Your search keyword '"Lanoy E"' showing total 304 results

101. C38 - Syndrome de Kaposi-Juliusberg de l’enfant : étude rétrospective de 38 cas

Author

Bourdon-Lanoy, E., primary, Barbarot, S., additional, Hadj-Rabia, S., additional, Tesici, A., additional, Hamel, D., additional, De Prost, Y., additional, and Bodemer, C., additional

Published

2005

102. P176 - Cellulite de Wells compliquant une primo infection à parvovirus B19

Author

Toulon, A., primary, Bourdon-Lanoy, E., additional, Hadj-Rabia, S., additional, Leruez-Ville, M., additional, Fraitag, S., additional, Bodemer, C., additional, De Prost, Y., additional, and Hamel, D., additional

Published

2005

103. C84 - Étude des urgences en dermatologie libérale (et.u.de) : analyse descriptive

Author

Penso-Assathiany, D., primary, Derancourt, C., additional, Bourdon-Lanoy, E., additional, Roujeau, J-C., additional, and Bastuji-Garin, S., additional

Published

2005

104. C79 - Connaissance et respect des mesures de photoprotection à une consultation d’oncologie dermatologique

Author

Meyer, N., primary, Pruvost-Balland, C., additional, Bourdon-Lanoy, E., additional, and Avril, M-F., additional

Published

2005

105. P165 - Duplication digestive kystique du plancher buccal chez un nouveau-né

Author

Grandpeix, C., primary, Manach, Y., additional, Brunelle, F., additional, Hadj-Rabia, S., additional, Bourdon-Lanoy, E., additional, Bodemer, C., additional, De Prost, Y., additional, and Hamel-Teillac, D., additional

Published

2005

106. Pemphigoïde du sujet jeune

Author

Bourdon-Lanoy, E., primary, Roujeau, J.-C., additional, Joly, P., additional, Guillaume, J.-C., additional, Bernard, P., additional, Prost, C., additional, Tancrède-Bohin, E., additional, Delaporte, E., additional, Picard-Dahan, C., additional, Albes, B., additional, Bedane, C., additional, Doutre, M.-S., additional, Chosidow, O., additional, Lok, C., additional, Pauwels, C., additional, Chevrand-Breton, J., additional, Sassolas, B., additional, and Richard, M.-A., additional

Published

2005

107. 1331TiP - Phase I Study of Tremelimumab (Trem) in Combination with Gefitinib (Gef) in Epidermal Growth Factor Receptor Mutant (Egfr-Mut) Non-Small Cell Lung Cancer (Nsclc)

Author

Planchard, D., Chaput-Gras, N., Barlesi, F., Mazieres, J., Byrne, N., Vuillier, D., Lacroix, L., Besse, B., Lanoy, E., Wunder, F., Jannin, C., Malekzadeh, K., Ngocamus, M., Nash, A., Di Pietro, A., and Soria, J-C

Published

2014

108. 826P - Contribution of Tumor Burden and Body Composition Parameters As Prognostic Factors of Metastatic Renal Cell Carcinoma (Mrcc) Treated By Targeted Therapy

Author

Lanoy, E., Antoun, S., Iacovelli, R., Loriot, Y., Merad, M., Massard, C., Fizazi, K., Dipalma, M., and Escudier, B.

Published

2014

109. Survival after neuroAIDS: association with antiretroviral CNS Penetration-Effectiveness score.

Author

Lanoy E, Guiguet M, Bentata M, Rouveix E, Dhiver C, Poizot-Martin I, Costagliola D, Gasnault J, and FHDH-ANRS CO4

Published

2011

110. CEMARA an information system for rare diseases.

Author

Landais P, Messiaen C, Rath A, Le Mignot L, Dufour E, Ben Said M, Jais J, Toubiana L, Baujat G, Bourdon-Lanoy E, Gérard-Blanluet M, Bodemer C, Salomon R, Aymé S, Le Merrer M, Verloes A, CEMARA Task Force, Safran C, Reti S, and Marin H

Published

2010

111. eHealth beyond the horizon -- get IT there. CEMARA: a Web dynamic application within a n-tier architecture for rare diseases.

Author

Messiaen C, Le Mignot L, Rath A, Richard J, Dufour E, Ben Said M, Jais J, Verloes A, Le Merrer M, Bodemer C, Baujat G, Gerard-Blanluet M, Bourdon-Lanoy E, Salomon R, Ayme S, Landais P, CEMARA task force, Andersen SK, Klein GO, and Schulz S

Published

2008

112. Survival after neuroAIDS

Author

Lanoy, E., Guiguet, M., Bentata, M., Rouveix, E., Dhiver, C., Poizot-Martin, I., Costagliola, D., and Gasnault, J.

Abstract

We examined if the CNS Penetration-Effectiveness (CPE) score of antiretroviral drugs was associated with survival after a diagnosis of HIV-related encephalopathy, progressive multifocal leukoencephalopathy (PML), cerebral toxoplasmosis, or cryptococcal meningitis.

