ACE-inhibitorische und antioxidative Aktivität von Pflanzenproteinhydrolysaten

Rudolph, Steffi

31 January 2019

Proteinhydrolysate gewinnen als Bestandteil von Lebens- und Futtermitteln zunehmend an Bedeutung. In Abhängigkeit ihrer Sequenz können darin enthaltene Peptide über Wechselwirkungen mit dem Angiotensin-Converting Enzym (ACE), welches eine Schlüsselfunktion bei der Blutdruckregulation einnimmt, physiologisch wirken und damit einen Beitrag zur Gesunderhaltung leisten oder hinsichtlich antioxidativer Eigenschaften einen positiven Effekt auf die Lagerstabilität und damit Qualität von Lebensmitteln ausüben. In der vorliegenden Arbeit wurde zunächst die ACE-inhibierende Aktivität von Pflanzenproteinen im Vergleich zum Molkenprotein hinsichtlich Struktur-Wirkbeziehungen und gegenüber den Domänen des ACEs sowie verschiedenen ACE-Spezies charakterisiert. Des Weiteren wurde eine Verkapselung von in Proteinhydrolysaten enthaltenen Dipeptiden angestrebt und der Einfluss auf deren proteolytische Stabilität untersucht. Dipeptide unterliegen während der gastrointestinalen Verdauung einem Abbau, was einen limitierenden Faktor für deren Bioaktivität darstellt. Zur Charakterisierung von Cyclodextrin-Komplexen mit aromatischen Aminosäuren sowie korrespondierenden Dipeptiden wurden UV- und fluorometrische Methoden sowie NMR-Techniken verwendet. Abschließend wurde das antioxidative Potential von Proteinhydrolysaten zunächst im Modellsystem und anschließend unter Nutzung von Lebensmittelmatrices abgeschätzt. Zusammenfassen konnte für die untersuchten Pflanzenproteinhydrolysate ein ausgesprochen gutes den potenten Milchproteinhydrolysaten vergleichbares ACE-inhibitorisches Potential als auch eine konzentrationsabhängige antioxidative Aktivität abgeleitet werden. Insbesondere Reisproteinhydrolysat erwies sich als potente Quelle physiologisch als auch antioxidativ wirksamer Peptide.

info:eu-repo/classification/ddc/540

ddc:540

Evaluation of Hospital Readmissions for Older Heart Failure Patients in Taiwan

Chen, Wei-Ling

28 July 2011

Research Objectives Heart failure (HF) is a common condition in persons older than 65 years. Existing literature indicated that hospital readmission rates after discharge for heart failure patients are immensely high. However, previous studies showed that almost half of the early hospital readmissions could be prevented. Moreover, Angiotensin-converting enzyme (ACE) inhibitor and Angiotensin receptor blocker (ARB) are the commonly used medications for heart failure patients to control blood pressure. Nevertheless, studies indicated that these two medications could also cause the risk of hospital readmission. Little studies examined the associations of medication use and hospital readmission of heart failure patients in Taiwan. This study aims to investigate the influence factors of hospital readmissions among heart failure patients in Taiwan. Study Design We collected the data from National Health Insurance (NHI) database during the period from year 2000 to 2006. Based on the rule of Bureau of National Health Insurance in Taiwan, the 14-day readmission is considered as a poor quality indicator. We categorized readmissions into 4 groups (14-day, 30-day, 180-day and over 180-day) and evaluated each group¡¦s demographic, hospital characteristics, medical resource utilization, Charlson Comorbidity Index and medication utilizations of ACE inhibitor and ARB. We conducted descriptive analyses by using chi-square and t tests and applied multivariate logistic regression analyses to estimate the probabilities of hospital readmissions of heart failure patients. Population Studied Patients aged 50 or older with heart failure were identified based on the International Classification of Diseases, Ninth Revision, Clinical Modification (ICD-9-CM). Principle Findings Among 1920 heart failure patients, 19.9% of them were readmitted within 14 days, 7.6% were readmitted within 30 days and 26% were readmitted within 180 days. The medical resource utilizations such as average inpatients cost per patient, average outpatients cost per patient, total medical cost, average of inpatients times per patient and average of outpatients times per patient were significantly higher in patients with readmissions than those without readmission. Age, Charlson Comorbidity Index, patients who had been treated with ACE inhibitors and patients who had been treated with ARB were significantly affected the probabilities of readmissions. Conclusion The heart failure patients with readmissions had significantly higher medical resource utilizations than those without readmission. The medication uses of ACE inhibitors or ARB were significantly affected the probabilities of hospital readmissions. By understanding more about the influence factors of readmissions among heart failure patients, we may provide continue improvements of quality of care and reduce unnecessary medical costs. This study results provide useful reference for policy-makers to establish effective disease management program and appropriate health care financing arrangement in the future.

