Facteurs diagnostiques et pronostiques dans l'insuffisance cardiaque aiguë

Heart failure (HF) is highly prevalent disease, and prevalence increases with age. HF is generally discovered on presentation of an acute episode of decompensation (or insufficiency). Acute decompensated heart failure (ADHF) is very frequent in elderly subjects and is difficult to diagnose when the patient is admitted with acute dyspnoea. The advent of plasma biomarkers, such as BNP or NT-proBNP represents a major advancement in the diagnostic of ADHF. ADHF leads to high rates of re-admission and mortality. The objectives of this doctoral thesis were: (1) to describe the epidemiology of ADHF in France in a one-day observational study of admissions for ADHF in 170 French hospitals; (2) to evaluate the prognostic and diagnostic value of natriuretic peptides (NPs) in ADHF; (3) to describe the extent of post-transcriptional modifications in these NPs in ADHF; and (4) to search for new biomarkers.The comparison of the prognostic and diagnostic properties of NPs showed that the 4 commercially available NPs (namely BNP, NT-proBNP, proBNP and MR-proANP) overall have very similar prognostic and diagnostic abilities. However, proBNP and BNP seem to be more useful for diagnosis, while MR-proANP appears to be better for the association with 5-year mortality.Amongthe post-transcriptional modifications of BNP, we studied the impact of glycosylation of pro¬BNP. Threonin 71 0-glycosylation prevents cleavage of proBNP into BNP and NT-proBNP, resulting in the release of proBNP from the cell without being cleaved. Conversely, non-glycosylated proBNP is cleaved into BNP and NT-proBNP by corin or furin. We showed that non-glycosylation of proBNP and activation of furin are two important mechanisms in the acceleration of production of NPs during ADHF. We also showed that production of NT-proBNP was more closely linked to the rate of glycosylation of proBNP than to the production of BNP. Thus, our results strongly suggest that NT-proBNP should be used in future studies exploring the concept of "biomarker-guided therapy" in ADHF.To investigate new biomarkers, we explored plasma concentrations of 5 microRNAs (miR-l/-21/-23/-126/-423-5p), in patients with acute dyspnoea. None of these microRNAs were shown to have any diagnostic value. Conversely, miR-423-5p appears to be a prognostic marker for re-admission at 1 year. Secondly, we investigated the consequences of cardiac congestion on the liver. The hepatic markers studied were alkaline phosphatise and transaminases. Markers of cholestasis were associated with hepatic congestive while markers of cellular necrosis (transaminases) were related to arterial hypertension and low cardiac output. An increase in transaminases was associated with various criteria of excess mortality in the short termL'insuffisance cardiaque (IC) est une maladie dont la prévalence est élevée, cette prévalence augmente avec l'âge. La découverte de la maladie se fait le plus souvent lors d'un épisode de décompensation (ou insuffisance) cardiaque aiguë (ICA). L'ICA est très fréquente chez les sujets âgés et est caractérisée par des difficultés diagnostiques quand le patient est admis avec une dyspnée aiguë. L'apport de biomarqueurs plasmatiques tels que le BNP ou le NT-proBNP a été majeur pour le diagnostic de l'ICA. La décompensation cardiaque aiguë est suivie d'un taux de réhospitalisations et d'une mortalité très élevés. Les objectifs de la thèse était 1- de préciser l'épidémiologie de l'ICA en France lors d'un observatoire d'une journée des hospitalisations pour ICA dans 170 hôpitaux français (OFICA), 2- d'identifier la puissance diagnostiques et pronostiques des peptides natriurétiques lors de l'ICA, 3-de définir l'importance des modifications post-transcriptionnelles de ces PNs lors de l'ICA, 4- de rechercher de nouveaux biomarqueurs.La comparaison des propriétés diagnostiques et pronostiques des peptides natriurétiques révèle que les 4 peptides natriurétiques commercialement accessibles (BNP, NT-proBNP, proBNP et MR-proANP) ont des qualités diagnostiques et pronostiques globalement très similaires. Néanmoins, proBNP et BNP semblent meilleurs pour le diagnostic tandis que MR-proANP apparaît meilleur pour son association avec la mortalité à 5 ans.Parmi les modifications post-transcriptionnelles du BNP, nous avons étudié l'impact de la glycosylation du pro-BNP. La O glycosylation en 71 inactive proBNP, qui est libéré hors de la cellule sans action préalable des enzymes de « cleavage » la corine ou la furine. En revanche, le proBNP non-glycosylé est scindé en BNP et NT-proBNP par la corine ou la furine. Nous avons pu montrer que la non-glycosylation du proBNP et l'activation de la furine étaient deux mécanismes très importants d'accélération de la production de peptides natriurétiques lors de l'ICA. On a pu également montrer que la production du NT-proBNP était beaucoup plus liée au niveau glycosylation du proBNP que ne l'est la production de BNP. Ainsi, nos résultats suggèrent fortement d'utiliser le NT-proBNP pour toute étude future souhaitant explorer le concept de « biomarker-guided therapy » dans l'ICA.Pour la recherche de nouveaux biomarqueurs, nous avons exploré 1-la concentration plasmatique de 5 microRNAs (miR-l/-21/-23/-126/-423-5p), chez des patients avec dyspnée aiguë. Aucun de ces miR n'a de valeur diagnostique, en revanche, le miR-423-5p apparaît être un marqueur pronostique de réhospitalisation à un an ; 2-les conséquences de la congestion cardiaque sur le foie. Les marqueurs hépatiques étudiés étaient la phosphatase alcaline et les transaminases : les marqueurs de la cholestase étaient associés à une congestion hépatique tandis que ceux de la nécrose cellulaires (transaminases) étaient liés à l'hypotension artérielle et au bas débit cardiaque. L'augmentation des transaminases a été associée à divers critères dont une surmortalité à court term

025 Benefit of Drug Eluting Stents over Bare Metal Stents after Rotational Atherectomy. A propensity score adjusted comparison in revascularization, mortality and MACE

RationaleRotational atherectomy makes possible to attempt small and calcified arteries while Drug Eluting Stents (DES) properties may reduce the restenosis process, rendering this combination attractive in selected cases. We compared 1year clinical outcome after rotational atherectomy following by either DES or Bare Metal Stents (BMS) implantation.MethodsSingle centre registry including all consecutive cases of rotational atherectomy use. Clinical follow-up was obtained in all patients. Propensity score for being treated with a DES was calculated using 18 clinical, angiographic and procedural variables. Comparison was adjusted on 4 strata of the propensity score.ResultsBetween 2002 and 2008, 223 patients were treated: 114 with BMS and 110 with DES. Most of the patients with BMS between 2002 and 2004 and later with DES. No significant difference was observed in clinical characteristics between groups: age 70 years, reference diameter 2.40±0.60mm, lesion length 10±9mm. Two cases of coronary perforation occurred, 7 lesion failure, and 12 transcient no-reflow. The use of GP2b3a inhibitors was similar in both groups, but, compared with BMS, patients in the DES group had longer duration of combination of aspirin and Clopidogrel. At one year, significantly lower rates of vessel revascularisation (2% vs 12%, p=0.005), of all cause mortality (5% vs 14%, p=0.05) and of MACE (10% vs 22%, p=0.02) were observed in the DES than in the BMS group. Adjustment on the strata of the propensity score did not change significantly these results (figure).ConclusionsDespite propensity score adjusted, this comparison has limitations. After rotational atherectomy we observed clear benefit for DES implantation over BMS on vessel revascularisation, mortality and MACE rates

Liver function abnormalities, clinical profile, and outcome in acute decompensated heart failure

AIMS: The aim of this study was to assess the prevalence of abnormal liver function tests (LFTs) and the associated clinical profile and outcome(s) in acute decompensated heart failure (ADHF) patients. Alteration in LFTs is a recognized feature of ADHF, but prevalence and outcomes data from a broad contemporary cohort of ADHF are scarce and the mechanism(s) of ADHF-induced cholestasis is unknown. METHODS AND RESULTS: We conducted a post hoc analysis of SURVIVE, a large clinical trial including ADHF patients treated with levosimendan or dobutamine. All LFTs were available in 1134 patients at baseline. Abnormal LFTs were seen in 46% of ADHF patients: isolated abnormal alkaline phosphatase (AP) was noted in 11%, isolated abnormal transaminases in 26%, and a combination of abnormal AP and transaminases in 9%. Abnormal AP was associated with marked signs of systemic congestion and elevated right-sided filling pressure. Abnormal AP had no relationship with 31-day mortality but was associated with worse 180-day mortality (23.5 vs. 34.9%, P = 0.001 vs. patients with normal AP). Abnormal transaminases were associated with clinical signs of hypoperfusion and with greater 31-day and 180-day mortality compared with normal transaminase profiles (17.6 vs. 8.4% and 31.6 vs. 22.4%, respectively; both P < 0.001). There was no additive value of abnormal AP plus abnormal transaminase on a long-term outcome. CONCLUSION: Abnormal LFTs were present in about a half of patients presenting with ADHF treated with inotropes. Abnormal AP and abnormal transaminases were associated with specific clinical, biological, and prognostic features, including a short-term overmortality with increased transaminases but not with biological signs of cholestasis, in ADHF patient