Published

2011

113. Impact of Newly Available Drugs on Clinical Progression in Patients with Virological Failure after Exposure to Three Classes of Antiretrovirals

Author

Costagliola, Dominique, Potard, Valérie, Duvivier, Claudine, Pradier, Christian, Dupont, Caroline, Salmon, Dominique, Duval, Xavier, Billaud, E, Boué, F, Costagliola, D, Duval, X, Duvivier, C, Enel, P, Fournier, S, Gasnault, J, Gaud, C, Gilquin, J, Grabar, S, Khuong, MA, Lang, JM, Mary-Krause, M, Matheron, S, Meyohas, MC, Pialoux, G, Poizot-Martin, I, Pradier, C, Rouveix, E, Salmon-Ceron, D, Sobel, A, Tattevin, P, Tissot-Dupont, H, Yasdanpanah, Y, Aronica, E, Tirard-Fleury, V, Tortay, I, Abgrall, S, Costagliola, D, Grabar, S, Guiguet, M, Lanoy, E, Leneman, H, Lièvre, L, Mary-Krause, M, Potard, V, Saidi, S, Matheron, S, Vildé, JL, Leport, C, Yeni, P, Bouvet, E, Gaudebout, C, Crickx, B, Picard-Dahan, C, Weiss, L, Tisne-Dessus, D, Tarnier-Cochin, GH, Sicard, D, Salmon, D, Gilquin, J, Auperin, I, Viard, JP, Roudière, L, Boué, F, Fior, R, Delfraissy, JF, Goujard, C, Lesprit, Ph, Jung, C, Meyohas, MC, Meynard, JL, Picard, O, Desplanque, N, Cadranel, J, Mayaud, C, Pialoux, JF, Rozenbaum, W, Bricaire, F, Katlama, C, Herson, S, Simon, A, Decazes, JM, Molina, JM, Clauvel, JF, Gerard, L, Widal, GH Lariboisière-Fernand, Sellier, P, Diemer, M, Dupont, C, Berthé, H, Saïag, P, Mortier, E, Chandemerle, C, de Truchis, P, Bentata, M, Honoré, P, Tassi, S, Jeantils, V, Mechali, D, Taverne, B, Laurichesse, H, Gourdon, F, Lucht, JF, Fresard, A, de Dijon, Chru, de Belfort, CH, Faller, JP, Eglinger, P, Bazin, C, Verdon, R, de Grenoble, Cisih, de Lyon, Cisih, Peyramond, D, Boibieux, A, Touraine, JL, Livrozet, JM, Trepo, C, Cotte, L, Ravaux, I, Tissot-Dupont, H, Delmont, JP, Moreau, J, Gastaut, JA, Poizot-Martin, I, Soubeyrand, J, Retornaz, F, Blanc, PA, Allegre, T, Galinier, A, Ruiz, JM, d'Arles, CH, d'Avignon, CH, Lepeu, G, Granet-Brunello, P, Pelissier, L, Esterni, JP, de Martigues, CH, Nezri, M, Cohen-Valensi, R, Laffeuillade, A, Chadapaud, S, de Nîmes, J Reynes; CHG, May, T, Rabaud, C, Raffi, F, Billaud, E, Pradier, C, Pugliese, P, Michelet, C, Arvieux, C, Caron, F, Borsa-Lebas, F, Lang, JM, Rey, D, de Mulhouse, P Fraisse; CH, Massip, P, Cuzin, L, Arlet-Suau, E, Legrand, MF Thiercelin, Rangueil, CHU, de Tourcoing, CH, Yasdanpanah, Y, Sobesky, M, Pradinaud, R, Gaud, C, and Contant, M

Abstract

Objective To study the prognosis of HIV-infected patients with virological failure after exposure to three classes of antiretroviral drugs (ARVs).Design Cohort study. Setting: French Hospital Database on HIV.Patients Patients previously exposed to at least two nucleoside reverse transcriptase inhibitors (NRTIs), two protease inhibitors and one non-NRTI, with viral load (VL) values of >5000 copies/ml after the exposure criteria were met and a new treatment initiated between 1998 and 2001 with VL >5000 copies/ml.Main outcome measures Risk of new AIDS-defining-events (ADEs) or death from first introduction of a drug never used before occurring between 1998 and 2001 defined as baseline.Results The main baseline characteristics of the 1092 patients were: previous ADE in 49% of cases, median CD4 cell count 181 µl, median VL 4.9 log10copies/ml, median duration of ARV therapy 5.0 years and previous exposure to a median of nine ARVs. The crude progression rates were 20.1/100 patient-years among patients included in 1998, 15.1 in 1999, 11.1 in 2000 and 8.6 in 2001. After adjustment for baseline characteristics, the calendar year of inclusion was associated with the risk of clinical progression (P<0.001). When the types of newly available drugs used at baseline or during follow-up were introduced into the model, year of inclusion was no longer associated with the risk of clinical progression (P=0.42), while exposure to amprenavir/r, lopinavir/r, abacavir or tenofovir was associated with a lower risk.Conclusions The clinical prognosis of heavily pretreated patients experiencing virological failure improved between 1998 and 2001, mainly thanks to the use of newly available drugs with more favourable resistance profiles.

