Cristina Panico scite author profile

Background: Inflammation is a key component of cardiac disease, with macrophages and T lymphocytes mediating essential roles in the progression to heart failure. Nonetheless, little insight exists on other immune subsets involved in the cardiotoxic response. Methods: Here, we used single-cell RNA sequencing to map the cardiac immune composition in the standard murine nonischemic, pressure-overload heart failure model. By focusing our analysis on CD45 + cells, we obtained a higher resolution identification of the immune cell subsets in the heart, at early and late stages of disease and in controls. We then integrated our findings using multiparameter flow cytometry, immunohistochemistry, and tissue clarification immunofluorescence in mouse and human. Results: We found that most major immune cell subpopulations, including macrophages, B cells, T cells and regulatory T cells, dendritic cells, Natural Killer cells, neutrophils, and mast cells are present in both healthy and diseased hearts. Most cell subsets are found within the myocardium, whereas mast cells are found also in the epicardium. Upon induction of pressure overload, immune activation occurs across the entire range of immune cell types. Activation led to upregulation of key subset-specific molecules, such as oncostatin M in proinflammatory macrophages and PD-1 in regulatory T cells, that may help explain clinical findings such as the refractivity of patients with heart failure to anti–tumor necrosis factor therapy and cardiac toxicity during anti–PD-1 cancer immunotherapy, respectively. Conclusions: Despite the absence of infectious agents or an autoimmune trigger, induction of disease leads to immune activation that involves far more cell types than previously thought, including neutrophils, B cells, Natural Killer cells, and mast cells. This opens up the field of cardioimmunology to further investigation by using toolkits that have already been developed to study the aforementioned immune subsets. The subset-specific molecules that mediate their activation may thus become useful targets for the diagnostics or therapy of heart failure.

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Early detection of elevated cardiac biomarkers to optimise risk stratification in patients with COVID-19

Stefanini

Chiarito

Ferrante

et al. 2020

Heart

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ObjectiveRisk stratification is crucial to optimise treatment strategies in patients with COVID-19. We aimed to evaluate the impact on mortality of an early assessment of cardiac biomarkers in patients with COVID-19.MethodsHumanitas Clinical and Research Hospital (Rozzano-Milan, Lombardy, Italy) is a tertiary centre that has been converted to the management of COVID-19. Patients with confirmed COVID-19 were entered in a dedicated database for cohort observational analyses. Outcomes were stratified according to elevated levels (ie, above the upper level of normal) of high-sensitivity cardiac troponin I (hs-TnI), B-type natriuretic peptide (BNP) or both measured within 24 hours after hospital admission. The primary outcome was all-cause mortality.ResultsA total of 397 consecutive patients with COVID-19 were included up to 1 April 2020. At the time of hospital admission, 208 patients (52.4%) had normal values for cardiac biomarkers, 90 (22.7%) had elevated both hs-TnI and BNP, 59 (14.9%) had elevated only BNP and 40 (10.1%) had elevated only hs-TnI. The rate of mortality was higher in patients with elevated hs-TnI (22.5%, OR 4.35, 95% CI 1.72 to 11.04), BNP (33.9%, OR 7.37, 95% CI 3.53 to 16.75) or both (55.6%, OR 18.75, 95% CI 9.32 to 37.71) as compared with those without elevated cardiac biomarkers (6.25%). A multivariate analysis identified concomitant elevation of both hs-TnI and BNP as a strong independent predictor of all-cause mortality (OR 3.24, 95% CI 1.06 to 9.93).ConclusionsAn early detection of elevated hs-TnI and BNP predicts mortality in patients with COVID-19. Cardiac biomarkers should be systematically assessed in patients with COVID-19 at the time of hospital admission in order to optimise risk stratification.

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Continuation versus discontinuation of ACE inhibitors or angiotensin II receptor blockers in COVID-19: effects on blood pressure control and mortality

Cannata

Chiarito

Reimers

et al. 2020

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Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), responsible for the coronavirus disease 2019 (COVID-19), employs angiotensin-converting enzyme 2 (ACE2) for cellular entry. 1 The effects of ACE inhibitors (ACEis) and angiotensin receptor blockers (ARBs) on ACE2 expression and activity are unclear. Concerns arose about possible interactions between renin-angiotensin-aldosterone system (RAAS) inhibitors and SARS-CoV-2 infectivity and virulence. 2 An opposite hypothesis 1 suggests that SARS-CoV-2 down-regulates ACE2 expression after cell entry, increasing RAAS activation and angiotensin II levels. Early evidence suggested that angiotensin II serum levels are increased in COVID-19 patients, and directly correlated with viral load and lung injury, 3 while large observational studies did not detect harmful associations between ACEi/ARB therapy and the likelihood of COVID-19 or in-hospital mortality. 4,5 However, no evidence is available on the effect on mortality of ACEi/ARB continuation or discontinuation in hospitalized COVID-19 patients. Consecutive patients with confirmed COVID-19 admitted to Humanitas Clinical and Research Hospital (Rozzano-Milan, Lombardy, Italy) up to 1 April 2020 were enrolled in a prospective registry, which complies with the Declaration of Helsinki and was approved by our institutional Ethics Committee. Discontinuation was defined as ACEi/ARB interruption at the time of hospital admission in patients known to be taking ACEis/ARBs at home. Patients suspending ACEis/ARBs during hospitalization for clinical reasons (e.g. hypotension, worsening renal function, etc.) were considered as the ACEi/ARB continuation group. The primary outcome was mortality. The odds ratio (OR) and 95% confidence interval (CI) were calculated with binary logistic regression. Clinical follow-up was censored at the

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Cristina Panico

Single-Cell Sequencing of Mouse Heart Immune Infiltrate in Pressure Overload–Driven Heart Failure Reveals Extent of Immune Activation

Early detection of elevated cardiac biomarkers to optimise risk stratification in patients with COVID-19

Continuation versus discontinuation of ACE inhibitors or angiotensin II receptor blockers in COVID-19: effects on blood pressure control and mortality

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