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3. Dabrafenib and trametinib exposure-efficacy and tolerance in metastatic melanoma patients: a pharmacokinetic–pharmacodynamic real-life study

Author

L.-T. Vu, Barouyr Baroudjian, Céleste Lebbé, L. Goldwirt, Clara Allayous, Julie Delyon, L. Da Meda, Florian Herms, Fanélie Jouenne, Baptiste Louveau, Samia Mourah, and H. Sauvageon

Subjects
Adult, Male, Proto-Oncogene Proteins B-raf, 0301 basic medicine, Oncology, Cancer Research, medicine.medical_specialty, Pyridones, Pyrimidinones, Toxicology, 03 medical and health sciences, 0302 clinical medicine, Pharmacokinetics, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Oximes, Humans, Medicine, Pharmacology (medical), Prospective Studies, Stage (cooking), Adverse effect, Melanoma, Neoplasm Staging, Pharmacology, Trametinib, Univariate analysis, medicine.diagnostic_test, business.industry, Imidazoles, Bayes Theorem, Dabrafenib, Middle Aged, medicine.disease, Progression-Free Survival, Treatment Outcome, 030104 developmental biology, Therapeutic drug monitoring, Area Under Curve, 030220 oncology & carcinogenesis, Mutation, Female, Drug Monitoring, business, medicine.drug
Abstract

Dabrafenib plus trametinib combination has greatly improved survival in BRAFV600mut metastatic melanoma patients. However, data regarding the influence of pharmacokinetic markers in real-life patients are lacking. In this study, we aimed to explore dabrafenib and trametinib pharmacokinetic impact on progression-free survival (PFS), duration of response (DOR) or all grades treatment-related adverse events (ARAE) occurrence in routine care patients. BRAFV600mut metastatic melanoma patients initiating standard doses of dabrafenib 150 mg BID plus trametinib 2 mg QD were included. Clinical data were collected via the French biobank MelBase, prospectively enrolling unresectable stage III or IV melanoma. Clinical response evaluation, ARAE reporting and dabrafenib and trametinib plasma quantification were performed. Association of individual Bayesian-estimated pharmacokinetic markers (AUC0–τ and Ctrough) and baseline clinical variables with DOR, PFS, clinical response, and ARAE was then assessed. Fifty patients (comprising 4 AJCC stage IIIc and 46 stage IV) were included. Median PFS reached 11.4 months, and overall response rate 70%. Fifty percent of patients experienced ARAE (G3 n = 10, G4 n = 0). In univariate analysis, median dabrafenib Ctrough within intermediate range was associated with a significantly higher PFS (HR [95% CI] = 0.41 [0.18; 0.91], p = 0.029) and DOR (HR [95% CI] = 0.39 [0.16; 0.94], p = 0.024), and association with DOR remained significant in multivariate analysis (HR [95% CI] = 0.34 [0.12; 0.95], p = 0.040). Trametinib pharmacokinetic markers were significantly higher in patients experiencing ARAE compared to patients without ARAE. In this study, exposure-efficacy and tolerance analysis highlighted the interest of therapeutic drug monitoring to optimize therapeutic management in BRAFV600mut metastatic melanoma patients based on trough concentrations of dabrafenib and trametinib.

Published
2021
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4. Impact des inhibiteurs de checkpoints immunitaires au cours de la COVID-19 chez les patients atteints de mélanome

Author

Aurélien Corneau, Selim Aractingi, Ludivine Grzelak, Timothée Bruel, P. Tetu, Jérôme Hadjadj, Catherine Blanc, Nikaïa Smith, L. Da Meda, C. Lebbé, Benjamin Terrier, J. Le Goff, Olivier Schwartz, Clara Allayous, J. Boussier, Nader Yatim, Isabelle Staropoli, Frédéric Rieux-Laucat, Darragh Duffy, and Nora Kramkimel

Subjects
Gynecology, 2019-20 coronavirus outbreak, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), Co018, business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Gastroenterology, Internal Medicine, medicine, business
Abstract

Introduction La restauration immunitaire induite par les inhibiteurs de checkpoints immunitaires ont révolutionné le pronostic des cancers métastatiques [1]. La contribution de cette stratégie thérapeutique pour la prise en charge des infections reste toutefois controversée, malgré quelques études en faveur de leur utilisation, notamment dans le contexte de paralysie immunitaire au décours d’un sepsis sévère [2], [3], ou dans les situations d’épuisement immunitaire au cours des infections virales chroniques [4], [5]. Au cours de la COVID-19, des études suggèrent qu’un état d’épuisement immunitaire en lien avec une anergie et/ou une déplétion des lymphocytes T serait partiellement responsable de la virulence du SARS-CoV-2 [6], [7], [8], [9], [10]. Certains proposent donc l’utilisation des anti-PD1 comme stratégie thérapeutique tandis que d’autres suggèrent qu’au contraire, elle pourrait aggraver l’hyperinflammation [11], [12]. Patients et méthodes Nous avons suivi de façon prospective 292 patients atteints de mélanome lors de la première vague de COVID-19 (de mars à juin 2020) dont la moitié était traitée par immunothérapie (anti-PD1 ± anti-CTLA4). Les patients présentant des symptômes de COVID-19 étaient dépistés par PCR. Une sérologie SARS-CoV-2 était recherchée de façon systématique. Les patients présentant une infection symptomatique active ( 21 jours du début des symptômes, PCR négative, sérologie positive) ont été inclus pour une étude approfondie de la réponse immunitaire par une analyse transcriptionnelle (Nanostring), protéomique (SIMOA, Luminex) et cellulaire (cytométrie de masse). Résultats Quinze patients atteints de COVID-19 ont été identifiés (infection active ou convalescente) avec une estimation de la séroprévalence à 8,6 % de la cohorte. Quatre patients sur 15 ont nécessité une hospitalisation (26,7 %). Les données cliniques ne retrouvaient pas d’éléments en faveur d’une forme plus sévère de COVID-19 lors d’un traitement par anti-PD1, seul un patient ayant également une leucémie lymphoïde chronique, a développé une forme sévère de la COVID-19 et est décédé de défaillance respiratoire. L’analyse de la réponse immunitaire, en comparaison avec une cohorte de patients non traités par immunothérapie, retrouvait une réponse immunitaire innée semblable dans les deux cohortes. De même, le taux d’anticorps anti-Spike (IgG et IgA), la capacité neutralisante ainsi que la longévité des anticorps (suivi du taux sur une période d’1 an) étaient similaires en présence ou non d’un traitement par immunothérapie. En revanche, l’analyse de la réponse cellulaire mettait en évidence, chez les patients traités par immunothérapie, une expansion de la population de lymphocytes T CD8+ effecteurs mémoires, une augmentation de l’activation des lymphocytes T CD4+ et CD8+, et une augmentation la production d’IFN-gamma lors d’une stimulation ex-vivo par des peptides issus du SARS-CoV-2. Conclusion Nos résultats sont en faveur d’une augmentation de la réponse cellulaire T anti-SARS-CoV-2 lors d’un traitement par anti-PD1 chez les patients suivis pour mélanome, et de l’absence d’une exacerbation de la réponse inflammatoire. Il est nécessaire de confirmer ces résultats avec un plus grand nombre de patients, dans d’autres types de cancers et dans d’autres centres.

Published
2021

5. Développement d’un panel « Next Generation Sequencing » ciblé en vue d’améliorer la prise en charge des patients atteints de mélanome

Author

Marisa Battistella, L. Da Meda, A. Lermine, Kevin Serror, P. Tetu, Barouyr Baroudjian, Aurélie Sadoux, E. Lopes, Aurélia Gruber, A. Ndiaye, O. Marco, Samia Mourah, Céleste Lebbé, Julie Delyon, Fanélie Jouenne, Baptiste Louveau, and Nicolas Dumaz

Subjects
Dermatology
Abstract

Introduction Les analyses de genetique somatique sont desormais essentielles dans la prise en charge des patients cancereux. Dans le melanome, ces analyses se sont longtemps limitees a l’etude du codon 600 de BRAF, maintenant elargies a une approche « next generation sequencing » (NGS) ciblant plusieurs genes. Des panels NGS pan-cancer ont ainsi ete implementes mais, dans un contexte de medecine personnalisee et de resistance aux therapies, des panels specifiques a chaque pathologie et ciblant ses genes d’interet, sont necessaires. Notre but est de mettre en evidence l’interet clinique d’un tel panel dans le melanome. Materiel et methodes Les patients atteints de melanome chez lesquels un screening moleculaire tumoral initial a ete realise entre juin 2017 et aout 2019 dans le cadre de leur prise en charge clinique de routine ont ete inclus dans cette etude retrospective. Les analyses moleculaires ont ete realisees a l’aide d’un panel NGS de 64 genes d’interet dans le melanome, detectant a la fois variants nucleotidiques (SNV) et variations du nombre de copies (CNV). Ces genes ont ete selectionnes sur la base de leur implication dans la classification moleculaire, le pronostic, le theranostique et la resistance aux traitements. Une analyse comprehensive a ete realisee afin de mettre en evidence les alterations d’interet clinique majeur. Resultats Au total, 421 cas de melanome, dont 240 primitifs et 172 metastases (9 indetermines), ont ete analyses. Apres filtrage bio-informatique selectionnant les alterations potentiellement impactantes, 561 SNVs, 164 CNVs (96 amplifications et 68 deletions) et 4 mutations au site d’epissage ont ete mis en evidence. 87,4 % (368/421) des lesions presentaient au moins une alteration et les genes les plus frequemment alteres etaient : BRAF (192 SNVs et 20 CNVs), NRAS (114 SNVs), CDKN2A (60 CNVs et 2 mutations au site d’epissage), CCND1 (20 CNVs) et MET (16 CNVs). Parmi les patients BRAFV600 mutes, 44,5 % (77/173) presentaient au moins une alteration concomitante pouvant entrainer une resistance aux inhibiteurs de MAPK. Parmi les patients avec une mutation RAS hotspot et les patients sans mutation hotspot de BRAFV600 ni RAS, 56,9 % (66/116) et 47,7 % (63/132) respectivement possedaient une alteration constituant une cible therapeutique alternative potentielle. Discussion Notre panel NGS, couple a une analyse comprehensive des alterations detectees, represente un atout important pour la prise en charge des patients atteints de melanomes. Applique a une cohorte de 421 patients, il nous a permis de definir un paysage exhaustif des alterations somatiques dans les melanomes primitifs et metastatiques, et de mettre en evidence les profils moleculaires de resistance aux inhibiteurs de MAPK ainsi que de nouvelles pistes de therapies alternatives pour une proportion importante de patients.