Published

2005

114. Incidence of tuberculosis among HIV-infected patients receiving highly active antiretroviral therapy in Europe and North America

Author

Costagliola, D., Dabis, F., Monforte, Ad, Wolf, F., Egger, M., Fatkenheuer, G., Gill, J., Hogg, R., Justice, A., Ledergerber, B., Lundgren, J., May, M., Phillips, A., Reiss, P., Sabin, C., Staszewski, S., Sterne, J., Weller, I., Beckthold, B., Yip, B., Dauer, B., Fusco, J., Grabar, S., Lanoy, E., Junghans, C., Lavignolle, V., Leth, F., Pereira, E., Pezzotti, P., Schmeisser, N., Billaud, E., Boue, F., Duval, X., Duvivier, C., Enel, P., Fournier, S., Gasnault, J., Gaud, C., Gilquin, J., Khuong, Ma, Lang, Jm, Mary-Krause, M., Matheron, S., Meyohas, Mc, Pialoux, G., Poizot-Martin, I., Pradier, C., Rouveix, E., Salmon-Ceron, D., Sobel, A., Tattevin, P., Tissot-Dupont, H., Yasdanpanah, Y., Aronica, E., Tirard-Fleury, V., Tortay, I., Abgrall, S., Guiguet, M., Leneman, H., Lievre, L., Potard, V., Saidi, S., Vilde, Jl, Leport, C., Yeni, P., Bouvet, E., Gaudebout, C., Crickx, B., Picard-Dahan, C., Weiss, L., Tisne-Dessus, D., Sicard, D., Salmon, D., Auperin, I., Viard, Jp, Roudiere, L., Delfraissy, Jf, Goujard, C., Lesprit, P., Jung, C., Meynard, Jl, Picard, O., Desplanque, N., Cadranel, J., Mayaud, C., Rozenbaum, W., Bricaire, F., Katlama, C., Herson, S., Simon, A., Decazes, Jm, Molina, Jm, Clauvel, Jp, Gerard, L., Widal, Ghlf, Sellier, P., Diemer, M., Dupont, C., Berthe, H., Saiag, P., Mortier, L., Mortier, E., Chandemerle, C., Truchis, P., Bentata, M., Honore, P., Tassi, S., Jeantils, V., Mechali, D., Taverne, B., Laurichesse, H., Gourdon, F., Lucht, F., Fresard, A., Faller, Jp, Eglinger, P., Bazin, C., Verdon, R., Peyramond, D., Boibieux, A., Touraine, Jl, Livrozet, Jm, Trepo, C., Cotte, L., Ravaux, I., Delmont, Jp, Moreau, J., Gastaut, Ja, Soubeyrand, J., Retornaz, F., Blanc, Pa, Allegre, T., Galinier, A., Ruiz, Jm, Lepeu, G., Granet-Brunello, P., Pelissier, L., Esterni, Jp, Nezri, M., Cohen-Valensi, R., Laffeuillade, A., Chadapaud, S., Reynes, J., May, T., Rabaud, C., Raffi, F., Pugliese, P., Michelet, C., Arvieux, C., Caron, F., Borsa-Lebas, F., Fraisse, P., Massip, P., Cuzin, L., Arlet-Suau, E., Legrand, Mft, Sobesky, M., Pradinaud, R., Guyon, F., Contant, M., Montroni, M., Scalise, G., Braschi, Mc, Aviano, Ar, Tirelli, U., Cinelli, R., Pastore, G., Ladisa, N., Minafra, G., Suter, F., Arici, C., Chiodo, F., Colangeli, V., Fiorini, C., Coronado, O., Carosi, G., Cadeo, Gp, Torti, C., Minardi, C., Bertelli, D., Rizzardini, G., Melzi, S., Manconi, Pe, Catanzaro, Pp, Cosco, L., Scerbo, A., Vecchiet, J., D Alessandro, M., Santoro, D., Pusterla, L., Carnevale, G., Citterio, P., Vigano, P., Mena, M., Ghinelli, F., Sighinolfi, L., Leoncini, F., Mazzotta, F., Pozzi, M., Lo Caputo, S., Angarano, G., Grisorio, B., Saracino, A., Ferrara, S., Grima, P., Tundo, P., Pagano, G., Cassola, G., Alessandrini, A., Piscopo, R., Toti, M., Chigiotti, S., Soscia, F., Tacconi, L., Orani, A., Perini, P., Scasso, A., Vincenti, A., Chiodera, F., Castelli, P., Scalzini, A., Palvarini, L., Moroni, M., Lazzarin, A., Cargnel, A., Vigevani, Gm, Caggese, L., Repetto, D., Galli, A., Merli, S., Pastecchia, C., Moioli, Mc, Esposito, R., Mussini, C., Abrescia, N., Chirianni, A., Izzo, Cm, Piazza, M., Marco, M., Viglietti, R., Manzillo, E., Nappa, S., Colomba, A., Abbadessa, V., Prestileo, T., Mancuso, S., Ferrari, C., Pizzaferri, P., Filice, G., Minoli, L., Bruno, R., Novati, S., Baldelli, F., Tinca, M., Petrelli, E., Cioppi, A., Alberici, F., Ruggieri, A., Menichetti, F., Martinelli, C., Stefano, C., La