Evaluation of the effect of sodium–glucose co‐transporter 2 inhibition with empagliflozin on morbidity and mortality of patients with chronic heart failure and a reduced ejection fraction: rationale for and design of the EMPEROR‐Reduced trial

Drugs that inhibit the sodium–glucose co‐transporter 2 (SGLT2) have been shown to reduce the risk of hospitalizations for heart failure in patients with type 2 diabetes. In populations that largely did not have heart failure at the time of enrolment, empagliflozin, canagliflozin and dapagliflozin decreased the risk of serious new‐onset heart failure events by ≈30%. In addition, in the EMPA‐REG OUTCOME trial, empagliflozin reduced the risk of both pump failure and sudden deaths, the two most common modes of death among patients with heart failure. In none of the three trials could the benefits of SGLT2 inhibitors on heart failure be explained by the actions of these drugs as diuretics or anti‐hyperglycaemic agents. These observations raise the possibility that SGLT2 inhibitors could reduce morbidity and mortality in patients with established heart failure, including those without diabetes. The EMPEROR‐Reduced trial is enrolling ≈3600 patients with heart failure and a reduced left ventricular ejection fraction (≤ 40%), half of whom are expected not to have diabetes. Patients are being randomized to placebo or empagliflozin 10 mg daily, which is added to all appropriate treatment with inhibitors of the renin–angiotensin system and neprilysin, beta‐blockers and mineralocorticoid receptor antagonists. The primary endpoint is the time‐to‐first event analysis of the combined risk of cardiovascular death and hospitalization for heart failure, but the trial will also evaluate the effects of empagliflozin on renal function, cardiovascular death, all‐cause mortality, and recurrent hospitalization events. By adjusting eligibility based on natriuretic peptide levels to the baseline ejection fraction, the trial will preferentially enrol high‐risk patients. A large proportion of the participants is expected to have an ejection fraction &lt; 30%, and the estimated annual event rate is expected to be at least 15%. The EMPEROR‐Reduced trial is well‐positioned to determine if the addition of empagliflozin can add meaningfully to current approaches that have established benefits in the treatment of chronic heart failure with left ventricular systolic dysfunction

Baseline characteristics of patients with heart failure with preserved ejection fraction in the EMPEROR-Preserved trial.

AIMS: EMPEROR-Preserved is an ongoing trial evaluating the effect of empagliflozin in patients with heart failure with preserved ejection fraction (HFpEF). This report describes the baseline characteristics of the EMPEROR-Preserved cohort and compares them with patients enrolled in prior HFpEF trials. METHODS AND RESULTS: EMPEROR-Preserved is a phase III randomized, international, double-blind, parallel-group, placebo-controlled trial in which 5988 symptomatic HFpEF patients [left ventricular ejection fraction (LVEF) >40%] with and without type 2 diabetes mellitus (T2DM) have been enrolled. Patients were required to have elevated N-terminal pro B-type natriuretic peptide (NT-proBNP) concentrations (i.e. >300?pg/mL in patients without and >900?pg/mL in patients with atrial fibrillation) along with evidence of structural changes in the heart or documented history of heart failure hospitalization. Among patients enrolled from various regions (45% Europe, 11% Asia, 25% Latin America, 12% North America), the mean age was 72?±?9?years, 45% were women. Almost all patients had New York Heart Association class II or III symptoms (99.6%), and 23% had prior heart failure hospitalization within 12?months. Thirty-three percent of the patients had baseline LVEF of 41-50%. The mean LVEF (54?±?9%) was slightly lower while the median NT-proBNP [974 (499-1731) pg/mL] was higher compared with previous HFpEF trials. Presence of comorbidities such as diabetes (49%) and chronic kidney disease (50%) were common. The majority of the patients were on angiotensin-converting enzyme inhibitors/angiotensin receptor blockers/angiotensin receptor-neprilysin inhibitors (80%) and beta-blockers (86%), and 37% of patients were on mineralocorticoid receptor antagonists. CONCLUSION: When compared with prior trials in HFpEF, the EMPEROR-Preserved cohort has a somewhat higher burden of comorbidities, lower LVEF, higher median NT-proBNP and greater use of mineralocorticoid receptor antagonists at baseline. Results of the EMPEROR-Preserved trial will be available in 2021

