In Trauma Patients, the Occurrence of Early-Onset Nosocomial Infections is Associated With Increased Plasma Concentrations of Chromogranin A:

In previously healthy persons suffering from acute illnesses, nosocomial infections (NIs) are frequent. Their prevalence suggests the existence of as yet unknown conditions that may promote care-related infection. This study assessed whether the measurement of plasma chromogranin A, a stress-related protein involved in innate defense, is related to NI risk, and whether any chromogranin A-derived fragment included in vasostatin-I displays immunosuppressive activities related to AP-1 or NF-kappa B downregulation. At the clinical level, trauma patients and healthy controls were recruited to be eligible. Clinical histories were recorded, and standard biological tests (including plasma chromogranin A) were performed. For 9 randomly chosen patients and 16 controls, the time-dependent concentrations of chromogranin A (CGA) were assessed twice a day over 66 h. The data show that trauma patients present a higher value of CGA concentration during 66 h in comparison with healthy controls. In addition, patients maintaining this significant increase in CGA readily develop NIs. We therefore studied the effects of chromogranin A-derived peptides on monocytes, focusing on transcription factors that play a central role in inflammation. In vitro assay demonstrated that a chromogranin A-derived fragment (CGA47-70) displays a significant inhibition of NF-kappa B and AP-1 transcriptional activities in these cells. In conclusion, the occurrence of NI in trauma patients is associated with significantly increased plasma CGA concentrations. Downregulation of the two transcription factors by CGA47-70 might induce early acquired immune defect after a serious medical stress

Hematopoietic progenitor cell liabilities and alarmins S100A8/A9-related inflammaging associate with frailty and predict poor cardiovascular outcomes in older adults

Frailty affects the physical, cognitive, and social domains exposing older adults to an increased risk of cardiovascular disease and death. The mechanisms linking frailty and cardiovascular outcomes are mostly unknown. Here, we studied the association of abundance (flow cytometry) and gene expression profile (RNAseq) of stem/progenitor cells (HSPCs) and molecular markers of inflammaging (ELISA) with the cardiorespiratory phenotype and prospective adverse events of individuals classified according to levels of frailty. Two cohorts of older adults were enrolled in the study. In a cohort of pre‐frail 35 individuals (average age: 75 years), a physical frailty score above the median identified subjects with initial alterations in cardiorespiratory function. RNA sequencing revealed S100A8/A9 upregulation in HSPCs from the bone marrow (>10‐fold) and peripheral blood (>200‐fold) of individuals with greater physical frailty. Moreover higher frailty was associated with increased alarmins S100A8/A9 and inflammatory cytokines in peripheral blood. We then studied a cohort of 104 more frail individuals (average age: 81 years) with multidomain health deficits. Reduced levels of circulating HSPCs and increased S100A8/A9 concentrations were independently associated with the frailty index. Remarkably, low HSPCs and high S100A8/A9 simultaneously predicted major adverse cardiovascular events at 1‐year follow‐up after adjustment for age and frailty index. In conclusion, inflammaging characterized by alarmin and pro‐inflammatory cytokines in pre‐frail individuals is mirrored by the pauperization of HSPCs in frail older people with comorbidities. S100A8/A9 is upregulated within HSPCs, identifying a phenotype that associates with poor cardiovascular outcomes

Cateslytin and Chromofungin, two CgA derived peptides actors of the immune and cardiac systems

