models, injection with regulatory T cells has been shown to decrease inflammation in viral myocarditis (19). Despite the implications of various pathways, a coherent immune-pathological mechanistic understanding of LM is lacking.

GCM is another histological subtype with a more severe clinical course and worse prognosis (1). The average age at diagnosis is 40 and approximately 20% of patients have an autoimmune condition (19). Histology of GCM is comprised of myocyte necrosis with T lymphocytes and multinucleated giant cell derived from macrophages (1, 21). Eosinophils and plasma cells may be found, but to a much smaller degree (1). The pathophysiology of GCM is not fully understood, but current evidence suggests an autoimmune etiology (22). The initial support of an autoimmune etiology for GCM came from basic science research where mice were injected with either membranous proteins or cardiac myosin (22). In this study, only the mice injected with cardiac myosin developed myocarditis with histology showing myocardial necrosis and giant cells (22). Thus, cardiac myosin was able to elicit an autoimmune-mediated myocarditis, with histology consistent with GCM (22). Further insight into the pathogenesis of GCM was offered with gene expression analysis, which has helped to characterize the specific immune response involved in GCM (23). In a study comparing gene expression of GCM vs. normal heart tissue samples, the authors found a large number of genes T cell activation genes upregulated in GCM samples (23). More specifically T helper type 1 (Th1) cells, were involved in precipitating the immune response in GCM (23). The predominantly T cell response in GCM is different from LM, where autoimmune damage in the latter occurred in part through B cells and cardiac autoantibodies (19).

To date, the exact mechanism of the development of myocarditis from ICI therapy is not understood (24, 34). However, novel research has focused on better elucidating the mechanisms of ICI-mediated myocarditis (17). Wei et al. provided insight on distinct cellular mechanisms of anti-CTLA-4 and anti-PD-1 on human melanoma and murine tumor models (17). The authors showed that anti-PD-1 therapies resulted in expansion of exhausted-like tumor infiltrating CD8+ T cells (17). This is in line with other studies which have also shown that dynamic expansion of CD8+ T cells takes place with PD-1 inhibition (35, 36). Conversely, anti-CTLA-4 therapies result in expansion of Inducible T cell CO-Stimulator Th1-like CD4 effector as well as exhausted-like CD8+ T cells (17). The expansion of Inducible T cell CO-Stimulator CD4+ T cells has been seen with CTLA-4 inhibition in various tumor subtypes, also confirming the preclinical findings of Wei et al. (17, 37–39). These results illustrate how anti-CTLA-4 and anti-PD-1 therapies results in unique cellular mechanisms (17).

Preclinical research has shown that CTLA-4 and PD-1 play a key role in peripheral immune tolerance, and disruption leads to activation T lymphocytes targeting cardiac antigens (24). Murine studies have shown that antibodies against CTLA-4 or CTLA-4 deficient murine models both result in the clinical picture of myocarditis (40–42). Similarly, murine models deficient in PD-1 and PD-L1 lead to myocarditis and dilated cardiomyopathy as well (43–45). In fact, one study investigating PD-1 knockout mice found myocarditis in 96% of the murine models (18). Another study delivered cardiac troponin antibodies to murine models deficient in PD-1, leading to a dilated cardiomyopathy, further highlighting the immunoregulatory significance of PD-1 and PD-L1 (46). This is of grave concern as T cells that escape negative selection, and may have reactivity to myocardial tissue, are now at a lower threshold for activation, leading to myocardial infiltration (18, 24).

In addition to murine models, there have been clinical studies examining immune profiles of patients with ICI-mediated myocarditis. Reuben et al. described a case of a patient with metastatic melanoma treated with ipilimumab who developed steroid refractory GCM (16). Immune analysis of post-mortem cardiac tissue by immunohistochemistry, T cell receptor sequencing, and gene expression profiling were conducted (16). Autopsy demonstrated a myocardial infiltrate composed of lymphocytes, multinucleated giant cells, and some eosinophils (16). The myocardium was cultured and negative for any infectious etiology. Immunohistochemical staining revealed predominantly CD4+ T cells in the heart (16). Forkhead box protein P3 (FoxP3) staining was used to identify regulatory T cells and CD45RO was used to identify antigen-experienced T cells (16). FoxP3 and CD45RO quantification showed few FoxP3 regulatory T cells in the heart, liver and lung metastasis with CD45RO expression predominant in the heart (16). These results demonstrate that CD4+ T cells were predominant in GCM with a concomitant increase expression of CD45RO+ cells (16). Thus, ipilimumab resulted in CD4+ T cell infiltration into the myocardium, resulting in the development of GCM (16).

Conversely, Johnson et al. described two cases of patients with melanoma treated with combination of ipilimumab and nivolumab who developed fatal LM (15). Both patients had immune infiltration affecting only the cardiac and skeletal muscle cells (15). Postmortem evaluation of these two patients revealed myocardium infiltrates with both CD4+ and CD8+ T cells (Figure 2) (15). Similarly, Laubli et al. discussed a case of patient with melanoma who was treated with pembrolizumab resulting in myocarditis (26). Infectious workup was negative and myocardial biopsy showed lymphocytic infiltration with predominantly CD8+ T cells (26). Thus, PD-1 inhibitor alone or in combination with CTLA-4 inhibitor mediates LM primarily comprised of CD8+ T cells; with immune profiling distinct from GCM patients (15, 26).