Published
2020
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6. Essai de phase 2 multicentrique évaluant le pembrolizumab dans la maladie de Kaposi classique ou endémique

Author

Vincent Allain, L. Toullec, V. Heidelberger, Guislaine Carcelain, L. Da Meda, Matthieu Resche-Rigon, Stéphane Dalle, J. Le Goff, Sophie Caillat-Zucman, Samia Mourah, C. Lebbé, Marisa Battistella, M. Renaud, and Julie Delyon

Subjects
Dermatology
Abstract

Introduction Alors que le traitement de la maladie de Kaposi (MK) iatrogenique et epidemique est relativement bien codifie, reposant avant tout sur une restauration des fonctions immunitaires, le traitement optimal de la MK classique/endemique reste a definir. Les patients avec atteinte cutanee etendue ou viscerale sont traites generalement par interferon ou chimiotherapie, mais la tolerance peut etre mediocre chez des sujets souvent âges, et les remissions a long terme sont rares. Les anti-PD1 ont fait preuve d’une efficacite spectaculaire dans de nombreux cancers dont le carcinome de Merkel, une tumeur viro-induite comme la MK, notamment mediee par l’immunogenicite des antigenes associes au virus. Compte tenu de l’implication du virus HHV8 dans la MK et de la bonne tolerance des anti-PD1 chez les sujets âges, les anti-PD1 apparaissent comme une option therapeutique interessante. Materiel et methodes Nous avons conduit un essai de phase 2 multicentrique incluant les patients atteints de MK classique/endemique avec atteinte cutanee etendue, evolutive, avec indication a un traitement systemique. Les patients etaient traites par pembrolizumab 200 mg/3 semaines IV pendant 6 mois. La reponse tumorale etait evaluee par une mesure clinique des lesions cibles (nombre, taille, infiltration, couleur) suivant les criteres ACTG pour definir la meilleure reponse dans les 6 mois (critere principal). Une probabilite de reponse > 30 % suivant le plan de Simon en 2 etapes permettait de conclure a l’efficacite. Resultats Dix-sept patients ont ete inclus (47 % et 53 % de MK classique et endemique), dont 6 avec une atteinte ganglionnaire associee. Une majorite (12, 71 %) avait deja recu de la chimiotherapie. Avec une mediane de suivi de 25 semaines, 2 patients etaient en reponse complete, 10 en reponse partielle, et 5 en stabilite comme meilleure reponse. Onze patients ont eu ≥ 1 effet secondaire lie au traitement dont 1 de grade 3 (œdeme aigu pulmonaire, OAP). Deux patients ont arrete prematurement pour toxicite (un OAP grade 3 sans myocardite et une pancreatite aigue grade 2, traites symptomatiquement, reversibles). Sur les biopsies initiales, l’absence d’expression de PDL1 sur les cellules tumorales et immunes etait associee a la non reponse au pembrolizumab. Le score de divergence entre alleles du HLA de classe 1 a ete mesure chez chaque patient, et etait significativement plus faible chez les 5 patients non repondeurs (p = 0,031). Discussion Dans ce premier essai clinique evaluant l’efficacite d’un anti-PD1 dans la MK classique/endemique, le pembrolizumab etait efficace (taux de reponse de 71 %) et la tolerance acceptable. Si confirmes, ces resultats suggerent que les anti-PD1 pourraient rapidement devenir un traitement systemique de premier plan dans cette indication.

Published
2020
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7. 1077MO PD1 blockade with pembrolizumab in classic and endemic Kaposi sarcoma: A multicenter phase II study

Author

L. Da Meda, M. Renaud, Marisa Battistella, Julie Delyon, Guislaine Carcelain, Samia Mourah, Matthieu Resche-Rigon, V. Heidelberger, Sophie Caillat-Zucman, Vincent Allain, L. Toullec, J. Le Goff, Stéphane Dalle, and C. Lebbé

Subjects
Oncology, medicine.medical_specialty, business.industry, Internal medicine, Phases of clinical research, Medicine, Hematology, Sarcoma, Pembrolizumab, business, medicine.disease, Blockade
Published
2020
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8. Étude de phase I-II multicentrique en ouvert évaluant le palbociclib en association au vémurafénib chez des patients atteints d’un mélanome métastatique BRAFV600 muté avec perte de CDKN2A et expression de RB1

Author

Thierry Lesimple, Mona Amini-Adle, Baptiste Louveau, Samuel Huguet, Didier Bouton, Barouyr Baroudjian, Marisa Battistella, Matthieu Resche-Rigon, Caroline Dutriaux, Samia Mourah, Annick Tibi, Zineb Ghrieb, K. Reizai, L. Da Meda, Julie Delyon, Fanélie Jouenne, Marc Pracht, and C. Lebbé

Subjects
Dermatology
Abstract

Introduction Parmi les mecanismes de resistance aux inhibiteurs de BRAF (iBRAF), les effecteurs du cycle cellulaire, notamment CDK4, sont impliques dans la reactivation de ERK. Dans cette etude de phase I-II multicentrique en ouvert, notre but etait d’etablir la Dose Maximale Toleree (DMT) du palbociclib (PB), un inhibiteur de CDK4/6, en association au vemurafenib (VM) chez les patients atteints de melanome metastatique et porteurs d’une mutation BRAFV600 ( NCT02202200 ). Materiel et methodes Les patients atteints d’un melanome metastatique mutes BRAFV600E/K presentant une perte de CDKN2A et une expression de RB1 ont ete inclus et ont recu des cycles de 21 jours de traitement associant : 1) une administration quotidienne de PB pendant 21 jours et 2) une administration biquotidienne de VM durant les 14 premiers jours du cycle. Les patients ont ete stratifies en 2 groupes selon la prise anterieure d’un traitement par iBRAF (Non : groupe 1 ; Oui : groupe 2). Les posologies de PB (mg/QD)/VM (mg/BID) allaient de 25/720 a 200/960. Le critere principal etait la survenue d’une toxicite limitant la dose au cours des deux premiers cycles de traitement. Les criteres secondaires comprenaient la meilleure reponse observee (RECIST v1.1), la survie globale (SG), la survie sans progression (SSP), les parametres pharmacocinetiques, le profil moleculaire tumoral initial (analyse transcriptomique). Resultats Dix-huit patients ont ete inclus, dont 15 (83 %) dans le groupe 2. Les principales caracteristiques a l’inclusion etaient : sexe masculin : 11 (61 %), âge median : 55 ans, melanome de stade IIIC non resecable : 2 (11 %), melanome de stade IV : 16 (89 %). Trois (17 %) patients presentaient des metastases cerebrales et 9 (50 %) un niveau de LDH eleve a l’inclusion. Le delai median entre le diagnostic de melanome et l’inclusion etait de 24,5 mois. Une DLT a ete observee pour 1 et 5 patients dans les groupes 1 et 2 respectivement definissant la DMT PB/VM a 25 mg/960 mg dans le groupe 2. Aucune interaction medicamenteuse significative entre PB et VM n’a ete mise en evidence. Dans le groupe 2, 4 (27 %) patients ont presente une reponse clinique et 8 (53 %) patients une maladie stable. La SSP mediane etait de 4,3 mois et la SG mediane de 19,9 mois. L’analyse transcriptomique initiale a revele un taux d’alteration eleve associe a la reponse clinique et un enrichissement des genes impliques dans les voies de la MAP-Kinase, du cycle cellulaire et de l’apoptose. Conclusion L’association au VM n’a pas permis d’augmenter la dose fixe de PB au-dessus de 25 mg. Cependant, un benefice clinique a ete observe chez les patients pretraites et l’analyse moleculaire sur les lesions a l’inclusion a revele une association entre les donnees transcriptomiques et la reponse clinique.