Gala, A., Ballardini, G., Rizzo, E., Magnani, G., Ursitti, Ma, Arlotti, M., Ortolani, P., Cauda, R., Dianzani, F., Ippolito, G., Antinori, A., Antonucci, G., D Elia, S., Narciso, P., Petrosillo, N., Vullo, V., Luca, A., Bacarelli, A., Zaccarelli, M., Acinapura, R., Longis, P., Brandi, A., Trotta, Mp, Noto, P., Lichtner, M., Capobianchi, MR, Carletti, F., Girardi, E., Rezza, G., Mura, Ms, Mannazzu, M., Caramello, P., Di Perri, G., Soranzo, Ml, Orofino, Gc, Arnaudo, I., Bonasso, M., Grossi, Pa, Basilico, C., Poggio, A., Bottari, G., Raise, E., Ebo, F., Lalla, F., Tositti, G., Resta, F., Loso, K., Lepri, Ac, Battegay, M., Bernasconi, E., Boni, J., Bucher, H., Burgisser, P., Cattacin, S., Cavassini, M., Dubs, R., Elzi, L., Erb, P., Fantelli, K., Fischer, M., Flepp, M., Fontana, A., Francioli, P., Furrer, H., Gorgievski, M., Hirschel, B., Kaiser, L., Kind, C., Klimkait, T., Lauper, U., Opravil, M., Paccaud, F., Pantaleo, G., Perrin, L., Piffaretti, Jc, Rickenbach, M., Rudin, C., Schmid, P., Schupbach, J., Speck, R., Telenti, A., Trkola, A., Vernazza, P., Weber, R., Yerly, S., Bronsveld, W., Hillebrand-Haverkort, Me, Prins, Jm, Bos, Jc, Schattenkerk, Jkme, Geerlings, Se, Godfried, Mh, Lange, Jma, Leth, Fc, Lowe, Sh, Meer, Jtm, Nellen, Fjb, Pogany, K., Poll, T., Ruys, Ta, Sankatsing, S., Steingrover, R., Twillert, G., Valk, M., Vonderen, Mga, Vrouenraets, Sme, Vugt, M., Wit, Fwmn, Kuijpers, Tw, Pajkrt, D., Scherpbier, Hj, Eeden, A., Ten Veen, Jh, Dam, Ps, Roos, Jc, Brinkman, K., Frissen, Phj, Weigel, Hm, Mulder, Jw, Gorp, Ecm, Meenhorst, Pl, Mairuhu, Ata, Ziekenhuis, S., Veenstra, J., Danner, Sa, Agtmael, Ma, Claessen, Fap, Perenboom, Rm, Rijkeboer, A., Vonderen, M., Richter, C., Berg, J., Leusen, R., Vriesendorp, R., Jeurissen, Fjf, Kauffmann, Rh, Koger, Elw, Bravenboer, B., Ten Napel, Chh, Kootstra, Gj, Sprenger, Hg, Miesen, Wmaj, Doedens, R., Scholvinck, Eh, Ten Kate, Rw, Houte, Dpf, Polee, M., Kroon, Fp, van den Broek, Dissel, Jt, Schippers, Ef, Schreij, G., Geest, Sv, Verbon, A., Koopmans, Pp, Keuter, M., Post, F., Ven, Ajam, Ende, Me, Gyssens, Ic, Feltz, M., Den Hollander, Jg, Marie, S., Nouwen, Jl, Rijnders, Bja, Vries, Tems, Driessen, G., Groot, R., Hartwig, N., Juttmann, Jr, Heul, C., Kasteren, Mee, Schneider, Mme, Bonten, Mjm, Borleffs, Jcc, Ellerbroek, Pm, Hoepelman, Im, Jaspers, Cajj, Schouten, I., Schurink, Cam, Geelen, Spm, Wolfs, Tfw, Blok, Wl, Tanis, Aa, Groeneveld, Php, Klinieken-Zwolle, I., Back, Nkt, Bakker, Meg, Berkhout, B., Jurriaans, S., Cuijpers, T., Rietra, Pjgm, Roozendaal, Kj, Pauw, W., Zanten, Ap, Blomberg, Bme, Savelkoul, P., Swanink, Cma, Franck, Pfh, Lampe, As, Hendriks, R., Schirm, J., Veenendaal, D., Storm, H., Weel, J., Zeijl, H., Kroes, Acm, Claas, Hcj, Bruggeman, Camva, Goossens, Vj, Galama, Jmd, Melchers, Wjg, Poort, Yag, Doornum, Gjj, Niesters, Mg, Osterhaus, Adme, Schutten, M., Buiting, Agm, Swaans, Cam, Boucher, Cab, Boel, E., Jansz, Af, Losso, M., Duran, A., Vetter, N., Karpov, I., Vassilenko, A., Clumeck, N., Wit, S., Poll, B., Colebunders, R., Machala, L., Rozsypal, H., Dalibor