En février, 2009 un rapport de PHRMA (Pharmaceutical Research and Manufacturers of America) confirmait que plus de 300 médicaments pour le traitement des maladies cardiaques étaient en phase d’essais cliniques ou en révision par les agences règlementaires. Malgré cette abondance de nouvelles thérapies cardiovasculaires, le nombre de nouveaux médicaments approuvés chaque année (toutes indications confondues) est en déclin avec seulement 17 et 24 nouveaux médicaments approuvés en 2007 et 2008, respectivement. Seulement 1 médicament sur 5000 sera approuvé après 10 à 15 ans de développement au coût moyen de 800 millions .Denombreusesinitiativesonteˊteˊlanceˊesparlesagencesreˋglementairesafind’augmenterletauxdesucceˋslorsdudeˊveloppementdesnouveauxmeˊdicamentsmaislesreˊsultatstardent.Cettestagnationestattribueˊeaumanqued’efficaciteˊdunouveaumeˊdicamentdansbiendescasmaisleseˊvaluationsd’innocuiteˊremportentlapalmedescausesd’arre^tdedeˊveloppement.Primumnonnocere,lamaximed’Hippocrate,peˋredelameˊdecine,demeured’actualiteˊendeˊveloppementpreˊcliniqueetcliniquedesmeˊdicaments.Environ3Eˊvoluantparmilescontraintesetlesdeˊfisdesprogrammesdedeˊveloppementsdesmeˊdicaments,nousavonseˊvalueˊl’efficaciteˊetl’innocuiteˊdel’oxytocine(OT),unpeptideendogeˋneaˋdesfinstheˊrapeutiques.L’OT,unehormonehistoriquementassocieˊeaˋlareproduction,adeˊmontreˊlacapaciteˊd’induireladiffeˊrentiationinvitrodeligneˊescellulaires(P19)maisaussidecellulessouchesembryonnairesencardiomyocytesbattants.Cesobservationsnousontameneˊaˋconsideˊrerl’utilisationdel’OTdansletraitementdel’infarctusdumyocarde.Afind’arriveraˋcetobjectifultime,nousavonsd’abordeˊvalueˊlapharmacocineˊtiquedel’OTdansunmodeˋlederatanestheˊsieˊ.Ceseˊtudesontmiseneˊvidencedescaracteˊristiquesuniquesdel’OTdontunecourtedemi−vieetunprofilpharmacocineˊtiquenon−lineˊaireenrelationavecladoseadministreˊe.Ensuite,nousavonseˊvalueˊleseffetscardiovasculairesdel’OTsurdesanimauxsainsdediffeˊrentesespeˋces.Enrecherchepreˊclinique,l’utilisationdeplusieursespeˋcesainsiquedediffeˊrentseˊtats(conscientsetanestheˊsieˊs)estreconnuecommeeˊtantunedesmeilleuresapprochesafind’accroı^trelavaleurpreˊdictivedesreˊsultatsobtenuschezlesanimauxaˋlareˊponsechezl’humain.Desmodeˋlesderatsanestheˊsieˊseteˊveilleˊs,dechiensanestheˊsieˊseteˊveilleˊsetdesingeseˊveilleˊsavecsuivicardiovasculaireparteˊleˊmeˊtrieonteˊteˊutiliseˊs.L’OTs’estaveˊreˊe^treunagentayantd’importantseffetsheˊmodynamiquespreˊsentantunereˊponsevariableselonl’eˊtat(anestheˊsieˊoueˊveilleˊ),ladose,lemoded’administration(bolusouinfusion)etl’espeˋceutiliseˊe.Ceseˊtudesnousontpermisd’eˊtablirlesdosesetreˊgimesdetraitementn’ayantpasd’effetscardiovasculairesadversesetpouvante^treutiliseˊesdanslecadredeseˊtudesd’efficaciteˊsubseˊquentes.Unmodeˋleporcind’infarctusdumyocardeavecreperfusionaeˊteˊutiliseˊafind’eˊvaluerleseffetsdel’OTdansletraitementdel’infarctusdumyocarde.Danslecadred’unprojetpilote,l’infusioncontinued’OTinitieˊeimmeˊdiatementaumomentdelareperfusioncoronarienneainduitdeseffetscardiovasculairesadversescheztouslesanimauxtraiteˊsincluantunereˊductiondelafractionderaccourcissementventriculairegaucheetuneaggravationdelacardiomyopathiedilateˊesuiteaˋl’infarctus.Consideˊrantcesobservations,l’approchetheˊrapeutiquefu^treˊviseˊeafind’eˊviterletraitementpendantlapeˊrioded’inflammationaigu¨econsideˊreˊemaximaleautourdu3ieˋmejoursuiteaˋl’ischeˊmie.Lorsqu’initieˊ8joursapreˋsl’ischeˊmiemyocardique,l’infusiond’OTaengendreˊdeseffetsadverseschezlesanimauxayantdesniveauxendogeˋnesd’OTeˊleveˊs.Parailleurs,aucuneffetadverse(ameˊliorationnon−significative)nefu^tobserveˊchezlesanimauxayantunfaibleniveauendogeˋned’OT.Chezlesanimauxdugroupeplacebo,unetendanceaˋobserverunemeilleurereˊcupeˊrationchezceuxayantdesniveauxendogeˋnesinitiauxeˊleveˊsfu^tnoteˊe.Bienquelatailledelazoneischeˊmiqueaˋrisquesoitcomparableaˋcellerencontreˊechezlespatientsatteintsd’infarctus,l’utilisationd’animauxjuveˊnilesetl’absencedemaladiescoronariennessontdeslimitationsimportantesdumodeˋleporcinutiliseˊ.Lepotentieldel’OTpourletraitementdel’infarctusdumyocardedemeuremaisnosreˊsultatssuggeˋrentqu’uneadministrationsysteˊmiqueaˋtitredetheˊrapiederemplacementdel’OTdevraite^treconsideˊreˊeenfonctionduniveauendogeˋne.Deplusampleseˊvaluationsdelaseˊcuriteˊdutraitementavecl’OTdansdesmodeˋlesanimauxd’infarctusdumyocardeserontneˊcessairesavantdeconsideˊrerl’utilisationd’OTdansunepopulationdepatientsatteintd’uninfarctusdumyocarde.Encontrepartie,lesniveauxendogeˋnesd’OTpourraientposseˊderunevaleurpronostiqueetdeseˊtudescliniquesaˋceteˊgardpourraiente^tred’inteˊre^t.Infebruary2009,areportfromPHRMA(PharmaceuticalResearchandManufacturersofAmerica)confirmedthatmorethan300drugsfortreatmentofcardiovasculardiseaseswereinclinicaltrialsorunderreviewbyregulatoryagencies.Despitetheabundanceofnewcardiovasculartherapies,thenumberofnewdrugsapprovedeachyear(allindicationscombined)isdecliningsteadilywithonly17and24newdrugsapprovedin2007and2008,respectively.Only1drugoutof5000candidateswillbeapprovedafter10to15yearsofdevelopmentwithanaveragecostof800 millions. Several initiatives have been launched by regulatory agencies to increase the success rate in drug development but results are still awaited. This stagnation is attributed to the lack of efficacy of several drug candidates but safety assessments are the leading cause of drug development discontinuation. Primum non nocere, the maxim from Hippocrate, father of medicine, remains of major relevance in preclinical and clinical drug development. Over the past 20 years, approximately 3% of approved drugs were subsequently withdrawn from the market due to adverse effects. Cardiovascular adverse effects represent the most frequent cause of drug development discontinuation or withdrawal (27%) followed by effects on the nervous system. After defining the context of safety pharmacology evaluations and the use of biomarkers in drug development, we validated safety pharmacology models to investigate drug-induced cardiovascular, respiratory and neurological effects.
As we progressed within constraints and challenges of drug development, we evaluated the efficacy and safety of oxytocin, an endogenous peptide with therapeutic potential. Oxytocin (OT), a hormone historically associated with reproduction, demonstrated the ability to induce in vitro differentiation of cell lines (P19) but also embryonic stem cells into beating cardiomyocytes. These observations lead us to consider the use of OT as a treatment for myocardial infarct. To achieve this ultimate goal, we first evaluated the pharmacokinetic of OT in an anesthetized rat model. These investigations highlighted the unique characteristics of OT including a very short half-life and a non-linear pharmacokinetic profile in response to the dose.