Published
2019
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9. Long-term outcome of neoadjuvant tyrosine kinase inhibitors (TKI) in locally advanced dermatofibrosarcoma protuberans (DFSP)

Author

L. Da Meda, Cécile Farges, Nicole Basset-Seguin, Marisa Battistella, C. Le Maignan, Delphine Kerob, J. Beaziz, Barouyr Baroudjian, Julie Delyon, C. Lebbé, O. Marco, and C Pages Laurent

Subjects
medicine.medical_specialty, medicine.diagnostic_test, business.industry, Retrospective cohort study, Hematology, Neutropenia, medicine.disease, Surgery, Metastasis, Pazopanib, Imatinib mesylate, Oncology, Biopsy, Dermatofibrosarcoma protuberans, medicine, Clinical endpoint, business, medicine.drug
Abstract

Background Imatinib mesylate is approved in unresectable tumors and has been also proposed in the neoadjuvant setting in order to reduce tumor size and post-operative relapses for difficult to resect DFSP. The aim of this study was to evaluate the long-term results of neoadjuvant imatinib and other TKI used in DFSP. Methods The files of all patients with the following criteria seen from 2007 to 2017 in our center were collected in this retrospective study: a/histologically proven primary or recurrent DFSP with COL1A1-PDGFB translocation b/ difficult to treat but surgically manageable as assessed in pluridisciplinary tumor board, c/received first-line neoadjuvant TKI (imatinib, pazopanib). The primary endpoint was long-term progression-free survival (PFS). Results 27 patients (median 42 years, range: 18-63) were included, of whom 9 (33%) had fibrosarcomatous transformation on pre-TKI biopsy. 10 patients had primary tumors and 17 presented recurrences. Median tumor size was 6 cm (range 3-30). 24 patients received imatinib (median dose= 600mg/day), 3 received pazopanib (median dose= 600mg/day) for a median of 7 months. The best MRI response to ITK treatment before surgery according to RECIST1.1 consisted of complete/partial response (33%) or stability (48%). DFSP was surgically removed in 24 patients (89%) after a median of 7 months and 2 surgeries. Two patients (7%) did not receive surgery because of metastasis progression. One other patient declined surgery. 23 of 24 patients surgically treated were disease-free after 50 months of median follow-up (range 10-133). One patient developed distant metastasis 37 months after the complete surgical resection. The median PFS was 44 months (range 10-133).The histological response localization was mainly patchy (n = 10) or diffuse (n = 7). The median percentage of therapeutic response surface was 65%.Treatment-related adverse events occurred in 23 patients (85%). 4 patients had grade 3 or higher toxicities (2 grade 3 and 4 neutropenia, 1 grade 3 cholestasis, 1 grade 3 nausea) requiring temporary treatment disruption and dose reductions. Conclusions TKI are effective neoadjuvant treatment for locally advanced or inoperable DFSP with long-term PFS and few severe adverse events. Legal entity responsible for the study The authors. Funding Has not received any funding. Disclosure All authors have declared no conflicts of interest.

Published
2019
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10. Étude rétrospective de l’incidence et du risque de diabète de type 1 et 2 chez les sujets traités par anti PD-1 pour un mélanome métastatique

Author

L. Da-Meda, Tiphaine Vidal-Trecan, Matthieu Resche-Rigon, Barouyr Baroudjian, Isabelle Madelaine-Chambrin, Sylvine Pinel, Martine Bagot, Céleste Lebbé, C. Pages, Philippe Boudou, Samia Mourah, Marie-Léa Gauci, Pirayeh Eftekhari, Pauline Laly, and Jean-François Gautier

Subjects
Dermatology
Abstract

Introduction Les anti-PD-1 connus pour augmenter la survie sans progression et la survie globale des sujets traites pour un melanome localement avance ou metastatique induisent des effets secondaires auto-immuns, dont le diabete de type 1 (DT1). Ils sont egalement responsables de l’augmentation de la secretion de cytokines pro-inflammatoires pouvant contribuer a la genese du diabete de type 2 (DT2). Materiel et methodes Une etude retrospective observationnelle a ete menee a l’hopital Saint-Louis entre iuillet 2014 et juin 2016, chez des sujets traites par anti PD-1 pour un melanome. La survenue d’un DT1 a ete definie par l’apparition de symptomes d’hyperglycemie, la presence d’anticorps (Ac) diriges contre la cellule β pancreatique et/ou un peptide C indetectable. L’evolution « ad random » de la glycemie (G) et de la CRP a ete appreciee avant (AV) et apres (AP) traitement. L’HbA1c en fin de traitement et 3 mois plus tot a ete mesuree. Les cas de pre-diabete (PD) ont ete definis selon les criteres de l’ADA. La base nationale de pharmacovigilance (BNPV) a ete interrogee le 26 decembre 2016 sur les cas de DT1 declares aux centres regionaux de pharmacovigilance. Resultats Cent trente deux sujets ont fait l’objet d’un recueil de donnees ; 119 ont ete inclus. Trois sujets ont developpe un DT1. L’evolution des parametres biologiques a ete analysee. Parmi les 116 autres patients traites, la G et l’HbA1c ne variaient pas significativement au cours du traitement : G (mmol/L) mediane 5,46 (q1 :4,95 ;q3 :6,07) AV vs 5,52 (q1 :4,98 ; q3 :6,44) AP traitement ; mediane d’HbA1c 5,3 % (q1 :5,1 ;q3 :5,6) en fin de traitement vs 5,3 % (q1 :5,1 ;q3 :5,55) 3 mois plus tot. 6 cas de PD ont ete reveles et un cas de DT2 est apparu apres 39 mois de traitement. Une augmentation de 44 % de la CRP (mg/l) a ete constatee (moyenne : 21,54 AV vs 31,08 AP traitement ; p = 0,016 ; mediane : 5 (q1 :2 ;q3 :18) AV vs 5 (q1 :0 ;q3 :21,75) AP traitement. Le sous-groupe de sujets ayant recu precedemment ( n = 45) ou concomitamment ( n = 8) un anti-CTLA-4 presentait une augmentation significative de la G (mmol/L) mediane : 5,1 (q1 :5,001-q3 :5,57) AV vs 5,68 (q1 :5,16–q3 :6,81) AP traitement ; p = 0,0003. 15 cas de DT1 ont ete enregistres dans la BNPV. Conclusion La survenue de cas de DT1 sous anti-PD1 est de plus en plus rapportee mais leur frequence reste faible. La valeur predictive de la positivite des auto-Ac sur la survenue du DT1 AV administration des anti-PD-1 est inconnue. Notre etude montre que ce traitement entraine une augmentation des marqueurs de l’inflammation (CRP), n’a pas d’incidence sur l’HbA1 C ou la G lorsque la duree de traitement est relativement courte mais pourrait, a long terme, avoir une incidence sur la survenue d’un PD ou d’un DT2. Cependant, le profil glycemique semble significativement affecte chez les sujets prealablement traites par anti-CTLA-4. D’autres etudes seront necessaires pour comprendre l’implication de PD-1 dans le DT2.

Published
2017
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11. Diabète de type 1 (DT1) révélé par une acidocétose sous anti-PD1

Author

Marie-Léa Gauci, Barouyr Baroudjian, J.F. Gautier, Nicole Basset-Seguin, I. Madelaine, J. Gottlieb, Pauline Laly, Martine Bagot, L. Da Meda, N. Madjlessi-Ezra, C. Pages, Philippe Boudou, and C. Lebbé

Subjects
030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, Dermatology
Abstract

Introduction Les anticorps anti-PD1, approuves dans le traitement du melanome metastatique, permettent d’atteindre une mediane de survie superieure a 24 mois. Leurs principaux effets secondaires sont des maladies auto-immunes. Nous decrivons un cas de DT1 sous nivolumab. Observations Un homme de 73 ans, sans antecedents (notamment metabolique), sauf une dyslipidemie, etait traite par nivolumab 3 mg/kg/2 semaines (dans le cadre de l’AMM) pour un melanome metastatique mute BRAF, apres echec de 3 mois d’association de vemurafenib et cobimetinib. Il avait recu en 2011, apres l’exerese d’un melanome SSM dorsal de 2,62 mm de Breslow, de l’interferon α a visee adjuvante, declarant alors une maladie de Basedow (actuellement en remission). A six semaines de traitement, il se plaignait brutalement de douleurs abdominales, vomissements et d’un syndrome polyuro-polydipsique. Resultats La glycemie etait a 27,78 mmol/l (patient normoglycemique jusque la) et la bandelette urinaire retrouvait trois croix de cetone et de glucose. Une insulinotherapie permettait la normalisation de la glycemie et la disparition des symptomes. L’HbA1c etait a 7,2 % puis a 8,8 % trois semaines plus tard temoignant d’une augmentation explosive de la glycemie et un controle difficile du diabete. Le peptide C etait effondre (insulinorequerance) (Fig. 1). L’exploration biologique retrospective sur serotheque montrait une positivite des auto-anticorps lors de la declaration du diabete mais aussi anterieure (J0 et 3 mois avant le debut de nivolumab) (Fig. 2). La reevaluation a trois mois montrait une reponse therapeutique, motivant la poursuite du nivolumab a la meme dose . Discussion Le contexte clinique, les investigations biologiques avant, au moment et apres mise sous nivolumab traduisent l’origine auto-immune de la maladie diabetique induite fort probablement par l’anti-PD1 chez un patient predispose. Dix cas de DT1 sous anti-PD1 ont ete decrits dans la litterature avec une presentation clinique similaire dont un cas a montre une reversibilite du processus auto-immun. Nous montrons pour la premiere fois un suivi retrospectif et prospectif du profil metabolique et auto-immun d’un patient declarant un diabete sous anti-PD1. La presence de ces auto-anticorps chez notre patient avant l’introduction du nivolumab est a rapprocher de la situation observee au cours du DT1 de l’enfant ; ils traduisent un etat pathologique infraclinique dit de prediabete chez des sujets predisposes. Conclusion Nous decrivons un nouveau cas de DT1 avec exploration metabolique et auto-immune permettant d’expliquer la genese de la maladie sous anti-PD1. Bien que rare, cet effet secondaire doit etre connu et la glycemie monitoree sous immunotherapie. La recherche des auto-anticorps pourrait permettre de depister les patients a risque a l’introduction de l’immunotherapie et de mieux les surveiller.