heart failure

Angiotensin receptor blocker (ARB)

readmission

quality of care

Πολυμορφισμός του γονιδίου του μετατρεπτικού ενζύμου της αγγειοτενσίνης και λειτουργία των αναπνευστικών μυών σε νεογνά

Παπακωνσταντίνου, Δέσποινα

24 January 2011

Το γονίδιο του ανθρώπινου μετατρεπτικού ενζύμου της αγγειοτενσίνης ACE περιέχει έναν πολυμορφισμό δύο αλληλομόρφων που αποτελείται είτε από την παρουσία (I) είτε από την απουσία (D) ενός τμήματος 287 ζευγών βάσεων (bp). Πρόσφατες μελέτες έχουν προτείνει ότι το αλληλόμορφο Ι, μπορεί να σχετίζεται με απόδοση σχετιζόμενη με τη μυϊκή αντοχή. Αντιθέτως, το αλληλόμορφο D γονίδιο έχει συσχετισθεί με απόδοση σχετιζόμενη με τη μυϊκή ισχύ. Επιπλέον, έχει καταδειχθεί ότι η δραστικότητα του κυκλοφορούντος ACE (cACE) συσχετίζεται ευθέως με τη μυική ισχύ σε υγιείς ενήλικες. Η φυσιολογία και η βιοχημεία των αναπνευστικών μυών είναι παρόμοια με αυτή των σκελετικών μυών. Επομένως, η λειτουργικότητα των αναπνευστικών μυών και ιδίως του διαφράγματος, του πλέον σημαντικού αναπνευστικού μυ, μπορεί να επηρεάζεται αναλόγως. Η κόπωση των αναπνευστικών μυών μπορεί να οδηγεί σε αδυναμία διατήρησης του απαραίτητου κυψελιδικού αερισμού. Διάφορες μέθοδοι έχουν χρησιμοποιηθεί για να αξιολογηθούν οι ιδιότητες αντοχής των αναπνευστικών μυών. Ο διαφραγματικός δείκτης πίεσης-χρόνου (PTIdi) και ο μη επεμβατικός δείκτης πίεσης-χρόνου των αναπνευστικών μυών (PTImus), είναι δύο μέθοδοι εκτίμησης της αντοχής του διαφράγματος και των αναπνευστικών μυών, αντίστοιχα. Έχουν χρησιμοποιηθεί σε ενήλικες και παιδιά και έχουν τεκμηριωθεί σε νεογνά. Η διαφραγματική ισχύς και η ισχύς των αναπνευστικών μυών στα νεογνά μπορεί να αξιολογηθούν ειδικά με τη μέτρηση της μέγιστης δια-διαφραγματικής πίεσης (Pdimax) και της μεγίστης εισπνευστικής πίεσης αεραγωγών (Pimax), αντίστοιχα. Σκοπός. Να εξετασθεί η πιθανή συσχέτιση του πολυμορφισμού I/D του ACE και του κυκλοφορούντος ACE με την λειτουργικότητα του διαφράγματος και των αναπνευστικών μυών σε νεογνά. Δευτερεύων σκοπός ήταν ο προσδιορισμός της κατανομής του πολυμορφισμού I/D του ACE στον συγκεκριμένο πληθυσμό και η συσχέτισή του με την δραστικότητα του cACE. Υλικό και Μέθοδοι. Μελετήθηκαν νεογνά που είχαν εισαχθεί στην Μονάδα Εντατικής Νοσηλείας Νεογνών- Παιδιατρική κλινική του Πανεπιστημίου Πατρών. Τα Ι και D αλληλόμορφα του γονιδίου του ACE προσδιορίστηκαν με αλυσιδωτή αντίδραση πολυμεράσης (PCR amplification) σε DNA το οποίο εξήχθη από 0,5 mL ολικού αίματος. Η δραστηριότητα του ACE ορού αξιολογήθηκε με τη χρησιμοποίηση μιας UV κινητικής μεθόδου. Η αντοχή του διαφράγματος και των αναπνευστικών μυών εκτιμήθηκαν με μέτρηση του διαφραγματικού δείκτη πίεση-χρόνου (PTIdi) και του δείκτη πίεσης-χρόνου των αναπνευστικών μυών (PTImus), αντίστοιχα. Η διαφραγματική ισχύς και η ισχύς των αναπνευστικών μυών στα νεογνά αξιολογήθηκαν με μέτρηση της μέγιστης δια-διαφραγματικής πίεσης (Pdimax) και της μεγίστης εισπνευστικής πίεσης αεραγωγών (Pimax), αντίστοιχα. Αποτελέσματα. Συνολικά εξετάστηκαν 171 νεογνά. Στην πρώτη μελέτη της διατριβής μελετήθηκαν 148 νεογνά, στην δεύτερη μελέτη 132 και στην τρίτη μελέτη 