La CgA est une pro-hormone stockée dans les granules de sécrétion et elle subit une maturation protéolytique conduisant à la formation d’un très grand nombre de peptides dérivés. La Chromofungine (Chr: CgA47-66) et la Cateslytine (Ctl: CgA344–358) possèdent des propriétés antimicrobiennes. Staphylococcus aureus est un pathogène très virulent qui provoque un très grand nombre de graves infections cliniques et il représente une des causes principales des infections nosocomiales et la destruction du tissu endocardiaque après implantation de valve cardiaque. La première partie de l’étude nous avons montré que la Chr induise un effet inotropique négatif sans changement de la pression coronarienne. L’activation de la voie de signalisation AKT/eNOS/cGMP/PKG est responsable de cet effet de Chr. Nous avons aussi montré que Chr agit comme un agent de post-conditionnement contre les effets négatifs de l’ischémie/reperfusion, a responsables de cette cardio-protection impliquent les cascades de signalisation PI3K, RISK, MitoKATP et miRNA-21. Dans le but d’élaborer un nouveau revêtement de valves cardiaques le peptide D*T*Ctl se révèle intéressant dans des conditions non oxydantes car (1) il présente une activité antimicrobienne contre S. aureus; (2) en présence de S. aureus il permet par clivage protéolytique de libérer le peptide Ctl actif. Une première expérience réalisée in vivo a montré le rôle de Ctl pour combattre l’infection à S. aureus au niveau systémique et au niveau cardiaque, mais aussi assurer la protection du myocarde.CgA is a pro-hormone costored in secretory granules and numerous cleavage products of this protein have been identified. Chromofungin (Chr: CgA47-66) and Cateslytin (Ctl: CgA344–358) are peptides that display antimicrobial activities.Staphylococcus aureus is an opportunistic pathogen and the leading cause of a wide range of severe clinical infections and one of the most important cause of hospital-acquired infections and leading infective cause of destruction of endocardial tissue after implantation of prosthetic heart valve. The first part of the study, we found that Chr induced negative inotropic effects without changing coronary pressure. The AKT/eNOS/cGMP/PKG pathway mediated this action. We also found that Chr acted as a postconditioning agent against ischemia/reperfusion damages. Cardioprotection involved PI3K, RISK pathway, MitoKATPand miRNA-21. In order to develop a new coating of cardiac valves, the peptide D*T *Ctl proves to be useful under non-oxidizing conditions because (1) it exhibits antimicrobial activity against S. aureus; (2) in the presence of S. aureus, it allows proteolytic cleavage to release the active Ct1 peptide.In the last part of this thesis we showed in vivo the antibacterial role of Ctl against S. aureus infection at the systemic and cardiac levels, but also its cardioprotective action

Cateslytin and Chromofungin, two CgA derived peptides actors of the immune and cardiac systems

La CgA est une pro-hormone stockée dans les granules de sécrétion et elle subit une maturation protéolytique conduisant à la formation d’un très grand nombre de peptides dérivés. La Chromofungine (Chr: CgA47-66) et la Cateslytine (Ctl: CgA344–358) possèdent des propriétés antimicrobiennes. Staphylococcus aureus est un pathogène très virulent qui provoque un très grand nombre de graves infections cliniques et il représente une des causes principales des infections nosocomiales et la destruction du tissu endocardiaque après implantation de valve cardiaque. La première partie de l’étude nous avons montré que la Chr induise un effet inotropique négatif sans changement de la pression coronarienne. L’activation de la voie de signalisation AKT/eNOS/cGMP/PKG est responsable de cet effet de Chr. Nous avons aussi montré que Chr agit comme un agent de post-conditionnement contre les effets négatifs de l’ischémie/reperfusion, a responsables de cette cardio-protection impliquent les cascades de signalisation PI3K, RISK, MitoKATP et miRNA-21. Dans le but d’élaborer un nouveau revêtement de valves cardiaques le peptide D*T*Ctl se révèle intéressant dans des conditions non oxydantes car (1) il présente une activité antimicrobienne contre S. aureus; (2) en présence de S. aureus il permet par clivage protéolytique de libérer le peptide Ctl actif. Une première expérience réalisée in vivo a montré le rôle de Ctl pour combattre l’infection à S. aureus au niveau systémique et au niveau cardiaque, mais aussi assurer la protection du myocarde.CgA is a pro-hormone costored in secretory granules and numerous cleavage products of this protein have been identified. Chromofungin (Chr: CgA47-66) and Cateslytin (Ctl: CgA344–358) are peptides that display antimicrobial activities.Staphylococcus aureus is an opportunistic pathogen and the leading cause of a wide range of severe clinical infections and one of the most important cause of hospital-acquired infections and leading infective cause of destruction of endocardial tissue after implantation of prosthetic heart valve. The first part of the study, we found that Chr induced negative inotropic effects without changing coronary pressure. The AKT/eNOS/cGMP/PKG pathway mediated this action. We also found that Chr acted as a postconditioning agent against ischemia/reperfusion damages. Cardioprotection involved PI3K, RISK pathway, MitoKATPand miRNA-21. In order to develop a new coating of cardiac valves, the peptide D*T *Ctl proves to be useful under non-oxidizing conditions because (1) it exhibits antimicrobial activity against S. aureus; (2) in the presence of S. aureus, it allows proteolytic cleavage to release the active Ct1 peptide.In the last part of this thesis we showed in vivo the antibacterial role of Ctl against S. aureus infection at the systemic and cardiac levels, but also its cardioprotective action

Cateslytine et Chromofungine, deux peptides dérivés de la chromogranine A qui sont de nouveaux acteurs des systèmes immunitaires et cardiaques