Published
2016
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12. Premier cas de myopathie nécrosante focale (MNF) responsable d’un syndrome de la tête tombante (STT) sous cobimétinib

Author

Céleste Lebbé, Anthony Behin, Pauline Laly, Marie-Léa Gauci, L. Da Meda, J. Gottlieb, Marisa Battistella, Nicole Basset-Seguin, Barouyr Baroudjian, S. Léonard-Louis, I. Madelaine, T. Maisonobe, Laetitia Vercellino, C. Pages, and Samia Mourah

Subjects
Dermatology
Abstract

Introduction En 5 annees, la mediane de survie du melanome metastatique a ete multipliee par trois grâce aux therapies ciblees et aux immunotherapies. La mutation NRAS constitue une cible therapeutique prometteuse des inhibiteurs de MEK (MEKi) et les perspectives therapeutiques orientent vers des associations entre immunotherapie et therapies ciblees. L’augmentation asymptomatique du taux de CPK a ete decrite sous MEKi. Nous decrivons un cas de myopathie necrosante focale (MNF) avec syndrome de la tete tombante (STT) induite par un MEKi, le cobimetinib. Observations Un homme de 72 ans souffrant d’une maladie de Parkinson controlee etait traite en 3e ligne par nivolumab 3 mg/kg toutes les deux semaines apres echec de la dacarbazine et de l’ipilimumab, pour un melanome metastatique mute NRAS. Apres 10 mois de traitement, nous observions un echappement modere motivant l’introduction, validee en RCP, du cobimetinib 60 mg/jour 21 sur 28 jours associe au nivolumab. A 1 mois de l’introduction du MEKi, il presentait une douleur interscapulaire, une fatigabilite axiale a la marche avec anteflexion de la nuque et difficulte a relever la tete. Resultats Il existait un deficit moteur isole aux muscles extenseurs cervicaux a 4/5, hypermetaboliques sur la TEP/TDM sans metastase associee (Fig. 1) et une augmentation des CPK a 1011 U/l (N Discussion Le STT, caracterise par une faiblesse des muscles extenseurs de la nuque responsable d’une cyphose cervicale et l’impossibilite de relever la tete, a pour principales etiologies les myopathies, la myasthenie et la maladie de Parkinson. Des cas de myopathie necrosante sous anti-PD1 ont ete rapportes mais du fait des donnees anatomocliniques le nivolumab ne pouvait pas etre impute. Trois cas similaires de STT ont ete decrits sous un MEKi, le selumetinib. Via le mode d’action du MEKi, cette necrose serait plutot de mecanisme toxique qu’immunomediee (comme pour les statines), MEK jouant aussi bien un role dans la proliferation cellulaire que dans la consommation des acides gras par la cellule musculaire. Le STT est retrouve chez 6 % des Parkinsoniens, ce qui constitue un biais. La cinetique d’evolution clinicobiologique et les donnees de la litterature suggerent que le terrain du patient peut avoir joue un role favorisant mais n’est pas la cause de la MNF. Conclusion Il s’agit du premier cas de MNF avec STT sous cobimetinib. Cette toxicite merite une attention particuliere en raison de la clinique stereotypee et de l’augmentation de prescription des therapies ciblees.

Published
2016
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14. MelBase, constitution et suivi d’une cohorte nationale de patients atteints de mélanome stade III inopérable ou stade IV avec collection d’une base de données clinico-biologiques

Author

Laurent Mortier, C. Dutriaux, S. Dalle, M. Barthelemy, J. Benessiano, P. Saiag, M.-T. Leccia, Thierry Lesimple, C. Lebbé, Raphaël Porcher, L. Demerville, L. Da Meda, P. Efthekary, E. Liegey, A. Dupuy, B. Dréno, Clara Allayous, Philippe Bahadoran, and E. Stoebner

Subjects
Dermatology
Abstract

Introduction Les avancees majeures dans le pronostic et le traitement du melanome metastatique imposent aujourd’hui d’associer des etudes clinico-epidemiologiques et biologiques. Il apparait ainsi indispensable de s’appuyer sur une base nationale clinico-biologique, MelBase pour evaluer l’interet therapeutique, la toxicite et l’impact medico-economique. Observations A l’initiative du groupe de cancerologie cutanee, et grâce au soutien de l’INCa et de divers partenaires industriels, la base clinico-biologique nationale MelBase a ete creee, avec comme gestionnaire le Departement de la Recherche Clinique et du Developpement. Il s’agit d’une cohorte prospective, multicentrique, incluant des patients majeurs, ayant donne leur consentement eclaire et presentant un melanome de stade IIIC inoperable ou IV, naifs de tout traitement systemique non adjuvant. Un dossier technico-reglementaire a ete constitue et valide par les autorites sanitaires (avis favorable du CPP, du CCTIRS et de la CNIL). Tous les centres participants ont signe une charte de gouvernance. Resultats Les inclusions ont debute en mars 2013 et actuellement 234 patients ont ete inclus dans 24 centres francais (23 CHU et 1 CLCC), tous adosses a un CRB. Cette base nationale active prevoit un recrutement sur 2 ans et un suivi pendant 3 ans. Sont collectees de facon anonyme dans un eCRF des donnees cliniques, a savoir, les caracteristiques des patients, de leur pathologie, les differentes lignes de traitement, les toxicites et tout autre cancer secondaire survenu. A cela s’ajoutent des donnees de couts medico-economiques et des questionnaires de qualite de vie. La collection biologique est composee d’une part d’echantillons tumoraux collectes dans le cadre du soin (melanome ou tout autre type de cancer). Et d’autre part, des echantillons sanguins (ADN, ARN, plasma, serum) realises a l’inclusion, puis tous les 6 mois et a chaque changement therapeutique. Un monitoring a distance est effectue. Discussion Des partenariats publics et prives sont en cours et MelBase est interconnectee a la base nationale CeNGEPS. Des interactions avec d’autres bases nationales europeennes sont en discussion. Conclusion MelBase montre la faisabilite de constituer des biobanques dans des maladies ou des therapies innovantes, mais couteuses, voient le jour. Soutenue par l’INCa et des partenariats publics et prives, l’exploitation de cette base nationale devrait permettre d’identifier de nouveaux marqueurs pronostiques et predictifs d’efficacite et de toxicite des schemas therapeutiques utilises. Le benefice risque et l’impact sur la qualite de vie des traitements autorises et en cours de validation seront egalement evaluable.

Published
2014
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16. Genomic profiling of a skin adnexal carcinomas cohort using a comprehensive high-throughput sequencing approach.

Author

Louveau B, Nakouri I, Jouenne F, Baroudjian B, Sadoux A, Da Meda L, Osio A, Reinhart F, Robert J, Herms F, Cribier B, Mortier L, Jouary T, Basset Seguin N, Lebbé C, Mourah S, and Battistella M

Subjects
Humans, Female, Male, Middle Aged, Carcinoma, Skin Appendage genetics, Carcinoma, Skin Appendage pathology, Carcinoma, Skin Appendage diagnosis, Aged, Mutation, Genomics methods, High-Throughput Nucleotide Sequencing, Skin Neoplasms genetics, Skin Neoplasms pathology
Abstract

Competing Interests: Conflicts of interest CL declares consulting and advisory fees from BMS, MSD, Pierre Fabre and Sanofi. SM declares consulting and advisory fees from Novartis and Roche, and research funding from Biocartis. The other authors declare no conflicts of interest.

Published
2024
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17. Effectiveness and safety of major systemic treatments in classic and endemic Kaposi sarcoma: a multicentre retrospective study of 110 patients.

Author

Grolleau C, Walter-Petrich A, Dupin N, Chanal J, Zehou O, Montlahuc C, Baroudjian B, Da Meda L, Resche-Rigon M, Le Cleach L, and Lebbé C

Subjects
Humans, Retrospective Studies, Sarcoma, Kaposi epidemiology, Skin Neoplasms therapy
Abstract

Competing Interests: Conflicts of interest C.L. declares financial interests with Amgen, Bristol Myers Squibb, Merck Serono, MSD, Novartis, Pierre Fabre and Roche.

Published
2024
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18. Combined PDE4+MEK inhibition shows antiproliferative effects in NRASQ61 mutated melanoma preclinical models.

Author

Louveau B, Reger De Moura C, Jouenne F, Sadoux A, Allayous C, Da Meda L, Bernard-Cacciarella M, Baroudjian B, Lebbé C, Mourah S, and Dumaz N

Subjects
Animals, Humans, Dimethyl Sulfoxide, Disease Models, Animal, Mitogen-Activated Protein Kinase Kinases, MAP Kinase Kinase Kinases metabolism, Melanoma drug therapy, Melanoma genetics, Skin Neoplasms
Abstract

Upregulation of phosphodiesterase type 4 (PDE4) has been associated with worse prognosis in several cancers. In melanomas harboring NRAS mutations, PDE4 upregulation has been shown to trigger a switch in signaling from BRAF to RAF1 which leads to mitogen-activated protein kinase pathway activation. Previous in vitro evidence showed that PDE4 inhibition induced death in NRASQ61mut melanoma cells and such a strategy may thus be a relevant therapeutic option in those cases with no molecular targeted therapies approved to date. In this study, we generated patient-derived xenografts (PDX) from two NRASQ61mut melanoma lesions. We performed ex vivo histoculture drug response assays and in vivo experiments. A significant ex vivo inhibition of proliferation with the combination of roflumilast+cobimetinib was observed compared to dimethyl sulfoxide control in both models (51 and 67%). This antiproliferative effect was confirmed in vivo for PDX-1 with a 56% inhibition of tumor growth. To decipher molecular mechanisms underlying this effect, we performed transcriptomic analyses and revealed a decrease in MKI67, RAF1 and CCND1 expression under bitherapy. Our findings strengthen the therapeutic interest of PDE4 inhibitors and support further experiments to evaluate this approach in metastatic melanoma., (Copyright © 2023 Wolters Kluwer Health, Inc. All rights reserved.)