110 νεογνά. Η κατανομή του πολυμορφισμού του ACE στο συγκεκριμένο πληθυσμό βρέθηκε κοντά σε προηγούμενα αναφερόμενα στοιχεία. Τα νεογνά με Ι/Ι γονότυπο είχαν χαμηλότερο PTIdi και PTImus από τα νεογνά με γονοτύπους είτε D/D ή I/D. Η ανάλυση των επιμέρους στοιχείων των PTIdi και PTImus έδειξε ότι μόνο οι λόγοι Pdimean (μέση διαδιαφραγματική πίεση) προς Pdimax και Pimean (μέση πίεση αεραγωγών) προς Pimax, αντίστοιχα, ήταν χαμηλότεροι σε νεογνά με γονότυπο I/I έναντι των νεογνών με γονοτύπους είτε D/D είτε I/D. Οι Pdimax και Pimax δεν ήταν στατιστικά διαφορετικές ανάμεσα στις τρείς ομάδες. Ανάλυση βηματικής παλινδρόμησης κατέδειξε σημαντική συσχέτιση των γονότυπων του ACE με τις τιμές του PTIdi και του PTImus, ανεξαρτήτως παραγόντων που θα μπορούσαν να επηρεάσουν την λειτουργικότητα του διαφράγματος και των αναπνευστικών μυών. Νεογνά με το D/D γονότυπο είχαν αυξημένη δραστικότητα ACE ορού σε σχέση με νεογνά με I/I ή I/D γονοτύπους. Η δραστικότητα του cACE σχετιζόταν σημαντικά ευθέως με τη Pimax και αντιστρόφως με το PTImus. Συμπεράσματα. Στις μελέτες αυτής της διατριβής ανεδείχθη συσχέτιση ανάμεσα στους γονοτύπους του ACE και την αντοχή του διαφράγματος και γενικότερα των αναπνευστικών μυών όπως αξιολογείται με τη μέτρηση των PTIdi και PTImus, αντίστοιχα, σε νεογνά. Δεν ανεδείχθη συσχέτιση ανάμεσα στους γονοτύπους του ACE και την ισχύ του διαφράγματος και γενικότερα των αναπνευστικών μυών όπως αξιολογείται με τη μέτρηση των Pdimax και Pimax, αντίστοιχα, σε αυτό τον πληθυσμό. Εντούτοις, κατεδείχθη μια θετική συσχέτιση μεταξύ της δραστικότητας του ACE ορού και της ισχύος των αναπνευστικών μυών, όπως αυτή αξιολογείται από μετρήσεις της Pimax , και μια αρνητική συσχέτιση ανάμεσα στη δραστικότητα του ACE ορού και του PTImus. Επιπλέον, δείχθηκε μια συσχέτιση του αλληλόμορφου D γονιδίου του γονοτύπου ACE με την αυξημένη δραστικότητα του cACE στα νεογνά. / The human ACE (angiotensin converting enzyme) gene contains a polymorphism consisting of either the presence (insertion, I) or absence (deletion, D) of a 287 base pair (bp) fragment. Recent studies have suggested that the I-allele may be associated with endurance performance. Conversely, D-allele has been associated with power-oriented performance. Moreover, it has been suggested that circulating ACE (cACE) activity is correlated with muscle strength in healthy adults. The physiological and biochemical properties of the respiratory and skeletal muscles are quite similar. Therefore, respiratory muscle and specific diaphragmatic function, may be similarly influenced. Fatigue of respiratory muscles may result in inability to maintain adequate alveolar ventilation. Several methods have been used to assess the endurance properties of respiratory muscles. Diaphragmatic pressure-time index (PTIdi) and the non-invasive pressure-time index of respiratory muscles (PTImus), are two methods of assessment of diaphragmatic and respiratory muscle endurance, respectively. They have been validated in both adults and infants. Diaphragmatic and respiratory muscle strength in infants can be assessed specifically, by