Pronostic and daignostic factors in acute heart failure

L'insuffisance cardiaque (IC) est une maladie dont la prévalence est élevée, cette prévalence augmente avec l'âge. La découverte de la maladie se fait le plus souvent lors d'un épisode de décompensation (ou insuffisance) cardiaque aiguë (ICA). L'ICA est très fréquente chez les sujets âgés et est caractérisée par des difficultés diagnostiques quand le patient est admis avec une dyspnée aiguë. L'apport de biomarqueurs plasmatiques tels que le BNP ou le NT-proBNP a été majeur pour le diagnostic de l'ICA. La décompensation cardiaque aiguë est suivie d'un taux de réhospitalisations et d'une mortalité très élevés. Les objectifs de la thèse était 1- de préciser l'épidémiologie de l'ICA en France lors d'un observatoire d'une journée des hospitalisations pour ICA dans 170 hôpitaux français (OFICA), 2- d'identifier la puissance diagnostiques et pronostiques des peptides natriurétiques lors de l'ICA, 3-de définir l'importance des modifications post-transcriptionnelles de ces PNs lors de l'ICA, 4- de rechercher de nouveaux biomarqueurs.La comparaison des propriétés diagnostiques et pronostiques des peptides natriurétiques révèle que les 4 peptides natriurétiques commercialement accessibles (BNP, NT-proBNP, proBNP et MR-proANP) ont des qualités diagnostiques et pronostiques globalement très similaires. Néanmoins, proBNP et BNP semblent meilleurs pour le diagnostic tandis que MR-proANP apparaît meilleur pour son association avec la mortalité à 5 ans.Parmi les modifications post-transcriptionnelles du BNP, nous avons étudié l'impact de la glycosylation du pro-BNP. La O glycosylation en 71 inactive proBNP, qui est libéré hors de la cellule sans action préalable des enzymes de « cleavage » la corine ou la furine. En revanche, le proBNP non-glycosylé est scindé en BNP et NT-proBNP par la corine ou la furine. Nous avons pu montrer que la non-glycosylation du proBNP et l'activation de la furine étaient deux mécanismes très importants d'accélération de la production de peptides natriurétiques lors de l'ICA. On a pu également montrer que la production du NT-proBNP était beaucoup plus liée au niveau glycosylation du proBNP que ne l'est la production de BNP. Ainsi, nos résultats suggèrent fortement d'utiliser le NT-proBNP pour toute étude future souhaitant explorer le concept de « biomarker-guided therapy » dans l'ICA.Pour la recherche de nouveaux biomarqueurs, nous avons exploré 1-la concentration plasmatique de 5 microRNAs (miR-l/-21/-23/-126/-423-5p), chez des patients avec dyspnée aiguë. Aucun de ces miR n'a de valeur diagnostique, en revanche, le miR-423-5p apparaît être un marqueur pronostique de réhospitalisation à un an ; 2-les conséquences de la congestion cardiaque sur le foie. Les marqueurs hépatiques étudiés étaient la phosphatase alcaline et les transaminases : les marqueurs de la cholestase étaient associés à une congestion hépatique tandis que ceux de la nécrose cellulaires (transaminases) étaient liés à l'hypotension artérielle et au bas débit cardiaque. L'augmentation des transaminases a été associée à divers critères dont une surmortalité à court termeHeart failure (HF) is highly prevalent disease, and prevalence increases with age. HF is generally discovered on presentation of an acute episode of decompensation (or insufficiency). Acute decompensated heart failure (ADHF) is very frequent in elderly subjects and is difficult to diagnose when the patient is admitted with acute dyspnoea. The advent of plasma biomarkers, such as BNP or NT-proBNP represents a major advancement in the diagnostic of ADHF. ADHF leads to high rates of re-admission and mortality. The objectives of this doctoral thesis were: (1) to describe the epidemiology of ADHF in France in a one-day observational study of admissions for ADHF in 170 French hospitals; (2) to evaluate the prognostic and diagnostic value of natriuretic peptides (NPs) in ADHF; (3) to describe the extent of post-transcriptional modifications in these NPs in ADHF; and (4) to search for new biomarkers.The comparison of the prognostic and diagnostic properties of NPs showed that the 4 commercially available NPs (namely BNP, NT-proBNP, proBNP and MR-proANP) overall have very similar prognostic and diagnostic abilities. However, proBNP and BNP seem to be more useful for diagnosis, while MR-proANP appears to be better for the association with 5-year mortality.Amongthe post-transcriptional modifications of BNP, we studied the impact of glycosylation of pro¬BNP. Threonin 71 0-glycosylation prevents cleavage of proBNP into BNP and NT-proBNP, resulting in the release of proBNP from the cell without being cleaved. Conversely, non-glycosylated proBNP is cleaved into BNP and NT-proBNP by corin or furin. We showed that non-glycosylation of proBNP and activation of furin are two important mechanisms in the acceleration of production of NPs during ADHF. We also showed that production of NT-proBNP was more closely linked to the rate of glycosylation of proBNP than to the production of BNP. Thus, our results strongly suggest that NT-proBNP should be used in future studies exploring the concept of "biomarker-guided therapy" in ADHF.To investigate new biomarkers, we explored plasma concentrations of 5 microRNAs (miR-l/-21/-23/-126/-423-5p), in patients with acute dyspnoea. None of these microRNAs were shown to have any diagnostic value. Conversely, miR-423-5p appears to be a prognostic marker for re-admission at 1 year. Secondly, we investigated the consequences of cardiac congestion on the liver. The hepatic markers studied were alkaline phosphatise and transaminases. Markers of cholestasis were associated with hepatic congestive while markers of cellular necrosis (transaminases) were related to arterial hypertension and low cardiac output. An increase in transaminases was associated with various criteria of excess mortality in the short ter