Cardiovascular effects of OT in healthy animals were then evaluated in various species. In preclinical research, the use of various animal species and state of consciousness (conscious or anesthetized) is recognized as one of the best strategies to increase the predictive value of results obtained in animals to the human response. Our initial investigations of OT treatment regimens used various animal models including conscious and anesthetized rats, anesthetized pigs, conscious dogs with indirect blood pressure monitoring and diuresis and conscious monkeys with cardiovascular telemetry monitoring. These studies confirmed OT to have significant hemodynamic effects with variable responses depending on the state of consciousness (conscious or anesthetized), the dose, the administration protocol (bolus or infusion) and the species that were used. These screening studies enabled selection of a treatment regimen and dose without adverse effects that could subsequently be tested in efficacy studies.
A porcine myocardial infarct (MI) model with reperfusion was used to evaluate the effects of OT following myocardial ischemia. In a pilot project, continuous infusion of OT initiated immediately at coronary reperfusion induced cardiovascular adverse effects in all treated animals including a reduction of left ventricular fraction shortening and worsening of dilated cardiomyopathy which is typical following MI. Considering these observations, the therapeutic strategy was revised to avoid OT treatment during the inflammatory phase which was considered maximal around day 3 post-ischemia. When initiated 8 days after MI, OT infusion induced adverse effects in animals with elevated endogenous levels of OT. In contrast, no significant effects (not statistically significant improvement) were observed in animals with low endogenous OT baseline. In placebo treated animals, a trend to observe a better recovery was noted in animals with high endogenous OT baseline. While the size of the ischemic zone was comparable to human patients with MI, the use of juvenile animals and the absence of coronary disease are important limitations of the porcine model.
The potential of OT for treatment of MI remains but our results suggest that systemic administration of OT by continuous infusion as part of a replacement therapy should be investigated further in relation to endogenous levels. Further investigations on safety of the treatment with OT on animal MI models are warranted before the use of OT can be considered in the patient population after myocardial infarct. On the other hand, endogenous levels of OT may have a prognostic value and clinical trials to investigate this hypothesis may be of interest
In silico modeling offers an opportunity to supplement and accelerate cardiac safety testing. With in silico modeling, computational simulation methods are used to predict electrophysiological interactions and pharmacological effects of novel drugs on critical physiological processes. The O’Hara-Rudy’s model was developed to predict the response to different ion channel inhibition levels on cardiac action potential duration (APD) which is known to directly correlate with the QT interval. APD data at 30% 60% and 90% inhibition were derived from the model to delineate possible ventricular arrhythmia scenarios and the marginal contribution of each ion channel to the model. Action potential values were calculated for epicardial, myocardial, and endocardial cells, with action potential curve modeling. This study assessed cardiac ion channel inhibition data combinations to consider when undertaking in silico modeling of proarrhythmic effects as stipulated in the Comprehensive in Vitro Proarrhythmia Assay (CiPA). As expected, our data highlight the importance of the delayed rectifier potassium channel (IKr) as the most impactful channel for APD prolongation. The impact of the transient outward potassium channel (Ito) inhibition on APD was minimal while the inward rectifier (IK1) and slow component of the delayed rectifier potassium channel (IKs) also had limited APD effects. In contrast, the contribution of fast sodium channel (INa) and/or L-type calcium channel (ICa) inhibition resulted in substantial APD alterations supporting the pharmacological relevance of in silico modeling using input from a limited number of cardiac ion channels including IKr, INa, and ICa, at least at an early stage of drug development