measurement of maximum transdiaphragmatic pressure (Pdimax) and maximum inspiratory pressure (Pimax), respectively. Aims. To examine the possible association of the I/D genotypes of ACE and cACE, with diaphragmatic and respiratory muscle performance, in infants. Secondary aims were to identify the distribution of the I/D genotypes of ACE in the specific population and its association with cACE activity. Material and methods. Infants cared for at the Neonatal Intensive Care Unit- Paediatric Department of the University General Hospital of Patras, Greece, were eligible for the study. ACE genotyping was performed by polymerase chain reaction amplification on DNA, extracted from 0,5 ml of whole blood. Serum ACE activity was assayed by using a UV-kinetic method. The endurance of the diaphragm and the respiratory muscles was assessed by measurement of diaphragmatic pressure-time index (PTIdi) and pressure-time index of the respiratory muscles (PTImus), respectively. Diaphragmatic and respiratory muscle strength was assessed by measurement of maximum transdiaphragmatic (Pdimax) and maximum inspiratory (Pimax) pressures, respectively. Results. One hundred seventy one infants were recruited. One hundred fourty eight infants were included in the first study, one hundred thirty two in the second study and one hundred ten in the third study of this thesis. The distribution of the I/D genotypes of ACE in the specific population was close to previous reported data. Infants with I/I ACE genotype had lower PTIdi and PTImus than infants with either D/D or I/D genotypes. Analysis of the components of the PTIdi and PTImus has shown that the ratios of Pdimean to Pdimax and Pimean to Pimax , only, were lower in infants with the I/I genotype, compared to infants with either the D/D or I/D genotypes. Neither Pdimax, nor Pimax were statistically different between the three groups. A stepwise regression analysis revealed that ACE genotypes were significantly related to the PTIdi and PTImus measurements, independent of other factors that may affect diaphragmatic and respiratory muscle function. Infants with D/D genotype had significantly higher serum ACE activity than infants with I/I or I/D genotypes. Circulating ACE activity was significantly related to Pimax and inversely related to PTImus. Conclusions. In the studies of this thesis, an association between ACE genotypes and the endurance of the diaphragm and the respiratory muscles, assessed by measurement of PTIdi and PTImus, respectively, was demonstrated, in infants. No such association was demonstrated between ACE genotypes and strength of the diaphragm and the respiratory muscles, assessed by measurement of Pdimax and Pimax, respectively, in the specific population. However, a positive correlation between serum ACE activity and respiratory muscle strength, assessed by measurement of Pimax and and a negative correlation between serum ACE activity and PTImus, was shown. Moreover, an association of D-allele of ACE genotype with increased circulating ACE activity in infants, was demonstrated.