The above preclinical and clinical studies highlight that CTLA-4 inhibition may cause development of GCM with predominantly CD4 infiltration while PD-1 inhibition preferentially results in the development of LM with predominantly CD8 infiltration. Hence, different ICI combinations precipitate distinct forms of myocarditis with a unique pattern of immune infiltration, a mechanism which may not necessarily translate into non-ICI myocarditis. This differential T cell infiltrative response to CTLA-4 inhibition PD-1 inhibition could be in part due to cytokine activation (47). Chemokines help with recruitment and T cell trafficking, and thus dictate the immune profiles of inflammatory processes (47). C-X-C Motif Chemokine Receptor 3 (CXCR3) is involved in several pathways, including mitogen-activated protein (MAP) kinases and phosphoinositide 3-kinase (PI3K)/ protein kinase B (Akt), leading to activation, differentiation, and recruitment of CD4+ T cells (48, 49). CXCR3 appears to favor recruitment of CD4+ T cells compared to CD8+ T cells (50). Additionally, increased expression of CXCR3 and its chemokine ligands have been found in GCM from CTLA-4 inhibition (16). Conversely, C-C chemokine receptor type 5 (CCR5) has been shown to recruit CD8+ T cells in response to chemokine ligand 3 (CCL3) and chemokine ligand 4 (CCL4), a mechanism that has also been found in other cardiovascular conditions (51, 52).

Similar recruitment has been demonstrated in Chagas disease, which is caused by Trypanosoma cruzi (52). Histologically, the non-ischemic cardiomyopathy in Chagas disease is characterized by a predominantly CD8+ T cell infiltrate (19, 52). In a murine study of Chagas disease, CCR5 and its chemokine ligands aided in T cell migration to cardiac tissue (52). Another example highlighting the importance of CCR5 in CD8+ T cell recruitment is Kawasaki disease, which is a fatal vasculitis in children that can lead to coronary artery aneurysms (53, 54). Although the exact mechanism of Kawasaki disease is not clear, histology is consistent with a predominantly CD8+ T cell infiltrate (54). Further, genetic haplotypes that result in loss of CCR5 expression have been shown to be inversely related to Kawasaki disease incidence (53). These findings further illustrate the role of CCR5 in CD8+ T cell recruitment (53). Thus, CD4+ versus CD8+ T cell infiltrate could be partially explained by differential chemokine response, specifically CXCR3 versus CCR5 in development of GCM or LM, respectively.

In addition to chemokine recruitment, studies have found the immunoproteasome to lead to CD4+ T cell recruitment (55). In a study by Bockstahler et al., murine models of autoimmune myocarditis were treated with an immunoproteasome inhibitor (55). Here, the immunoproteasome was found to increase cytokine production, which led to a decrease in T regulatory cells and differentiation of CD4+ T cells to Th1 and Th17 cells (55). The authors found that blocking the immunoproteasome led to a significant reduction in the autoimmune response and subsequent myocarditis (55). Thus, given the predominantly CD4+ T cell response, the immunoproteasome may play a key role in the development of GCM and myocarditis caused by ICIs directed at CTLA-4.

While the above pre-clinical and clinical data demonstrate the complex interplay between ICI, chemokine signaling, and distinct immune myocardial infiltrates, the molecular mechanism behind injury to cardiomyocytes is thought to be due to a shared antigen (34). As mentioned above, Johnson et al. discussed two cases of melanoma treated with ICI who developed fatal myocarditis (15). Interestingly, the affected tissues were cardiac muscle, skeletal muscle, and tumor, all with T cell infiltrates that had similar T cell receptor homology (15). Additionally, histology of the tumor samples from the two patients demonstrated desmin and troponin, which are antigens found in muscle, further illustrating the possibility of a shared antigen leading to ICI mediated myocarditis (15, 34). Recent case reports have shown that anti-striated muscle antibody might be a key factor as the elevation of this antibody and subsequent decrease with intravenous immunoglobulin (IVIG) can result in improvement in clinical outcomes (12).

With the expanding use of ICIs, data on the clinical features of ICI mediated myocarditis continues to expand (56). Mahmood et al. conducted a retrospective case-control study comparing 35 cases of myocarditis due to various ICIs to 105 control patients who received ICIs, but did not develop myocarditis, from 2013 to 2017 (56). Data from this study showed that the average time from initiation of ICI to myocarditis presentation was 34 days, 94% of cases had troponin elevation, 89% of cases had an abnormal electrocardiogram, 51% of cases had a normal ejection fraction, and 46% of cases had major adverse cardiac events (56). Interestingly, of the 46% of cases that developed major adverse cardiac events, 38% had a normal left ventricular ejection fraction (56). Compared to non-ICI mediated myocarditis cases, data from this study suggest that a higher percentage ICI mediated myocarditis cases develop a more severe course, and of those that develop a fulminant course, a higher percentage have a normal ejection fraction (56–58).

Also of growing interest is the association of specific ICI therapies to myocarditis prevalence and outcomes. Studies have shown that combination therapies lead to higher rates of myocarditis, as well as worse outcomes (59). For example, one study showed that nivolumab (PD-1 inhibitor) and ipilimumab (CTLA-4 inhibitor) had almost a 5 times greater incidence of myocarditis compared to single agent nivolumab (59). In another study, Moslehi et al. examined 101 cases of ICI mediated myocarditis, and mortality rates were significantly higher among individuals who received combination ICI therapy versus monotherapy (67 vs. 36%, respectively) (60). Further, Chen et al. conducted a retrospective study using FDA Adverse Event Reporting System and found a stronger association of PD-1 inhibitors and myocarditis compared to CTLA-4 and PD-L1 inhibitors (61). As more data becomes available, we will have a better understanding on the prevalence and outcomes of myocarditis with specific ICI therapy.