CgA is a pro-hormone costored in secretory granules and numerous cleavage products of this protein have been identified. Chromofungin (Chr: CgA47-66) and Cateslytin (Ctl: CgA344–358) are peptides that display antimicrobial activities.Staphylococcus aureus is an opportunistic pathogen and the leading cause of a wide range of severe clinical infections and one of the most important cause of hospital-acquired infections and leading infective cause of destruction of endocardial tissue after implantation of prosthetic heart valve. The first part of the study, we found that Chr induced negative inotropic effects without changing coronary pressure. The AKT/eNOS/cGMP/PKG pathway mediated this action. We also found that Chr acted as a postconditioning agent against ischemia/reperfusion damages. Cardioprotection involved PI3K, RISK pathway, MitoKATPand miRNA-21. In order to develop a new coating of cardiac valves, the peptide D*T *Ctl proves to be useful under non-oxidizing conditions because (1) it exhibits antimicrobial activity against S. aureus; (2) in the presence of S. aureus, it allows proteolytic cleavage to release the active Ct1 peptide.In the last part of this thesis we showed in vivo the antibacterial role of Ctl against S. aureus infection at the systemic and cardiac levels, but also its cardioprotective action.La CgA est une pro-hormone stockée dans les granules de sécrétion et elle subit une maturation protéolytique conduisant à la formation d’un très grand nombre de peptides dérivés. La Chromofungine (Chr: CgA47-66) et la Cateslytine (Ctl: CgA344–358) possèdent des propriétés antimicrobiennes. Staphylococcus aureus est un pathogène très virulent qui provoque un très grand nombre de graves infections cliniques et il représente une des causes principales des infections nosocomiales et la destruction du tissu endocardiaque après implantation de valve cardiaque. La première partie de l’étude nous avons montré que la Chr induise un effet inotropique négatif sans changement de la pression coronarienne. L’activation de la voie de signalisation AKT/eNOS/cGMP/PKG est responsable de cet effet de Chr. Nous avons aussi montré que Chr agit comme un agent de post-conditionnement contre les effets négatifs de l’ischémie/reperfusion, a responsables de cette cardio-protection impliquent les cascades de signalisation PI3K, RISK, MitoKATP et miRNA-21. Dans le but d’élaborer un nouveau revêtement de valves cardiaques le peptide D*T*Ctl se révèle intéressant dans des conditions non oxydantes car (1) il présente une activité antimicrobienne contre S. aureus; (2) en présence de S. aureus il permet par clivage protéolytique de libérer le peptide Ctl actif. Une première expérience réalisée in vivo a montré le rôle de Ctl pour combattre l’infection à S. aureus au niveau systémique et au niveau cardiaque, mais aussi assurer la protection du myocarde

Recent Advances in Multifunctional Antimicrobial Peptides as Immunomodulatory and Anticancer Therapy: Chromogranin A-Derived Peptides and Dermaseptins as Endogenous versus Exogenous Actors

International audienceAntimicrobial peptides (AMPs) are produced by all living organisms exhibiting antimicrobial activities and representing the first line of innate defense against pathogens. In this context, AMPs are suggested as an alternative to classical antibiotics. However, several researchers reported their involvement in different processes defining them as Multifunctional AMPs (MF-AMPs). Interestingly, these agents act as the endogenous responses of the human organism against several dangerous stimuli. Still, they are identified in other organisms and evaluated for their anticancer therapy. Chromogranin A (CgA) is a glyco-phosphoprotein discovered for the first time in the adrenal medulla but also produced in several cells. CgA can generate different derived AMPs influencing numerous physiological processes. Dermaseptins (DRSs) are a family of α-helical-shaped polycationic peptides isolated from the skin secretions of several leaf frogs from the Phyllomedusidae family. Several DRSs were identified as AMPs and, until now, more than 65 DRSs have been classified. Recently, these exogenous molecules were characterized for their anticancer activity. In this review, we summarize the role of these two classes of MF-AMPs as an example of endogenous molecules for CgA-derived peptides, able to modulate inflammation but also as exogenous molecules for DRSs, exerting anticancer activities

Cateslytin and Chromofungin, two CgA derived peptides: actors of the immune and cardiac systems