Introduction The Safety Pharmacology Society (SPS) has conducted a survey of its membership to identify industry practices related to testing considered in the Comprehensive In vitro Proarrhythmia Assay (CiPA). Methods Survey topics included nonclinical approaches to address proarrhythmia issues, conduct of in silico studies, in vitro ion channel testing methods used, drugs used as positive controls during the conduct of cardiac ion channel studies, types of arrhythmias observed in non-clinical studies and use of the anticipated CiPA ion channel assay. Results In silico studies were used to evaluate effects on ventricular action potentials by only 15% of responders. In vitro assays were used mostly to assess QT prolongation (95%), cardiac Ca2 + and Na+ channel blockade (82%) and QT shortening or QRS prolongation (53%). For de-risking of candidate drugs for proarrhythmia, those assays most relevant to CiPA including cell lines stably expressing ion channels used to determine potency of drug block were most frequently used (89%) and human stem cell-derived or induced pluripotent stem cell cardiomyocytes (46%). Those in vivo assays related to general proarrhythmia derisking include ECG recording using implanted telemetry technology (88%), jacketed external telemetry (62%) and anesthetized animal models (53%). While the CiPA initiative was supported by 92% of responders, there may be some disconnect between current practice and future expectations, as explained. Discussion Proarrhythmia liability assessment in drug development presently includes study types consistent with CiPA. It is anticipated that CiPA will develop into a workable solution to the concern that proarrhythmia liability testing remains suboptimal
The human voltage-gated sodium channel Nav1.5 (hNav1.5/SCN5A) plays a critical role in the initiation and propagation of action potentials in cardiac myocytes, and its modulation by various drugs has significant implications for cardiac safety. Drug-dependent block of Nav1.5 current (INa) can lead to significant alterations in cardiac electrophysiology, potentially resulting in conduction slowing and an increased risk of proarrhythmic events. This review aims to provide a comprehensive overview of the mechanisms by which various pharmacological agents interact with Nav1.5, focusing on the molecular determinants of drug binding and the resultant electrophysiological effects. We discuss the structural features of Nav1.5 that influence drug affinity and specificity. Special attention is given to the concept of state-dependent block, where drug binding is influenced by the conformational state of the channel, and its relevance to therapeutic efficacy and safety. The review also examines the clinical implications of INa block, highlighting case studies of drugs that have been associated with adverse cardiac events, and how the Vaughan-Williams Classification system has been employed to qualify unsafe sodium channel block. Furthermore, we explore the methodologies currently used to assess INa block in nonclinical and clinical settings, with the hope of providing a weight of evidence approach including in silico modeling, in vitro electrophysiological assays and in vivo cardiac safety studies for mitigating proarrhythmic risk early in drug discovery. This review underscores the importance of understanding Nav1.5 pharmacology in the context of drug development and cardiac risk assessment
In this paper we present the first high-resolution laser spectroscopy results
obtained at the GISELE laser laboratory of the GANIL-SPIRAL2 facility, in
preparation for the first experiments with the S3-Low Energy Branch. Studies
of neutron-deficient radioactive isotopes of erbium and tin represent the first
physics cases to be studied at S3. The measured isotope-shift and hyperfine
structure data are presented for stable isotopes of these elements. The erbium
isotopes were studied using the 4f126s23H6→4f12(3H)6s6pJ=5 atomic transition (415 nm) and the tin isotopes were studied by
the 5s25p2(3P0)→5s25p6s(3P1) atomic transition (286.4
nm), and are used as a benchmark of the laser setup. Additionally, the tin
isotopes were studied by the 5s25p6s(3P1)→5s25p6p(3P2)
atomic transition (811.6 nm), for which new isotope-shift data was obtained and
the corresponding field-shift F812 and mass-shift M812 factors are
presented
Through an international consortium, we have collected 37 tau- and TAR DNA-binding protein 43 (TDP-43)-negative frontotemporal lobar degeneration (FTLD) cases, and present here the first comprehensive analysis of these cases in terms of neuropathology, genetics, demographics and clinical data. 92% (34/37) had fused in sarcoma (FUS) protein pathology, indicating that FTLD-FUS is an important FTLD subtype. This FTLD-FUS collection specifically focussed on aFTLD-U cases, one of three recently defined subtypes of FTLD-FUS. The aFTLD-U subtype of FTLD-FUS is characterised clinically by behavioural variant frontotemporal dementia (bvFTD) and has a particularly young age of onset with a mean of 41 years. Further, this subtype had a high prevalence of psychotic symptoms (36% of cases) and low prevalence of motor symptoms (3% of cases). We did not find FUS mutations in any aFTLD-U case. To date, the only subtype of cases reported to have ubiquitin-positive but tau-, TDP-43- and FUS-negative pathology, termed FTLD-UPS, is the result of charged multivesicular body protein 2B gene (CHMP2B) mutation. We identified three FTLD-UPS cases, which are negative for CHMP2B mutation, suggesting that the full complement of FTLD pathologies is yet to be elucidated
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