Published
2024
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19. Durability of response to immune checkpoint inhibitors in metastatic Merkel cell carcinoma after treatment cessation.

Author

Weppler AM, Da Meda L, Pires da Silva I, Xu W, Grignani G, Menzies AM, Carlino MS, Long GV, Lo SN, Nordman I, Steer CB, Lyle M, Trojaniello C, Ascierto PA, Lebbe C, and Sandhu S

Subjects
Humans, Immune Checkpoint Inhibitors adverse effects, Progression-Free Survival, Withholding Treatment, Retrospective Studies, Carcinoma, Merkel Cell drug therapy, Carcinoma, Merkel Cell pathology, Skin Neoplasms drug therapy, Skin Neoplasms pathology
Abstract

Background: Metastatic Merkel cell carcinoma (mMCC) is highly responsive to immune checkpoint inhibitors (ICIs); however, durability of response after treatment cessation and response to retreatment in the setting of progression is unknown., Methods: Patients (pts) having mMCC from 10 centres who discontinued ICI treatment for a reason other than progression were studied., Results: Forty patients were included. Median time on treatment was 13.5 months (range 1-35). Thirty-one patients (77.5%) stopped treatment electively while 9 patients (22.5%) stopped due to treatment-related toxicity. After median of 12.3 months from discontinuation, 14 pts (35%) have progressed (PD). Disease progression rate following ICI discontinuation was 26% (8 of 31) in patients who discontinued in complete response (CR), 57% (4 of 7) in patients in partial response and 100% (2 of 2) in those with stable disease. Median progression-free survival (PFS) after treatment cessation was 21 months (95% confidence interval [CI], 18- not reached [NR]), with a third of patients progressing during their first year off treatment. PFS was longer for patients who discontinued ICI electively (median PFS 29 months; 95% CI, 21-NR) compared to those who stopped due to toxicity (median PFS 11 months; 95% CI, 10-NR). ICI was restarted in 8 of 14 pts (57%) with PD, with response rate of 75% (4 CR, 2 partial response, 1 stable disease, 1 PD)., Conclusion: ICI responses in mMCC do not appear durable off treatment, including in patients who achieve a CR, though response to retreatment is promising. Extended duration of treatment needs to be investigated to optimise long-term outcomes., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published
2023
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20. Telomere-Associated Changes in Nuclear Architecture of Cancer-Associated Macrophage-like Cells in Liquid Biopsies from Melanoma Patients.

Author

Rangel-Pozzo A, Wechsler J, Groult J, Da Meda L, Lebbe C, and Mai S

Abstract

During phagocytosis, tumor-associated macrophages (TAMs) can incorporate genetic material from tumor cells. The incorporation of extra genetic material may be responsible for advanced malignant behavior observed in some TAMs, making TAMs potentially important players in cancer progression. More recently, similar cells were described in the blood as cancer-associated macrophage-like cells (CAMLs). CAMLs may be equivalent to TAMs cells in the blood, and they express macrophage markers. However, their origin is still unclear. In a previous study, we showed for the first time the distinct telomere 3D structure of circulating tumor cells (CTCs) in melanoma and other cancers. In the present pilot study, we investigated, comparatively, the 3D telomere structure of CAMLs, CTCs and leucocytes from nine melanoma patients with metastatic cutaneous melanoma stage IV. CTC capture was performed by size-based filtration followed by cytological and immunocytological evaluation. Three-dimensional Quantitative Fluorescent in situ Hybridization was performed to measure differences in five 3D telomere parameters. Telomere parameters, such as number, length, telomere aggregates, nuclear volume, and a / c ratio, were compared among different cellular types (CTCs, CAMLs, and normal leucocytes). Three telomere parameters were significantly different between CAMLs and leucocytes. The combination of two telomere parameters (telomere length against the number of telomeres) resulted in the identification of two CAMLs subpopulations with different levels of genomic instability. Those populations were classified as profile 1 and 2. Profile 2, characterized by a high number of short telomeres, was observed in four of the nine melanoma patients. To our knowledge, this is the first pilot study to investigate 3D telomere parameters as hallmarks of nuclear architecture in CAMLs' population in comparison to leucocytes from the same patient. Further studies involving a larger patient sample size are necessary to validate these findings and explore their potential prognostic value.

Published
2022
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21. 18FDG PET Assessment of Therapeutic Response in Patients with Advanced or Metastatic Melanoma Treated with First-Line Immune Checkpoint Inhibitors.

Author

Rivas A, Delyon J, Martineau A, Blanc E, Allayous C, Da Meda L, Merlet P, Lebbé C, Baroudjian B, and Vercellino L

Abstract

Background: Immune checkpoint inhibitors (ICI) are currently the first-line treatment for patients with metastatic melanoma. We investigated the value of positron emission tomography (PET) response criteria to assess the therapeutic response to first-line ICI in this clinical context and explore the potential contribution of total tumor metabolic volume (TMTV) analysis., Methods: We conducted a retrospective study in patients treated with first-line ICI for advanced or metastatic melanoma, with 18F-FDG PET/CT performed at baseline and 3 months after starting treatment. Patients' metabolic response was classified according to PERCIST5 and imPERCIST 5 criteria. TMTV was recorded for each examination., Results: Twenty-nine patients were included. The median overall survival (OS) was 51.2 months (IQR 13.6-not reached), and the OS rate at 2 years was 58.6%. Patients classified as responders (complete and partial response) had a 90.9% 2-year OS rate versus 38.9% for non-responders (stable disease and progressive disease) ( p = 0.03), for PERCIST5 and imPERCIST 5 criteria. The median change in metabolic volume was 9.8% (IQR -59-+140%). No significant correlation between OS and changes in TMTV was found., Conclusion: The evaluation of response to immunotherapy using metabolic imaging with PERCIST5 and imPERCIST5 was significantly associated with OS in patients with advanced or metastatic melanoma.

Published
2022
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22. PD-1 blockade with pembrolizumab in classic or endemic Kaposi's sarcoma: a multicentre, single-arm, phase 2 study.

Author

Delyon J, Biard L, Renaud M, Resche-Rigon M, Le Goff J, Dalle S, Heidelberger V, Da Meda L, Toullec L, Carcelain G, Mourah S, Caillat-Zucman S, Allain V, Battistella M, and Lebbe C

Subjects
Adolescent, Adult, Antibodies, Monoclonal, Humanized adverse effects, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Humans, Programmed Cell Death 1 Receptor, Prospective Studies, Sarcoma, Kaposi drug therapy, Sarcoma, Kaposi etiology
Abstract

Background: Although the treatment of iatrogenic and HIV-related Kaposi sarcoma is well defined and mostly based on restoring immune function, the treatment of classic and endemic Kaposi sarcoma is less well established. Chemotherapy or interferon α is used for patients with extensive cutaneous or visceral Kaposi sarcoma, but tolerance might be poor and long-term remission is rare. We aimed to evaluate the activity of pembrolizumab in classic and endemic Kaposi sarcoma with cutaneous extension requiring systemic treatment., Methods: We did a multicentre, single-arm, proof-of-concept, phase 2 trial in adults aged 18 years or older with histologically proven classic or endemic Kaposi's sarcoma with progressive cutaneous extension requiring systemic treatment and an Eastern Cooperative Oncology Group performance status of 0-1 in three hospitals in France. The patients were treated with 200 mg pembrolizumab intravenously every 3 weeks for 6 months (eight cycles) or until severe toxicity. The primary endpoint was the best overall response rate within the 6-month timeframe, defined by the occurrence of a complete response or partial response and assessed by an investigator using the modified AIDS Clinical Trial Group (ACTG) criteria. Three or more responses among a total 17 patients were needed for the primary endpoint to be met, using a Simon's two-stage optimal design assuming a 30% response rate as desirable. For this final study analysis, all patients were included following the intention-to-treat principle. This study is registered with ClinicalTrials.gov, NCT03469804, and is closed to new participants., Findings: 30 patients were screened for eligibility and 17 patients (eight [47%] with classic and nine [53%] with endemic Kaposi's sarcoma) were enrolled between July 2, 2018, and Dec 16, 2019. The median follow-up was 20·4 months (IQR 18·1-24·1). Two (12%) patients had a complete response, ten (59%) had a partial response, and five (29%) had stable disease as the best response within the 6-month treatment timeframe, with a best overall response rate of 71% (95% CI 44-90), meeting the predefined primary outcome (ie, exceeding a response rate of 30%). Treatment-related adverse events occurred in 13 (76%) of 17 patients, including two grade 3 adverse events (one [6%] acute cardiac decompensation and one [6%] granulomatous reaction). Treatment was prematurely discontinued in two (12%) patients due to grade 3 acute reversible cardiac decompensation and grade 2 pancreatitis, and one other patient had a grade 3 granulomatous reaction in mediastinal lymph nodes requiring steroids and methotrexate treatment. There were no serious adverse events or treatment-related deaths., Interpretation: In this prospective trial, which to our knowledge is the first to assess the role of PD-1 blockade in patients with classic and endemic Kaposi's sarcoma, pembrolizumab showed promising anti-tumour activity with an acceptable safety profile. If this result is supported by further studies, treatment with anti-PD-1 could be part of the therapeutic armamentarium for patients with classic and endemic Kaposi's sarcoma., Funding: MSD France., Competing Interests: Declarations of interests JD reports support for travel or accommodation from Pierre Fabre and Roche; research funding from Merck Sharpe and Dohme and Amgen; and honoraria from Bristol Myers Squibb. SD reports institutional research grants from and travel costs covered by Bristol Myers Squibb and Merck Sharpe and Dohme. VH reports support for attending meetings from Merck Sharpe and Dohme. SM reports a consulting role for and research funding from Novartis, Bristol Myers Squibb, Biocartis, and Roche. VA reports support for attending meetings from Bediagenomics. MB reports board member fees from Bristol Myers Squibb; travel expenses from Roche; research grants from Takeda; expert consultancy for Innate Pharma and Kyowa Kirin; and speaker board fees from Kyowa Kirin. CL reports research funding from Roche and Bristol Myers Squibb; consulting fees from Bristol Myers Squibb, Merck Sharpe and Dohme, Novartis, Amgen, Roche, Merck Serono, Sanofi, and Pierre Fabre; honoraria from Roche, Bristol Myers Squibb, Novartis, Amgen, Merck Sharpe and Dohme, Pierre Fabre, Pfizer, and Incyte; fees for speaker's bureau from Roche, Bristol Myers Squibb, Novartis, Amgen, and Merck Sharpe and Dohme; support for attending meetings from Bristol Myers Squibb, Merck Sharpe and Dohme, Novartis, Sanofi, and Pierre Fabre; and fees from Avantis Medical Systems. All other authors declare no competing interests., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published
2022
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23. Dabrafenib and trametinib exposure-efficacy and tolerance in metastatic melanoma patients: a pharmacokinetic-pharmacodynamic real-life study.