Sedlacek, Nielsen, J., Benfield, T., Kirk, O., Gerstoft, J., Katzenstein, T., Hansen, Abe, Skinhoj, P., Pedersen, C., Zilmer, K., Girard, Pm, Saint-Marc, T., Vanhems, P., Dietrich, M., Manegold, C., Lunzen, J., Stellbrink, Hj, Bickel, M., Goebel, Fd, Rockstroh, J., Schmidt, R., Kosmidis, J., Gargalianos, P., Sambatakou, H., Perdios, J., Panos, G., Filandras, A., Karabatsaki, E., Banhegyi, D., Mulcahy, F., Yust, I., Turner, D., Burke, M., Pollack, S., Hassoun, G., Sthoeger, Z., Maayan, S., Chiesi, A., Borghi, R., Pristera, R., Gabbuti, A., Montesarchio, E., Iacomi, F., Finazzi, R., Viksna, L., Chaplinskas, S., Hemmer, R., Staub, T., Bruun, J., Maeland, A., Ormaasen, V., Knysz, B., Gasiorowski, J., Horban, A., Prokopowicz, D., Wiercinska-Drapalo, A., Boron-Kaczmarska, A., Pynka, M., Beniowski, M., Mularska, E., Trocha, H., Antunes, F., Valadas, E., Mansinho, K., Matez, F., Duiculescu, D., Babes, V., Streinu-Cercel, A., Vinogradova, E., Rakhmanova, A., Jevtovic, D., Mokras, M., Stanekova, D., Gonzalez-Lahoz, J., Sanchez-Conde, M., Garcia-Benayas, T., Martin-Carbonero, L., Soriano, V., Clotet, B., Jou, A., Conejero, J., Tural, C., Gatell, Jm, Miro, Jm, Blaxhult, A., Karlsson, A., Pehrson, P., Soravia-Dunand, V., Kravchenko, E., Chentsova, N., Barton, S., Johnson, Am, Mercey, D., Johnson, Ma, Mocroft, A., Murphy, M., Weber, J., Scullard, G., Fisher, M., Brettle, R., Loveday, C., Gatell, J., Johnson, A., Vella, S., Gjorup, I., Friis-Moeller, N., Cozzi-Lepri, A., Bannister, W., Mollerup, D., Podlevkareva, D., Olsen, Ch, Kjaer, J., Raffanti, S., Dieterch, D., Becker, S., Scarsella, A., Fusco, G., Most, B., Balu, R., Rana, R., Beckerman, R., Ising, T., Irek, R., Johnson, B., Hirani, A., Dejesus, E., Pierone, G., Lackey, P., Irek, C., Burdick, J., Leon, S., Arch, J., Helm, Eb, Carlebach, A., Muller, A., Haberl, A., Nisius, G., Lennemann, T., Rottmann, C., Wolf, T., Stephan, C., Mosch, M., Gute, P., Locher, L., Lutz, T., Klauke, S., Knecht, G., Doerr, Hw, Sturmer, M., Hentig, N., Jennings, B., Beylot, J., Chene, G., Dupon, M., Longy-Boursier, M., Pellegrin, Jl, Ragnaud, Jm, Salamon, R., Thiebaut, R., Lewden, C., Lawson-Ayayi, S., Mercie, P., Moreau, Jf, Moriat, P., Bernard, N., Lacoste, D., Malvy, D., Neau, D., Blaizeau, Mj, Decoin, M., Delveaux, S., Hannapier, C., Labarrere, S., Lavignolle-Aurillac, V., Uwamaliya-Nziyumvira, B., Palmer, G., Touchard, D., Balestre, E., Alioum, A., Jacqmin-Gadda, H., Morlat, P., Bonarek, M., Bonnet, F., Coadou, B., Gellie, P., Nouts, C., Bocquentin, F., Dutronc, H., Lafarie, S., Aslan, A., Pistonne, T., Thibaut, P., Vatan, R., Chambon, D., La Taille, C., Cazorla, C., Ocho, A., Castera, L., Fleury, H., Lafon, Me, Masquelier, B., Pellegrin, I., Breilh, D., Blanco, P., Loste, P., Caunegre, L., Bonnal, F., Farbos, S., Ferrand, M., Ceccaldi, J., Tchamgoue, S., Witte, S., Buy, E., Alexander, C., Barrios, R., Braitstein, P., Brumme, Z., Chan, K., Cote, H., Gataric, N., Geller, J., Guillemi, S., Harrigan, Harris, M., Joy, R., Levy, A., Montaner, J., Montessori, V., Palepu, A., Phillips, E., Phillips, P., Press, N., Tyndall, M., Wood, E., Ballinger, J., Bhagani, S., Breen, R., Byrne, P., Carroll, A., Cropley, I., Cuthbertson, Z., Drinkwater, T., Fernandez, T., Geretti, Am, Murphy, G., Ivens, D., Johnson, M., Kinloch-De Loes, S., Lipman, M., Madge, S., Prinz, B., Bell, Dr, Shah, S., Swaden, L., Tyrer, M., Youle, M., Chaloner, C., Gumley, H., Holloway, J., Puradiredja, D., Sweeney, J., Tsintas, R., Bansi, L., Fox, Z., Lampe, F., Smith, C., Amoah, E., Clewley, G., Dann, L., Gregory, B., Jani, I., Janossy, G., Kahan, M., Thomas, M., Gill, Mj, Read, R., Schmeisser, V., Voigt, K., Wasmuth, Jc, Wohrmann, A., and Antiretroviral Therapy Cohort Coll