Αναπνευστικοί μύες

Πολυμορφισμός

Νεογνολογία

618.922

Angiotensin converting enzyme (ACE)

Respiratory muscles

Polymorphism

Neonatology

Associa??o da frequ?ncia al?lica dos polimorfismos dos genes do sistema renina angiotensina com a for?a muscular e press?o arterial de idosas

Oliveira, Hildeamo Bonif?cio

12 December 2012

Made available in DSpace on 2014-12-17T14:13:45Z (GMT). No. of bitstreams: 1 HildeamoBO_TESE.pdf: 915178 bytes, checksum: 80d936a712feea6bd3e9ced994b731a6 (MD5) Previous issue date: 2012-12-12 / Physiological changes induced by the aging process is dynamic and progressive, reducing the adaptability and independence of older people and may be influenced by genetic and environmental factors. Thus the aim of this thesis was to investigate the association between polymorphism of the ACE gene ID and the phenotypes of muscular strength and blood pressure of 62 elderly Brazilian (67.35 ? 5.66 years) during a 16-week program of supervised training. The elderly women were stratified by age, with the group 1 (G1, n = 34) <70 years and group 2 (G2 n = 28) &#8805; 70 years, and in three groups by ACE, ACE-II (n = 8) ACE- DD (n = 35) and ACE-ID (n = 19). The level of muscle strength was evaluated by the method of maximum repetitions and measures of blood pressure (BP) were measured before and after training (PAPr?1 and PAP?s1) and before and after each training session (PAPre2 and PAP?s2), in place of training. DNA samples were isolated from peripheral blood leukocytes polymorphism and insertion / deletion (ID) of the ACE gene (rs1800795) was genotyped by polymerase chain reaction (PCR) plus PCR-confirmatory. The genotype distribution of the polymorphism ID attended the prerogatives of Hardy-Weit?herg. There was variation in power levels before and after training and the age between groups (t-test) and the ACE polymorphism (ANOVA) (p <0.05). Depending on the results it was concluded that resistance training helps to reduce SBP and increased muscle strength of upper and lower limbs when considering the age and ACE polymorphism. In this study the Elderly carriers of the D allele were more reactive to changes in BP resistance training. This study was multidisciplinary project involving researchers in the areas Medical, Physical Education, Pharmacy, Nutrition, Gerontology and Statistics. This fulfilled the requirements of the multidisciplinary Graduate Program in Health Sciences / As altera??es fisiol?gicas induzidas pelo processo de envelhecimento s?o din?micas e progressivas, reduzindo a capacidade de adapta??o e autonomia do idoso, podendo ser influenciada por fatores gen?ticos e ambientais. Assim o objetivo desta tese foi verificar a associa??o entre o polimorfismo ID do gene da ECA e os fen?tipos de for?a muscular e press?o arterial sist?mica de 62 idosas brasileiras (67,35?5,66 anos) durante um programa de 16 semanas de treinamento supervisionado. As idosas foram estratificadas pela idade, sendo o grupo1 (G1, n=34 )<70 anos e grupo 2 (G2 n=28)&#8805; 70 anos, e em tr?s grupos pela ECA, ECA-II (n=8) ECA-DD (n=35) e ECA-ID (n=19). O n?vel de for?a muscular foi avaliado pelo m?todo de repeti??es m?ximas e as medidas da press?o arterial (PA) foram aferidas antes e ap?s o treinamento (PAPr?1 e PAP?s1) e antes e ap?s cada sess?o de treino (PAPre2 e PAP?s2), no local de treinamento. Amostras de DNA foram isoladas a partir de leuc?citos de sangue perif?rico e o polimorfismo de inser??o/dele??o (ID) do gene ECA (rs1800795) foi genotipado pela rea??o em cadeia de polimerase (PCR) acrescida de PCR-confirmat?ria. A distribui??o genot?pica do polimorfismo ID atendeu as prerrogativas do equil?brio de Hardy-Weit?herg. Houve varia??o nos n?veis de for?a pr? e p?s-treinamento e entre os grupos pela idade (teste t) e pelo polimorfismo da ECA (ANOVA) com (p<0,05). Em fun??o dos resultados concluiu-se que o treinamento contra resist?ncia contribui para redu??o da PAS e aumento da for?a muscular de membros superiores e inferiores quando consideradas a idade e o polimorfismo da ECA. Neste estudo as Idosas portadoras do alelo D foram mais reativas as varia??es da PA ao treinamento resistido. A realiza??o deste estudo teve car?ter multidisciplinar, envolvendo pesquisadores das ?reas Medicina, Educa??o F?sica, Farm?cia, Nutri??o, Gerontologia e Estat?stica. Este aspecto preencheu os requisitos da multidisciplinaridade do Programa de P?s-gradua??o em Ci?ncias da Sa?de

CNPQ::CIENCIAS DA SAUDE

Análise dos constituintes de baixa massa molecular de quatro venenos do gênero Bitis e suas atividades biológicas. / Analysis of the low molecular mass constituents from the venom of four species of the Bitis genus and biological activities.