Author

Goldwirt L, Louveau B, Baroudjian B, Allayous C, Jouenne F, Da Meda L, Vu LT, Sauvageon H, Herms F, Delyon J, Lebbé C, and Mourah S

Subjects
Adult, Antineoplastic Combined Chemotherapy Protocols adverse effects, Antineoplastic Combined Chemotherapy Protocols pharmacokinetics, Area Under Curve, Bayes Theorem, Drug Monitoring methods, Female, Humans, Imidazoles administration & dosage, Male, Melanoma genetics, Melanoma pathology, Middle Aged, Mutation, Neoplasm Staging, Oximes administration & dosage, Progression-Free Survival, Prospective Studies, Pyridones administration & dosage, Pyrimidinones administration & dosage, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Melanoma drug therapy, Proto-Oncogene Proteins B-raf genetics
Abstract

Purpose: Dabrafenib plus trametinib combination has greatly improved survival in BRAFV600 mut metastatic melanoma patients. However, data regarding the influence of pharmacokinetic markers in real-life patients are lacking. In this study, we aimed to explore dabrafenib and trametinib pharmacokinetic impact on progression-free survival (PFS), duration of response (DOR) or all grades treatment-related adverse events (ARAE) occurrence in routine care patients., Methods: BRAFV600 mut metastatic melanoma patients initiating standard doses of dabrafenib 150 mg BID plus trametinib 2 mg QD were included. Clinical data were collected via the French biobank MelBase, prospectively enrolling unresectable stage III or IV melanoma. Clinical response evaluation, ARAE reporting and dabrafenib and trametinib plasma quantification were performed. Association of individual Bayesian-estimated pharmacokinetic markers (AUC 0-τ and C trough ) and baseline clinical variables with DOR, PFS, clinical response, and ARAE was then assessed., Results: Fifty patients (comprising 4 AJCC stage IIIc and 46 stage IV) were included. Median PFS reached 11.4 months, and overall response rate 70%. Fifty percent of patients experienced ARAE (G3 n = 10, G4 n = 0). In univariate analysis, median dabrafenib C trough within intermediate range was associated with a significantly higher PFS (HR [95% CI] = 0.41 [0.18; 0.91], p = 0.029) and DOR (HR [95% CI] = 0.39 [0.16; 0.94], p = 0.024), and association with DOR remained significant in multivariate analysis (HR [95% CI] = 0.34 [0.12; 0.95], p = 0.040). Trametinib pharmacokinetic markers were significantly higher in patients experiencing ARAE compared to patients without ARAE., Conclusion: In this study, exposure-efficacy and tolerance analysis highlighted the interest of therapeutic drug monitoring to optimize therapeutic management in BRAFV600 mut metastatic melanoma patients based on trough concentrations of dabrafenib and trametinib., (© 2021. The Author(s), under exclusive licence to Springer-Verlag GmbH Germany, part of Springer Nature.)

Published
2021
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24. Immune checkpoint inhibitors increase T cell immunity during SARS-CoV-2 infection.

Author

Yatim N, Boussier J, Tetu P, Smith N, Bruel T, Charbit B, Barnabei L, Corneau A, Da Meda L, Allayous C, Baroudjian B, Jebali M, Herms F, Grzelak L, Staropoli I, Calmettes V, Hadjadj J, Peyrony O, Cassius C, LeGoff J, Kramkimel N, Aractingi S, Fontes M, Blanc C, Rieux-Laucat F, Schwartz O, Terrier B, Duffy D, and Lebbé C

Subjects
Adaptive Immunity drug effects, Adaptive Immunity immunology, Aged, Antibodies, Viral immunology, CD8-Positive T-Lymphocytes drug effects, CD8-Positive T-Lymphocytes immunology, CD8-Positive T-Lymphocytes virology, COVID-19 complications, COVID-19 virology, Female, Humans, Immune Checkpoint Inhibitors therapeutic use, Immunologic Memory drug effects, Immunologic Memory immunology, Lymphocyte Activation drug effects, Lymphocyte Activation immunology, Male, Melanoma complications, Melanoma drug therapy, Middle Aged, Prospective Studies, SARS-CoV-2 metabolism, SARS-CoV-2 physiology, Spike Glycoprotein, Coronavirus immunology, Spike Glycoprotein, Coronavirus metabolism, T-Lymphocytes drug effects, T-Lymphocytes virology, COVID-19 immunology, Immune Checkpoint Inhibitors immunology, Melanoma immunology, SARS-CoV-2 immunology, T-Lymphocytes immunology
Abstract

The COVID-19 pandemic has spread worldwide, yet the role of antiviral T cell immunity during infection and the contribution of immune checkpoints remain unclear. By prospectively following a cohort of 292 patients with melanoma, half of which treated with immune checkpoint inhibitors (ICIs), we identified 15 patients with acute or convalescent COVID-19 and investigated their transcriptomic, proteomic, and cellular profiles. We found that ICI treatment was not associated with severe COVID-19 and did not alter the induction of inflammatory and type I interferon responses. In-depth phenotyping demonstrated expansion of CD8 effector memory T cells, enhanced T cell activation, and impaired plasmablast induction in ICI-treated COVID-19 patients. The evaluation of specific adaptive immunity in convalescent patients showed higher spike (S), nucleoprotein (N), and membrane (M) antigen-specific T cell responses and similar induction of spike-specific antibody responses. Our findings provide evidence that ICI during COVID-19 enhanced T cell immunity without exacerbating inflammation., (Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works. Distributed under a Creative Commons Attribution License 4.0 (CC BY).)

Published
2021
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25. Phase I-II Open-Label Multicenter Study of Palbociclib + Vemurafenib in BRAF V600MUT Metastatic Melanoma Patients: Uncovering CHEK2 as a Major Response Mechanism.

Author

Louveau B, Resche-Rigon M, Lesimple T, Da Meda L, Pracht M, Baroudjian B, Delyon J, Amini-Adle M, Dutriaux C, Reger de Moura C, Sadoux A, Jouenne F, Ghrieb Z, Vilquin P, Bouton D, Tibi A, Huguet S, Rezai K, Battistella M, Mourah S, and Lebbe C

Subjects
Adult, Female, Humans, Male, Melanoma secondary, Middle Aged, Skin Neoplasms pathology, Treatment Outcome, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Checkpoint Kinase 2 physiology, Melanoma drug therapy, Melanoma genetics, Piperazines administration & dosage, Proto-Oncogene Proteins B-raf genetics, Pyridines administration & dosage, Skin Neoplasms drug therapy, Skin Neoplasms genetics, Vemurafenib administration & dosage
Abstract

Purpose: In BRAF V600MUT metastatic melanoma, cyclin D-CDK4/6-INK4-Rb pathway alterations are involved in resistance to MAPK inhibitors, suggesting a clinical benefit of cyclin-dependent kinase 4 (CDK4) inhibitors. In this phase I-II study, we aimed to establish the MTD of palbociclib when added to vemurafenib., Patients and Methods: Patients with BRAF V600E/KMUT metastatic melanoma harboring CDKN2A loss and RB1 expression were included and stratified into two groups according to previous BRAF inhibitor treatment (no:strata 1; yes:strata 2). Treatment comprised palbociclib once daily for 14 days followed by a 7-day break + continuous dosing of vemurafenib. The primary endpoint was the occurrence of dose-limiting toxicity (DLT), and the secondary endpoints included the best response, survival, pharmacokinetics, and tumor molecular profiling., Results: Eighteen patients were enrolled, with 15 in strata 2. Characteristics at inclusion were American Joint Committee on Cancer stage IVM1c ( N = 16; 88.9%), high lactate dehydrogenase ( N = 9; 50.0%), and median number of previous treatments of 2. One and 5 patients experienced DLT in strata 1 and 2, respectively, defining the MTD at palbociclib 25 mg and vemurafenib 960 mg in strata 2. No significant evidence for drug-drug interactions was highlighted. The median progression-free survival was 2.8 months, and 5 (27.8%) patients showed a clinical response. The baseline differential mRNA expression analysis and in vitro data revealed the role of CHEK2 in the response to palbociclib., Conclusions: Although the combination of palbociclib + fixed-dose vemurafenib did not allow an increased palbociclib dosage above 25 mg, a significant clinical benefit was achieved in pretreated patients with melanoma. An association between the transcriptomic data and clinical response was highlighted., (©2021 American Association for Cancer Research.)