Doctorate in “Life Sciences” and Physics and Physical Chemistry” Ciclo XXIXChromogranin A (CgA) belongs to the granin family of uniquely acidic secretory that are ubiquitous in secretory cells of the nervous, endocrine, immune system. Numerous cleavage products of the granins have been identified, some of these peptides showed biological activities and are costored in secretory granules of different cells. Chromofungin (Chr: CgA47-66) and Cateslytin (Ctl: CgA344–358) are peptides that display antimicrobial activities and activate neutrophils, with important implications in inflammation and innate immunity. Staphylococcus aureus is an opportunistic pathogen and the leading cause of a wide range of severe clinical infections and one of the most important cause of hospital-acquired infections, in fact infections caused by this bacterium have classically an important impact in morbidity and mortality in the nosocomial and community scene. Furthermore, this pathogen is the primary cause of surgical site infections and the most frequently isolated pathogen in Gram-positive sepsis. In the specific field of cardiovascular disease S. aureus leading infective cause of destruction of endocardial tissue after implantation of prosthetic heart valve. This pathogen is also notorious for its ability to resist the available antibiotics and dissemination of various multidrug-resistant S. aureus clones that limit therapeutic options for a S. aureus infection. Aslam et al. in 2013 shown that Ctl is resistant to the degradation of S. aureus protease and is the most antibacterial CgA derived peptide against this bacterium. The aim of study was to evaluate the: 1) Effects of Chr on isolated and Langendorff perfused rat hearts in basal and pathological conditions; 2) In vitro antibacterial activity of a synthetic Cateslytin-derived peptide to cover artificial heart valves and prevent infection by S. aureus; 3) In vivo antibacterial activity of Ctl in rat infected with S. aureus. The first part of the study was performed by using the isolated and Langendorff perfused rat hearts, Elisa assay and real-time PCR. We found that, under basal conditions, increasing doses (11–165 nM) of Chr induced negative inotropic effects without changing coronary pressure. The AKT/eNOS/cGMP/PKG pathway mediated this action. We also found that Chr acted as a postconditioning (PostC) agent against ischemia/reperfusion (I/R) damages, reducing infarct size and LDH level. Cardioprotection involved PI3K, RISK pathway, MitoKATPand miRNA-21. Therefore, we suggest that Chr directly affects heart performance, protects against I/R myocardial injuries through the activation of prosurvival kinases. Results may propose Chr as a new physiological neuroendocrinemodulator able to prevent heart dysfunctions, also encouraging the clarification of its clinical potential. In the second part of the study, two new synthetic peptides containing Ctl (RSMRLSFRARGYGFR) were designed: D*T*Ctl (DOPA-K-DOPA-K-DOPATLRGGE- RSMRLSFRARGYGFR), T*Ctl (TLRGGE-RSMRLSFRARGYGFR) with D*: DOPA-K-DOPA-K-DOPA and T*: TLRGGE. This study is based on the observation of the adhesive properties of the DOPA-K-DOPA-K-DOPA sequence and on the ability of S. aureus endoprotease Glu-C to cleave the TLRGGE sequence. Firstly, using techniques of biochemistry, proteomics (sequencing, mass spectrometry) and microbiology we shown that the digestion by the Glu-C protease of T*Ctl and D*T*Ctl is able to release active Ctl. The prediction analisys of the secondary structure suggested the presence of an alpha helix domain in the case of D*T*Ctl with respect to T*Ctl. The D* group stabilized the secondary structure and facilitated the cleavage by Glu-C to the release of the active peptide Ctl. Subsequently, the effect of the oxidation by NaIO4 of D*T*Ctl on the release of Ctl and the antibacterial activity was analized. Proteomic analysis showed the formation of polymers inhibiting the action of Glu-C and the release of Ctl. We also shown that D*T*Ctl had a MIC value around 75 μM against different strains of S. aureus. This data shown that D*T*Ctl had a direct action against the bacteria without Glu-C cleavage. However, in oxidizing conditions the formation of aggregates of D*T*Ctl reduced the antibacterial action of this synthetic peptide. In the last part of this thesis, we evaluated the in vivo antibacterial activity of Ctl and whether and to which extent Ctl elicit cardioprotection in rat infected with S. aureus, as a model of infection with this bacterium. Identification of specific molecular targets of tissue and systemic inflammation and damage were analysed by Western blotting, ELISA and microbiological analysis in cardiac homogenates and plasma. A strong reduction of plasma bacterial growth, TNF-α, IL-1β and LDH plasma levels was observed in infected rat treated with Ctl. Western blotting analysis of cardiac extracts showed that Ctl treatment is accompanied by reduction of expression of pro-inflammatory markers, such as iNOS and COX-2. These preliminary data suggest that in vivo Ctl treatment is able to counteract the deleterious effects of S. aureus, and elicits myocardial protection.University of Calabria-Italy Inserm U1121University of Strasbourg-Franc