Pronostic and daignostic factors in acute heart failure

L'insuffisance cardiaque (IC) est une maladie dont la prévalence est élevée, cette prévalence augmente avec l'âge. La découverte de la maladie se fait le plus souvent lors d'un épisode de décompensation (ou insuffisance) cardiaque aiguë (ICA). L'ICA est très fréquente chez les sujets âgés et est caractérisée par des difficultés diagnostiques quand le patient est admis avec une dyspnée aiguë. L'apport de biomarqueurs plasmatiques tels que le BNP ou le NT-proBNP a été majeur pour le diagnostic de l'ICA. La décompensation cardiaque aiguë est suivie d'un taux de réhospitalisations et d'une mortalité très élevés. Les objectifs de la thèse était 1- de préciser l'épidémiologie de l'ICA en France lors d'un observatoire d'une journée des hospitalisations pour ICA dans 170 hôpitaux français (OFICA), 2- d'identifier la puissance diagnostiques et pronostiques des peptides natriurétiques lors de l'ICA, 3-de définir l'importance des modifications post-transcriptionnelles de ces PNs lors de l'ICA, 4- de rechercher de nouveaux biomarqueurs.La comparaison des propriétés diagnostiques et pronostiques des peptides natriurétiques révèle que les 4 peptides natriurétiques commercialement accessibles (BNP, NT-proBNP, proBNP et MR-proANP) ont des qualités diagnostiques et pronostiques globalement très similaires. Néanmoins, proBNP et BNP semblent meilleurs pour le diagnostic tandis que MR-proANP apparaît meilleur pour son association avec la mortalité à 5 ans.Parmi les modifications post-transcriptionnelles du BNP, nous avons étudié l'impact de la glycosylation du pro-BNP. La O glycosylation en 71 inactive proBNP, qui est libéré hors de la cellule sans action préalable des enzymes de « cleavage » la corine ou la furine. En revanche, le proBNP non-glycosylé est scindé en BNP et NT-proBNP par la corine ou la furine. Nous avons pu montrer que la non-glycosylation du proBNP et l'activation de la furine étaient deux mécanismes très importants d'accélération de la production de peptides natriurétiques lors de l'ICA. On a pu également montrer que la production du NT-proBNP était beaucoup plus liée au niveau glycosylation du proBNP que ne l'est la production de BNP. Ainsi, nos résultats suggèrent fortement d'utiliser le NT-proBNP pour toute étude future souhaitant explorer le concept de « biomarker-guided therapy » dans l'ICA.Pour la recherche de nouveaux biomarqueurs, nous avons exploré 1-la concentration plasmatique de 5 microRNAs (miR-l/-21/-23/-126/-423-5p), chez des patients avec dyspnée aiguë. Aucun de ces miR n'a de valeur diagnostique, en revanche, le miR-423-5p apparaît être un marqueur pronostique de réhospitalisation à un an ; 2-les conséquences de la congestion cardiaque sur le foie. Les marqueurs hépatiques étudiés étaient la phosphatase alcaline et les transaminases : les marqueurs de la cholestase étaient associés à une congestion hépatique tandis que ceux de la nécrose cellulaires (transaminases) étaient liés à l'hypotension artérielle et au bas débit cardiaque. L'augmentation des transaminases a été associée à divers