115. When to initiate combined antiretroviral therapy to reduce mortality and aids-defining illness in HIV-infected persons in developed countries

Author

Cain, L. E., Logan, R., Robins, J. M., Hernán, M. A., Sterne, J. A. C., Sabin, C., Bansi, L., Goulet, J., Justice, A., Sighem, A., Wolf, F., Bucher, H. C., Wyl, V., Esteve, A., Casabona, J., Del Amo, J., Moreno, S., Seng, R., Meyer, L., Santiago Pérez-Hoyos, Muga, R., Lodi, S., Lanoy, E., and Costagliola, D.

116. Prothrombotic markers and early spontaneous recanalization in ST-segment elevation myocardial infarction

Author

Mg, Huisse, Lanoy E, Tcheche D, Laurent Feldman, Bezeaud A, Anglès-Cano E, Mary-Krause M, de Prost D, Mc, Guillin, and Pg, Steg

117. The French Society of Dermatology. Joint session between the French Society of Pediatric Dermatology, the French Society of Dermatology and the British Society of Paediatric Dermatology | Société Française de Dermatologie: Séance conjointe entre la Société Française de Dermatologie Pédiatrique, la Société Française de Dermatologie et la British Society of Paediatric Dermatology

Author

Wierzbicka, E., Robert, M., Herbreteau, D., Lorette, G., Jury, C. S., Mealyea, M., Mchenry, P., Lever, R., Wallach, D., Coste, J., Tilles, G., Taïeb, A., Debons, M., Bernier, C., Sebastien Barbarot, Chavigny, J. M., Le Fol, C., Bauer, D., Anton, M., Mollé, I., Gagnayre, R., Stalder, J. F., Carrie, E., Hadj-Rabia, S., Bourdon-Lanoy, E., Pruskowski, A., Hamel, D., Prost, Y., Casanova, J. L., Bodemer, C., Boutet, A., Mechinaud, F., Mazereeuw-Hautier, J., Wilson, L., Atherton, D., Harper, J. I., Titeux, M., Prost-Squarcioni, C., Hovnanian, A., Onyon, C., Goodyear, H., Giacchero, D., Allieri-Rosenthal, M., Bouillet, L., Ortonne, J. P., Lacour, J. P., Mak, R. K. H., Paige, D., Leigh, I. M., Kelsell, D. P., O Toole, E. A., Larregue, M., Biedere, C., Lhuillier, N., Leverger, G., Descargues, P., Lesueur, F., Bonafé, J., Fischer, J., Frot, A. S., Piloquet, H., Lamant, L., Cassagnau, E., Morice, F. M., Leaute-Labreze, C., Boralevi, F., Lepreux, S., Lang-Bandon, J., Webber, N. K., Paige, D. G., Galliot-Repkat, C., Olivier-Faivre, L., Couillault, G., Piard, F., Bougeard, G., Frebourg, T., Vabres, P., Gass, J., Firth, H., Burrows, N., Corradini, N., Rouse, P., Sidwell, R. U., Jiskoot, Green, J. S. A., Mowbray, M., Schofield, O. M. V., Viseux, V., Devoldere, C., El Hanache, A., Chaby, G., Morin, G., Lok, C., Vourc H, M., and Thomas, C.

118. Bullous pemphigoid in young patients: A retrospective study of 74 cases,Pemphigoïde du sujet jeune: Étude rétrospective de 74 cas

Author

Bourdon-Lanoy, E., Roujeau, J. -C, Joly, P., Guillaume, J. -C, Bernard, P., Prost, C., Tancrède-Bohin, E., Delaporte, E., Picard-Dahan, C., Albes, B., Bedane, C., Doutre, M. -S, Chosidow, O., Lok, C., Pauwels, C., Chevrand-Breton, J., Sassolas, B., and Richard, M. -A

119. CEMARA: a Web dynamic application within a N-tier architecture for rare diseases

Author

Claude Messiaen, Le Mignot, L., Rath, A., Richard, J. -B, Dufour, E., Ben Said, M., Jais, J. -P, Verloes, A., Le Merrer, M., Bodemer, C., Baujat, G., Gerard-Blanluet, M., Bourdon-Lanoy, E., Salomon, R., Ayme, S., and Landais, P.