The antimicrobial peptides secreted by the chromaffin cells of the adrenal medulla link the neuroendocrine and immune systems: From basic to clinical studies

The increasing resistance to antibiotic treatments highlights the need for the development of new antimicrobial agents. Antimicrobial peptides (AMPs) have been studied to be used in clinical settings for the treatment of infections. Endogenous AMPs represent the first line defense of the innate immune system against pathogens; they also positively interfere with infection-associated inflammation. Interestingly, AMPs influence numerous biological processes, such as the regulation of the microbiota, wound healing, the induction of adaptive immunity, the regulation of inflammation, and finally express anti-cancer and cytotoxic properties. Numerous peptides identified in chromaffin secretory granules from the adrenal medulla possess antimicrobial activity: they are released by chromaffin cells during stress situations by exocytosis via the activation of the hypothalamo-pituitary axis. The objective of the present review is to develop complete informations including (i) the biological characteristics of the AMPs produced after the natural processing of chromogranins A and B, proenkephalin-A and free ubiquitin, (ii) the design of innovative materials and (iii) the involvement of these AMPs in human diseases. Some peptides are elective biomarkers for critical care medicine, may play an important role in the protection of infections (alone, or in combination with others or antibiotics), in the prevention of nosocomial infections, in the regulation of intestinal mucosal dynamics and of inflammation. They could play an important role for medical implant functionalization, such as catheters, tracheal tubes or oral surgical devices, in order to prevent infections after implantation and to promote the healing of tissues

Chromogranin A and Its Fragments in the Critically Ill: An Expanding Domain of Interest for Better Care

Life-threatening diseases challenge immunity with a release of chromogranins. This report focuses on Chromogranin A (CGA) and some of its derived peptides in critically ill patients, with attention paid to their potential to become biomarkers of severity and actors of defense. First, we studied whether circulating CGA may be a biomarker of outcome in non-selected critically ill patients: CGA concentrations were reliably associated with short-term death, systemic inflammation, and multiple organ failure. Additionally, when studying Vasostatin-I, the major N-terminal fragment of CGA, we noted its reliable prognostic value as early as admission if associated with age and lactate. In trauma patients, CGA concentrations heralded the occurrence of care-related infections. This was associated with an in vitro inhibitor impact of Chromofungin on both NF-kappa B- and API-transcriptional activities. Secondly, in life-threatening disease-induced oxidative stress, the multimerization of Vasostatin-I occurs with the loss of its anti-microbial properties ex vivo. In vivo, a 4%-concentration of non-oxidized albumin infusion reversed multimerization with a decrease in care-related infections. Finally, in vitro Catestatin impacted the polymorphonuclear cells-Ca++-dependent, calmodulin–regulated iPLA2 pathway by releasing immunity-related proteins. Furthermore, human Cateslytin, the active domain of Catestatin, helped destroy S. aureus: this prompted the creation of synthetic D-stereoisomer of CGA-derived peptides against superbugs for the protection of implanted devices. In conclusion, CGA consideration in the critically ill is only starting, but it offers interesting perspectives for improved outcomes

Effects of RAGE Deletion on the Cardiac Transcriptome during Aging

Cardiac aging is characterized by increased cardiomyocyte hypertrophy, myocardial stiffness, and fibrosis, which enhance cardiovascular risk. The receptor for advanced glycation end-products (RAGE) is involved in several age-related diseases. RAGE knockout (Rage−/−) mice show an acceleration of cardiac dimension changes and interstitial fibrosis with aging. This study identifies the age-associated cardiac gene expression signature induced by RAGE deletion. We analyzed the left ventricle transcriptome of 2.5-(Young), 12-(Middle age, MA), and 21-(Old) months-old female Rage−/− and C57BL/6N (WT) mice. By comparing Young, MA, and Old Rage−/− versus age-matched WT mice, we identified 122, 192, and 12 differently expressed genes, respectively. Functional inference analysis showed that RAGE deletion is associated with: (i) down-regulation of genes involved in antigen processing and presentation of exogenous antigen, adaptive immune response, and cellular responses to interferon beta and gamma in Young animals; (ii) up-regulation of genes related to fatty acid oxidation, cardiac structure remodeling and cellular response to hypoxia in MA mice; (iii) up-regulation of few genes belonging to complement activation and triglyceride biosynthetic process in Old animals. Our findings show that the age-dependent cardiac phenotype of Rage−/− mice is associated with alterations of genes related to adaptive immunity and cardiac stress pathways