Kodama, Roberto Tadashi

07 August 2015

Na África subsaariana, as serpentes do gênero Bitis são de extrema importância, pois suas vítimas apresentam sintomas como dano local, hemorragia e uma severa hipotensão. Este trabalho identificou moléculas capazes de inibir a atividade da enzima conversora de angiotensina I (ECA) presentes no veneno de quatro serpentes do gênero Bitis. Para isto, as porções de baixa massa molecular desses 4 venenos foram fracionadas em RP-HPLC e as frações com boa inibição sobre a atividade da ECA foram analisadas por espectrometria de massas. Foram identificados 34 oligopeptídeos ricos em prolina (PRO), sendo 8 sintetizados e suas constantes de inibição (Ki) determinadas. Em testes com substratos naturais da ECA, angiotensina I e bradicinina, foi constatada a maior inibição da hidrólise da angiotensina I por quatro PROs. Todos os PROs in vivo reduziram a pressão arterial, e seis deles aumentaram a frequência cardíaca em ratos Wistar. Com isto, conclui-se que existem toxinas no veneno de serpentes do gênero Bitis responsáveis pela hipotensão. / In the sub-saharian Africa, snakes from the Bitis genus are of extreme medical importance, since its victims show symptoms as local tissue damage, hemorrhage and a severe hypotension. This work identified molecules that inhibit the angiotensin I converting enzyme (ACE) in the venom of 4 snakes from the Bitis genus. The low molecular portions of the venom of these snakes were fractionated in RP-HPLC and the fractions that efficiently inhibited the ACE activity were analyzed by mass spectrometry. 34 proline-rich oligopeptides were identified, 8 of them synthesized and had their inhibition constants (Ki) determined. In tests using natural substrates of ACE, angiotensin I and bradykinin, the angiotensin I hydrolysis were better inhibited by four PROs. In vivo tests results showed that all PROs decreased the mean arterial pressure and six of them increased the heart rate. Therefore, we can conclude that there are toxins present in the venom of Bitis capable of cause hypotension.

Bitis

Bitis

Angiotensin-converting enzyme (ACE)

Bradykinin-potentiating peptide (BPP)

Enzima conversora de angiotensina I

Hipotensão

Hypotension

Peptídeo rico em prolina

Proline-rich oligpeptide

Veneno

Venom

Análise dos constituintes de baixa massa molecular de quatro venenos do gênero Bitis e suas atividades biológicas. / Analysis of the low molecular mass constituents from the venom of four species of the Bitis genus and biological activities.

Roberto Tadashi Kodama

07 August 2015

Na África subsaariana, as serpentes do gênero Bitis são de extrema importância, pois suas vítimas apresentam sintomas como dano local, hemorragia e uma severa hipotensão. Este trabalho identificou moléculas capazes de inibir a atividade da enzima conversora de angiotensina I (ECA) presentes no veneno de quatro serpentes do gênero Bitis. Para isto, as porções de baixa massa molecular desses 4 venenos foram fracionadas em RP-HPLC e as frações com boa inibição sobre a atividade da ECA foram analisadas por espectrometria de massas. Foram identificados 34 oligopeptídeos ricos em prolina (PRO), sendo 8 sintetizados e suas constantes de inibição (Ki) determinadas. Em testes com substratos naturais da ECA, angiotensina I e bradicinina, foi constatada a maior inibição da hidrólise da angiotensina I por quatro PROs. Todos os PROs in vivo reduziram a pressão arterial, e seis deles aumentaram a frequência cardíaca em ratos Wistar. Com isto, conclui-se que existem toxinas no veneno de serpentes do gênero Bitis responsáveis pela hipotensão. / In the sub-saharian Africa, snakes from the Bitis genus are of extreme medical importance, since its victims show symptoms as local tissue damage, hemorrhage and a severe hypotension. This work identified molecules that inhibit the angiotensin I converting enzyme (ACE) in the venom of 4 snakes from the Bitis genus. The low molecular portions of the venom of these snakes were fractionated in RP-HPLC and the fractions that efficiently inhibited the ACE activity were analyzed by mass spectrometry. 34 proline-rich oligopeptides were identified, 8 of them synthesized and had their inhibition constants (Ki) determined. In tests using natural substrates of ACE, angiotensin I and bradykinin, the angiotensin I hydrolysis were better inhibited by four PROs. In vivo tests results showed that all PROs decreased the mean arterial pressure and six of them increased the heart rate. Therefore, we can conclude that there are toxins present in the venom of Bitis capable of cause hypotension.