Published
2021
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26. Long-Term Outcome of Neoadjuvant Tyrosine Kinase Inhibitors Followed by Complete Surgery in Locally Advanced Dermatofibrosarcoma Protuberans.

Author

Beaziz J, Battistella M, Delyon J, Farges C, Marco O, Pages C, Le Maignan C, Da Meda L, Basset-Seguin N, Resche-Rigon M, Walter Petrich A, Kérob D, Lebbé C, and Baroudjian B

Abstract

In locally advanced dermatofibrosarcoma protuberans (DFSP), imatinib mesylate has been described as an efficient neoadjuvant therapy. This retrospective study included patients with locally advanced DFSP who received neoadjuvant TKI (imatinib or pazopanib) from 2007 to 2017 at Saint Louis Hospital, Paris. The primary endpoint was the evaluation of the long-term status. A total of 27 patients were included, of whom nine had fibrosarcomatous transformation. The median duration of treatment was 7 months. The best response to TKI treatment before surgery, evaluated according to RECIST1.1 on MRI, consisted of complete/partial response (38.5%) or stability (46.2%). DFSP was surgically removed in 24 (89%) patients. A total of 23 patients (85%) were disease-free after 64.8 months of median follow-up (95% confidence interval 47.8; 109.3). One patient developed distant metastases 37 months after surgical tumor resection and finally died. Two patients (7%) did not get surgery because of metastatic progression during TKI treatment, and one patient refused surgery even though the tumor decreased by 30%. Treatment-related adverse events (AE) occurred in 23 patients (85%). Only four patients (imatinib: n = 3, pazopanib: n = 1) had grade ≥3 AE requiring temporary treatment disruption. Neoadjuvant TKI followed by complete surgery with micrographic analysis is an effective strategy for locally advanced and unresectable DFSP, with durable local recurrence disease-free survival.

Published
2021
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27. A Multicenter Phase II Study of Pazopanib in Patients with Unresectable Dermatofibrosarcoma Protuberans.

Author

Delyon J, Porcher R, Battistella M, Meyer N, Adamski H, Bertucci F, Guillot B, Jouary T, Leccia MT, Dalac S, Mortier L, Ghrieb Z, Da Meda L, Vicaut E, Pedeutour F, Mourah S, and Lebbe C

Subjects
Adult, Aged, Biomarkers, Tumor antagonists & inhibitors, Biomarkers, Tumor genetics, Dermatofibrosarcoma genetics, Dermatofibrosarcoma pathology, Drug Resistance, Neoplasm genetics, Epidermal Growth Factor genetics, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Humans, Indazoles adverse effects, Male, Middle Aged, Protein Kinase Inhibitors adverse effects, Pyrimidines adverse effects, Response Evaluation Criteria in Solid Tumors, Skin drug effects, Skin pathology, Skin Neoplasms genetics, Skin Neoplasms pathology, Sulfonamides adverse effects, Tumor Burden drug effects, Dermatofibrosarcoma drug therapy, Indazoles administration & dosage, Protein Kinase Inhibitors administration & dosage, Pyrimidines administration & dosage, Skin Neoplasms drug therapy, Sulfonamides administration & dosage
Abstract

Dermatofibrosarcoma protuberans (DFSP) is a soft-tissue sarcoma characterized by a high risk of local infiltration. The identification of the COL1A1-PDGFB t(17;22) translocation activating the PDGF pathway led to the use of imatinib in unresectable DFSP, with a response rate of 36-80%. Pazopanib is a multitarget tyrosine kinase inhibitor approved for soft-tissue sarcomas. We conducted a phase II study of patients with unresectable DFSP to evaluate the efficacy and safety of pazopanib. Patients received 800 mg of pazopanib daily. The primary endpoint was the objective response rate defined as the reduction of the largest diameter of the tumor by ≥30% at 6 months or at surgery. A total of 23 patients, including one pretreated with imatinib, were enrolled. With a median follow-up of 6.2 months (interquartile range = 5.6-7.8 months), five patients (22%, 95% confidence interval = 7-22%) had a partial response to pazopanib. The best objective response rate was 30% (95% confidence interval = 13-53%) using Response Evaluation Criteria in Solid Tumors. One patient with metastatic DFSP previously treated with imatinib died after 2.4 months. Nine patients (39%) discontinued the treatment owing to adverse events. Pharmacodynamics analyses of tumor samples were conducted: the enrichment of EGF and the EGFR-associated gene panel was associated with resistance, suggesting that EGFR-targeted therapies could be a therapeutic option to explore in DFSP. TRIAL REGISTRATION: ClinicalTrials.gov identifier: NCT01059656., (Copyright © 2021 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2021
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28. A Melanoma-Tailored Next-Generation Sequencing Panel Coupled with a Comprehensive Analysis to Improve Routine Melanoma Genotyping.

Author

Louveau B, Jouenne F, Têtu P, Sadoux A, Gruber A, Lopes E, Delyon J, Serror K, Marco O, Da Meda L, Ndiaye A, Lermine A, Dumaz N, Battistella M, Baroudjian B, Lebbe C, and Mourah S

Subjects
Female, Genotype, Humans, Male, Melanoma pathology, High-Throughput Nucleotide Sequencing methods, Melanoma genetics
Abstract

Background: Tumor molecular deciphering is crucial in clinical management. Pan-cancer next-generation sequencing panels have moved towards exhaustive molecular characterization. However, because of treatment resistance and the growing emergence of pharmacological targets, tumor-specific customized panels are needed to guide therapeutic strategies., Objective: The objective of this study was to present such a customized next-generation sequencing panel in melanoma., Methods: Melanoma patients with somatic molecular profiling performed as part of routine care were included. High-throughput sequencing was performed with a melanoma tailored next-generation sequencing panel of 64 genes involved in molecular classification, prognosis, theranostic, and therapeutic resistance. Single nucleotide variants and copy number variations were screened, and a comprehensive molecular analysis identified clinically relevant alterations., Results: Four hundred and twenty-one melanoma cases were analyzed (before any treatment initiation for 94.8% of patients). After bioinformatic prioritization, we uncovered 561 single nucleotide variants, 164 copy number variations, and four splice-site mutations. At least one alteration was detected in 368 (87.4%) lesions, with BRAF, NRAS, CDKN2A, CCND1, and MET as the most frequently altered genes. Among patients with BRAFV600 mutated melanoma, 44.5% (77 of 173) harbored at least one concurrent alteration driving potential resistance to mitogen-activated protein kinase inhibitors. In patients with RAS hotspot mutated lesions and in patients with neither BRAFV600 nor RAS hotspot mutations, alterations constituting potential pharmacological targets were found in 56.9% (66 of 116) and 47.7% (63 of 132) of cases, respectively., Conclusions: Our tailored next-generation sequencing assay coupled with a comprehensive analysis may improve therapeutic management in a significant number of patients with melanoma. Updating such a panel and implementing multi-omic approaches will further enhance patients' clinical management.

Published
2020
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29. Baseline Genomic Features in BRAFV600 -Mutated Metastatic Melanoma Patients Treated with BRAF Inhibitor + MEK Inhibitor in Routine Care.

Author

Louveau B, Jouenne F, Reger de Moura C, Sadoux A, Baroudjian B, Delyon J, Herms F, De Masson A, Da Meda L, Battistella M, Dumaz N, Lebbe C, and Mourah S

Abstract

In BRAF V600mut metastatic melanoma, the combination of BRAF and MEK inhibitors (BRAFi, MEKi) has undergone multiple resistance mechanisms, limiting its clinical benefit and resulting in the need for response predicting biomarkers. Based on phase III clinical trial data, several studies have previously explored baseline genomic features associated with response to BRAFi + MEKi. Using a targeted approach that combines the examination of mRNA expression and DNA alterations in a subset of genes, we performed an analysis of baseline genomic alterations involved in MAPK inhibitors' resistance in a real-life cohort of BRAF V600mut metastatic melanoma patients. Twenty-seven patients were included in this retrospective study, and tumor samples were analyzed when the BRAFi + MEKi therapy was initiated. The clinical characteristics of our cohort were consistent with previously published studies. The BRAFi + MEKi treatment was initiated in seven patients as a following-line treatment, and had a specific transcriptomic profile exhibiting 14 genes with lower mRNA expression. However, DNA alterations in CCND1 , RB1 , and MET were only observed in patients who received BRAFi + MEKi as the first-line treatment. Furthermore, KIT mRNA expression was significantly higher in patients showing clinical benefit from the combined therapy, emphasizing the tumor-suppressor role of KIT already described within the context of BRAF -mutant melanoma.

Published
2019
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30. Occurrence of type 1 and type 2 diabetes in patients treated with immunotherapy (anti-PD-1 and/or anti-CTLA-4) for metastatic melanoma: a retrospective study.