120. Evolution of laparoscopic liver surgery in France over the last decade.

Author

Deyrat, J., Fuks, D., Murris, J., Lanoy, E., Nassar, A., Dhote, A., Marchese, U., Mallet, V., Katsahian, S., Gaillard, M., and Tzedakis, S.

Published

2024

121. Evolution of minimally invasive liver surgery in France over the last decade.

Author

Deyrat J, Fuks D, Murris J, Lanoy E, Nassar A, Dhote A, Marchese U, Mallet V, Katsahian S, Gaillard M, and Tzedakis S

Subjects

Humans, France, Female, Male, Middle Aged, Liver Neoplasms surgery, Aged, Minimally Invasive Surgical Procedures statistics & numerical data, Minimally Invasive Surgical Procedures trends, Laparoscopy statistics & numerical data, Laparoscopy trends, Laparoscopy methods, Retrospective Studies, Hepatectomy statistics & numerical data, Hepatectomy trends, Hepatectomy methods

Abstract

Background: Despite evidence of benefits on postoperative outcomes, minimally invasive liver surgery (MILS) had a very low diffusion up to 2014, and recent evolution is unknown. Our aim was to analyze the recent diffusion and adoption of MILS and compare the trends in indications, extent of resection, and institutional practice with open liver surgery (OLS)., Methods: We analyzed the French nationwide, exhaustive cohort of all patients undergoing a liver resection in France between January 1, 2013 and December 31, 2022. Average annual percentage changes (AAPC) in the incidence of MILS and OLS were compared using mixed-effects log-linear regression models. Time trends were analyzed in terms of extent of resection, indication, and institutional practice., Results: MILS represented 25.2% of 74,671 liver resections and year incidence doubled from 16.5% in 2013 to 35.4% in 2022. The highest AAPC were observed among major liver resections [+ 22.2% (19.5; 24.9) per year], primary [+ 10.2% (8.5; 12.0) per year], and secondary malignant tumors [+ 9.9% (8.2; 11.6) per year]. The highest increase in MILS was observed in university hospitals [+ 14.7% (7.7; 22.2) per year] performing 48.8% of MILS and in very high-volume (> 150 procedures/year) hospitals [+ 12.1% (9.0; 15.3) per year] performing 19.7% of MILS. OLS AAPC decreased for all indications and institutions and accelerated over time from - 1.8% (- 3.9; - 0.3) per year in 2013-2018 to - 5.9% (- 7.9; - 3.9) per year in 2018-2022 (p = 0.013)., Conclusions: This is the first reported trend reversal between MILS and OLS. MILS has considerably increased at a national scale, crossing the 20% tipping point of adoption rate as defined by the IDEAL framework., (© 2024. The Author(s), under exclusive licence to Springer Science+Business Media, LLC, part of Springer Nature.)

Published

2024

122. Mortality in hepatitis C virus-cured vs. hepatitis C virus-uninfected people with HIV.

Author

Requena MB, Grabar S, Lanoy E, Pialoux G, Billaud E, Duvivier C, Merle P, Piroth L, Tattevin P, Salmon D, Weiss L, Costagliola D, and Lacombe K

Subjects

Male, Humans, Middle Aged, Female, Hepacivirus, Antiviral Agents therapeutic use, Liver Cirrhosis epidemiology, HIV Infections complications, HIV Infections drug therapy, HIV Infections epidemiology, Hepatitis C, Chronic complications, Hepatitis C, Chronic drug therapy, Hepatitis C, Chronic epidemiology, Hepatitis C complications, Hepatitis C drug therapy, Hepatitis C epidemiology

Abstract

Objective: It is unknown whether hepatitis C virus (HCV)-cured people with HIV (PWH) without cirrhosis reached the same mortality risk as HCV-uninfected PWH. We aimed to compare mortality in PWH cured of HCV by direct-acting antivirals (DAAs) to mortality in individuals with HIV monoinfection., Design: Nationwide hospital cohort., Methods: HIV-controlled participants without cirrhosis and HCV-cured by DAAs started between September 2013 and September 2020, were matched on age (±5 years), sex, HIV transmission group, AIDS status, and body mass index (BMI) (±1 kg/m 2 ) to up to 10 participants with a virally suppressed HIV monoinfection followed at the time of HCV cure ±6 months. Poisson regression models with robust variance estimates were used to compare mortality in both groups after adjusting for confounders., Results: The analysis included 3961 HCV-cured PWH (G1) and 33 872 HCV-uninfected PWH (G2). Median follow-up was 3.7 years in G1 [interquartile range (IQR): 2.0-4.6], and 3.3 years (IQR: 1.7-4.4) in G2. Median age was 52.0 years (IQR: 47.0-56.0), and 29 116 (77.0%) were men. There were 150 deaths in G1 [adjusted incidence rate (aIR): 12.2/1000 person-years] and 509 (aIR: 6.3/1000 person-years) in G2, with an incidence rate ratio (IRR): 1.9 [95% confidence interval (CI), 1.4-2.7]. The risk remained elevated 12 months post HCV cure (IRR: 2.4 [95% CI, 1.6-3.5]). Non-AIDS/non-liver-related malignancy was the most common cause of death in G1 (28 deaths)., Conclusions: Despite HCV cure and HIV viral suppression, after controlling on factors related to mortality, DAA-cured PWH without cirrhosis remain at higher risk of all-cause mortality than people with HIV monoinfection. A better understanding of the determinants of mortality is needed in this population., (Copyright © 2023 Wolters Kluwer Health, Inc. All rights reserved.)