Bitis

Enzima conversora de angiotensina I

Hipotensão

Peptídeo rico em prolina

Veneno

Bitis

Angiotensin-converting enzyme (ACE)

Bradykinin-potentiating peptide (BPP)

Hypotension

Proline-rich oligpeptide

Venom

Étude du rôle de R-spondin3 dans la formation des artères coronaires et des nouvelles fonctions dans la signalisation de l'acide rétinoïque au cours du développement et de la réparation cardiaque / The role of R-spondin3 in coronary artery formation and novel roles for retinoic acid signaling in cardiac development and repair

Da Silva, Fabio

13 October 2017

Les maladies coronariennes sont l'une des principales causes de décès dans le monde. Comment les artères coronaires sont modelées et quelles sont les molécules de signalisation qui régissent ce processus, sont des mécanismes mal compris. Dans la première partie de ma thèse, j'ai identifié le modulateur de signalisation Wnt Rspo3 comme un régulateur crucial de la formation de l'artère coronaire dans le cœur en développement. Rspo3 est spécifiquement exprimé autour des branches coronaires à des moments critiques dans leur développement. L'ablation temporelle de Rspo3 conduit à une diminution de la signalisation de β-caténine et à une réduction de la prolifération spécifique des artères. En conséquence, les branches coronariennes sont défectueuses et l'arbre artériel ne se forme pas correctement. Ces résultats identifient un mécanisme par lequel l'expression localisée de RSPO3 induit la prolifération des artères coronaires à leurs branches permettant leur formation. Le traitement des patients qui se remettent d'un infarctus du myocarde (IM) est difficile car les cardiomyocytes ont une capacité très limitée à régénérer le cœur endommagé. La voie de signalisation de l'acide rétinoïque (AR) est essentielle pour le développement cardiaque et joue un rôle protecteur dans les cœurs endommagés. Pour la deuxième partie de ma thèse, j'ai utilisé une nouvelle lignée rapportrice de l’AR et j'ai observé une réponse spécifique des cardiomyocytes. L'ablation de la signalisation de l’AR par délétion génétique des enzymes Raldh1/2/3 entraîne une augmentation de l'apoptose myocytaire à la fin du développement tardif et après l'IM. Le séquençage des ARNs des cardiomyocytes primaires révèle que le traitement à l’AR réprime l'expression de Ace1, indiquant un nouveau lien entre la signalisation AR et le système Rénine Angiotensine dans le contexte de la réparation cardiaque. / Coronary heart disease is one of the leading causes of death worldwide. How coronary arteries are remodeled and the signaling molecules that govern this process are poorly understood. For the first part of my thesis, I have identified the Wnt-signaling modulator Rspo3 as a crucial regulator of coronary artery formation in the developing heart. Rspo3 is specifically expressed around the coronary stems at critical time-points in their development. Temporal ablation of Rspo3 leads to decreased β-catenin signaling and a reduction in arterial-specific proliferation. As a result, the coronary stems are defective and the arterial tree does not form properly. These results identify a mechanism through which localized expression of RSPO3 induces proliferation of the coronary arteries at their stems and permits their formation. Treating patients recovering from myocardial infarction (MI) is difficult since cardiomyocytes have a very limited capacity to proliferate and regenerate the damaged heart. The Retinoic Acid (RA) signaling pathway is essential for cardiac development and plays a protective role in damaged hearts. For the second part of my thesis, I have utilized a novel RA reporter line and I have observed a cardiomyocyte-specific response. Ablation of RA signaling through genetic deletion of the Raldh1/2/3 enzymes leads to increased myocyte apoptosis both during late development and after MI. RNA sequencing analysis of primary cardiomyocytes reveals atRA treatment represses Ace1 expression, providing a novel link between RA signaling and the Renin Angiotensin System in the context of heart repair.

R-spondin3

Signalisation Wnt

Artères coronaires

Signalisation acide rétinoïque

Infarctus du myocarde

Raldh

R-spondin3

Wnt signaling

Coronary arteries

Retinoic Acid signaling

Myocardial infarction

Raldh

Angiotensin converting enzyme (ACE)