Author

Gauci ML, Boudou P, Baroudjian B, Vidal-Trecan T, Da Meda L, Madelaine-Chambrin I, Basset-Seguin N, Bagot M, Pages C, Mourah S, Resche-Rigon M, Pinel S, Sassier M, Rouby F, Eftekhari P, Lebbé C, and Gautier JF

Subjects
Adult, Aged, Aged, 80 and over, CTLA-4 Antigen immunology, Diabetes Mellitus, Type 1 chemically induced, Diabetes Mellitus, Type 2 chemically induced, Female, Follow-Up Studies, France epidemiology, Humans, Incidence, Male, Melanoma secondary, Middle Aged, Prognosis, Programmed Cell Death 1 Receptor immunology, Retrospective Studies, Antibodies, Monoclonal adverse effects, CTLA-4 Antigen antagonists & inhibitors, Diabetes Mellitus, Type 1 epidemiology, Diabetes Mellitus, Type 2 epidemiology, Immunotherapy adverse effects, Melanoma drug therapy, Programmed Cell Death 1 Receptor antagonists & inhibitors
Abstract

Anti-PD-1 and anti-CTLA-4 antibodies cause immune-related side effects such as autoimmune type 1 diabetes (T1D). It has also been suggested that by increasing TNF-α, IL-2 and IFN-γ production, anti-PD-1 and/or anti-CTLA-4 treatment could affect pancreatic beta cell function and insulin sensitivity. This study was based on a retrospective observational analysis from 2 July 2014 to 27 June 2016, which evaluated the occurrence of T1D and changes in glycemia and C-reactive protein (CRP) plasma concentrations in patients undergoing anti-PD-1 and/or anti-CTLA-4 treatment for melanoma at the Saint Louis Hospital. All cases of T1D that developed during immunotherapy registered in the French Pharmacovigilance Database (FPVD) were also considered. Among the 132 patients included, 3 cases of T1D occurred. For the remaining subjects, blood glucose was not significantly affected by anti-PD-1 treatment, but CRP levels (mg/l) significantly increased during anti-PD-1 treatment (p = 0.017). However, 1 case of type 2 diabetes (T2D) occurred (associated with a longer therapy duration). Moreover, glycemia of patients pretreated (n = 44) or concomitantly treated (n = 8) with anti-CTLA-4 tended to increase during anti-PD-1 therapy (p = 0.068). From the FPVD, we obtained 14 cases of T1D that occurred during immunotherapy and were primarily characterized by the rapidity and severity of onset. In conclusion, in addition to inducing this rare immune-related diabetes condition, anti-PD-1 treatment appears to increase CRP levels, a potential inflammatory trigger of insulin resistance, but without any short-term impact on blood glucose level.

Published
2018
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31. Autoimmune diabetes induced by PD-1 inhibitor-retrospective analysis and pathogenesis: a case report and literature review.

Author

Gauci ML, Laly P, Vidal-Trecan T, Baroudjian B, Gottlieb J, Madjlessi-Ezra N, Da Meda L, Madelaine-Chambrin I, Bagot M, Basset-Seguin N, Pages C, Mourah S, Boudou P, Lebbé C, and Gautier JF

Subjects
Aged, Antibodies, Monoclonal immunology, Autoantibodies blood, Autoantibodies immunology, Humans, Male, Nivolumab, Programmed Cell Death 1 Receptor immunology, Retrospective Studies, Antibodies, Monoclonal adverse effects, Diabetes Mellitus, Type 1 chemically induced, Melanoma drug therapy, Skin Neoplasms drug therapy
Abstract

Anti-PD-1 antibody treatment is approved in advanced melanoma and provides median overall survival over 24 months. The main treatment-related side effects are immune-related adverse events, which include rash, pruritus, vitiligo, thyroiditis, diarrhoea, hepatitis and pneumonitis. We report a case of autoimmune diabetes related to nivolumab treatment. A 73-year-old man was treated in second line with nivolumab at 3 mg/kg every two weeks for metastatic melanoma. At 6 weeks of treatment, he displayed diabetic ketoacidosis. Nivolumab was withheld 3.5 weeks and insulin therapy was initiated, enabling a normalization of glycaemia and the disappearance of symptoms. Laboratory investigations demonstrated the presence of islet cell autoantibodies, while C-peptide was undetectable. Retrospective explorations on serum banked at week 0 and 3 months before the start of nivolumab, already showed the presence of autoantibodies, but normal insulin, C-peptide secretion and glycaemia. Partial response was obtained at month 3, and nivolumab was then resumed at the same dose. The clinical context and biological investigations before, at and after nivolumab initiation suggest the autoimmune origin of this diabetes, most likely induced by anti-PD-1 antibody in a predisposed patient. The role of PD-1/PD-L1 binding is well known in the pathogenesis of type 1 diabetes. Therefore, this rare side effect can be expected in a context of anti-PD-1 treatment. Glycaemia should be monitored during PD-1/PD-L1 blockade. The presence of autoantibodies before treatment could identify individuals at risk of developing diabetes, but systematic titration may not be relevant considering the rarity of this side effect.

Published
2017
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32. Remitting seronegative symmetrical synovitis with pitting edema (RS3PE) syndrome induced by nivolumab.

Author

Gauci ML, Baroudjian B, Laly P, Madelaine I, Da Meda L, Vercellino L, Bagot M, Lioté F, Pages C, and Lebbé C

Subjects
Adrenal Cortex Hormones therapeutic use, Aged, 80 and over, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents therapeutic use, Edema drug therapy, Humans, Male, Melanoma drug therapy, Nivolumab, Skin Neoplasms drug therapy, Syndrome, Synovitis drug therapy, Treatment Outcome, Antibodies, Monoclonal adverse effects, Antineoplastic Agents adverse effects, Edema chemically induced, Synovitis chemically induced
Abstract

Introduction: A new articular syndrome described as immunrelated side effect of immunotherapy: PD-1 inhibitors have revolutionized the treatment of advanced melanoma but are responsible for immune-related toxicity. We report a case of remitting seronegative symetrical synovitis with pitting edema (RS3PE) syndrome induced by nivolumab., Case Report: A 80 year-old man with stage IV BRAF-wild type and NRAS exon 2-mutated melanoma was treated first line by nivolumab 3mg/kg every 2 weeks. At week 4, before the 3rd infusion, he presented with inflammatory arthralgia, synovitis of proximal interphalangeal, wrist and ankle joints, and edema of both hands and forearms. Laboratory tests showed inflammatory syndrome (CRP = 8.4mg/dL), negative rheumatoid factor, and anti-CCP antibodies. Radiographs did not show any joint erosion but joint ultrasound displayed intra-articular effusion and tenosynovitis. PET/CT performed 6 and 3 months before treatment for melanoma work-up showed an isolated hypermetabolism of the shoulder girdle. The diagnosis of RS3PE was retained. A systemic corticosteroid treatment (0.5mg/kg/d) was initiated; nivolumab was hold during 4 weeks leading to remission of clinical symptoms within 10 days, CRP level normalization and without relapse when nivolumab was resumed. Corticosteroids were progressively tapered and stopped after 9 months. After 5 months, anti-PD1 was definitively stopped because of disease progression., Conclusion: With this atypical case, clinicians should remain alert on a whole range of autoimmune diseases susceptible to be induced., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published
2017
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33. Focal necrotizing myopathy with 'dropped-head syndrome' induced by cobimetinib in metastatic melanoma.

Author

Gauci ML, Laly P, Leonard-Louis S, Behin A, Gottlieb J, Madelaine-Chambrin I, Baroudjian B, Da-Meda L, Mourah S, Battistella M, Basset-Seguin N, Bagot M, Pages C, Vercellino L, Maisonobe T, and Lebbé C

Subjects
Aged, Azetidines pharmacology, Humans, MAP Kinase Kinase 1 pharmacology, Male, Melanoma pathology, Muscular Diseases pathology, Piperidines pharmacology, Skin Neoplasms pathology, Azetidines adverse effects, MAP Kinase Kinase 1 adverse effects, Melanoma complications, Muscular Diseases etiology, Piperidines adverse effects, Skin Neoplasms complications
Abstract

Therapeutic advances derived from targeted therapy and immune checkpoint inhibitors can improve melanoma prognosis. Since 2015, cobimetinib has been approved in combination with vemurafenib in the first-line treatment for BRAF-mutated melanoma. For NRAS-mutated melanomas, MEK inhibition seems to be a therapeutic target, and association with checkpoint inhibitor provides a further therapeutic perspective. Infraclinical creatine phosphokinase (CPK) elevation is an MEK inhibitor side effect. We describe a case of focal necrotizing myopathy with 'dropped-head syndrome' induced by cobimetinib, 1 month after its introduction. The clinical presentation comprised interscapular pain, axial fatigue with cervical hypotonia, CPK elevation, intense fluorine-18-fluorodeoxyglucose uptake in cervical muscles, and necrotizing myopathy was confirmed by muscle biopsy. Cobimetinib was temporarily discontinued, resulting in CPK normalization. Re-evaluation showed partial response, motivating continuation of combination therapy with a reduced dose of cobimetinib (40 mg/day). Because prescription of targeted therapies is likely to increase, this adverse event should be known.

Published
2017
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34. Clinical value of early detection of circulating tumour DNA- BRAF V600mut in patients with metastatic melanoma treated with a BRAF inhibitor.

Author

Louveau B, Tost J, Mauger F, Sadoux A, Podgorniak MP, How-Kit A, Pages C, Roux J, Da Meda L, Lebbe C, and Mourah S

Abstract

Competing Interests: Competing interests: CL declares honoraria from Roche, advisory roles at Roche, GSK, Novartis, BMS, MSD and Amgen, and travel accommodation provided by Roche. SM declares a consulting role at Roche and Novartis.

Published
2017
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