critères dont une surmortalité à court termeHeart failure (HF) is highly prevalent disease, and prevalence increases with age. HF is generally discovered on presentation of an acute episode of decompensation (or insufficiency). Acute decompensated heart failure (ADHF) is very frequent in elderly subjects and is difficult to diagnose when the patient is admitted with acute dyspnoea. The advent of plasma biomarkers, such as BNP or NT-proBNP represents a major advancement in the diagnostic of ADHF. ADHF leads to high rates of re-admission and mortality. The objectives of this doctoral thesis were: (1) to describe the epidemiology of ADHF in France in a one-day observational study of admissions for ADHF in 170 French hospitals; (2) to evaluate the prognostic and diagnostic value of natriuretic peptides (NPs) in ADHF; (3) to describe the extent of post-transcriptional modifications in these NPs in ADHF; and (4) to search for new biomarkers.The comparison of the prognostic and diagnostic properties of NPs showed that the 4 commercially available NPs (namely BNP, NT-proBNP, proBNP and MR-proANP) overall have very similar prognostic and diagnostic abilities. However, proBNP and BNP seem to be more useful for diagnosis, while MR-proANP appears to be better for the association with 5-year mortality.Amongthe post-transcriptional modifications of BNP, we studied the impact of glycosylation of pro¬BNP. Threonin 71 0-glycosylation prevents cleavage of proBNP into BNP and NT-proBNP, resulting in the release of proBNP from the cell without being cleaved. Conversely, non-glycosylated proBNP is cleaved into BNP and NT-proBNP by corin or furin. We showed that non-glycosylation of proBNP and activation of furin are two important mechanisms in the acceleration of production of NPs during ADHF. We also showed that production of NT-proBNP was more closely linked to the rate of glycosylation of proBNP than to the production of BNP. Thus, our results strongly suggest that NT-proBNP should be used in future studies exploring the concept of "biomarker-guided therapy" in ADHF.To investigate new biomarkers, we explored plasma concentrations of 5 microRNAs (miR-l/-21/-23/-126/-423-5p), in patients with acute dyspnoea. None of these microRNAs were shown to have any diagnostic value. Conversely, miR-423-5p appears to be a prognostic marker for re-admission at 1 year. Secondly, we investigated the consequences of cardiac congestion on the liver. The hepatic markers studied were alkaline phosphatise and transaminases. Markers of cholestasis were associated with hepatic congestive while markers of cellular necrosis (transaminases) were related to arterial hypertension and low cardiac output. An increase in transaminases was associated with various criteria of excess mortality in the short ter

Insuffisance cardiaque chronique (impact de la fréquence cardiaque et place de l'ivabradine)

BESANCON-BU Médecine pharmacie (250562102) / SudocSudocFranceF

Réponses systémiques et périphériques à la prise en charge de l insuffisance cardiaque aiguë

BESANCON-BU Médecine pharmacie (250562102) / SudocSudocFranceF