Published

2023

123. eIF4F translation initiation complex, a predictive marker of response to immunotherapy in mucosal melanoma.

Author

Moya-Plana A, Ngo C, Lanoy E, Vagner S, and Robert C

Subjects

Humans, Cell Line, Tumor, Immunotherapy, Eukaryotic Initiation Factor-4F, Melanoma therapy

Published

2023

124. Protective effect of obesity on survival in cancers treated with immunotherapy vanishes when controlling for type of cancer, weight loss and reduced skeletal muscle.

Author

Antoun S, Lanoy E, Ammari S, Farhane S, Martin L, Robert C, Planchard D, Routier E, Voisin AL, Messayke S, Champiat S, Michot JM, Laghouati S, Lambotte O, Marabelle A, and Baracos V

Subjects

Humans, Prospective Studies, Weight Loss, Obesity epidemiology, Body Mass Index, Muscle, Skeletal, Immunotherapy, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Melanoma drug therapy

Abstract

Introduction: Association of high body mass index (BMI) with longer survival has been reported in patients on immune checkpoint inhibitors (ICIs), but results are inconsistent. This 'obesity paradox' is potentially confounded by the effects of BMI change over time and of skeletal muscle depletion., Methods: We conducted a secondary analysis of a prospective cohort, including consecutive patients receiving ICI treatment for melanoma (n = 411) and non-small cell lung cancer (NSCLC) (n = 389) in routine care., Results: In the univariable analysis of the entire population, overweight/obesity (BMI ≥ 25 kg/m 2 ) was associated with longer survival (p < 0.01); however, this effect was limited to NSCLC (p < 0.01) and was absent in melanoma. Weight loss (WL) and reduced skeletal muscle mass were observed in patients within all BMI categories. WL was associated with shorter survival in multivariable analysis in both tumour sites (p < 0.01), and for NSCLC, BMI lost significance when WL was included (p = 0.13). In models further adjusted for CT-defined skeletal muscle mass, WL retained significance for both tumour types (p < 0.01), and reduced skeletal muscle only for NSCLC (p = 0.02) was associated with shorter survival. WL retained significance when biomarkers (lactate dehydrogenase enzyme, albumin and derived neutrophil to lymphocyte ratio) were added to the multivariable model., Conclusions: The so-called 'obesity paradox', counterintuitive association between high BMI and longer survival, vanished when controlling for confounders, such as type of cancer, and manifestations of depletion (WL and reduced skeletal muscle mass)., Competing Interests: Conflict of interest statement The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Pr Robert reported consultant advisory for BMS, Novartis, MSD, AstraZeneca, Pierre Fabre, Sanofi, Roche and co-founder of Robonexus outside submitted work. Dr Planchard reported consulting advisory role or lectures from AstraZeneca, Bristol-Myers Squibb, Boehringer Ingelheim, Celgene, Daiichi Sankyo, Eli Lilly, Merck, Novartis, Pfizer, prIME Oncology, Peer CME, Roche, Janssen, Abbvie, honoraria from AstraZeneca, Bristol-Myers Squibb, Boehringer Ingelheim, Celgene, Eli Lilly, Merck, Novartis, Pfizer, prIME Oncology, Peer CME, Roche, Janssen, Abbvie outside submitted work, Clinical trials research as principal or co-investigator (Institutional financial interests) from AstraZeneca, Bristol-Myers Squibb, Boehringer Ingelheim, Eli Lilly, Merck, Novartis, Pfizer, Roche, Medimmun, Sanofi-Aventis, Taiho Pharma, Novocure, Daiichi Sankyo, Janssen, Abbvie outside submitted work and travel, accommodations, expenses from AstraZeneca, Roche, Novartis, Pfizer. Dr Routier reported consultant advisory for BMS, Novartis, Roche, clinical trials research principal or co-investigator for BMS, Novartis, Roche, Merck-Serono, MSD, Idera, Iovance, Regeneron, Debiopharm, Replimune outside submitted work and travel accommodations, expenses from BMS, Novartis, MSD. Dr Champiat reported consulting advisory role for Advisory Board: Alderaan Biotechnology, Amgen, AstraZeneca, Avacta, Ellipses Pharma, Oncovita, Seagen, UltraHuman, reported honoraria from Amgen, Astellas, AstraZeneca, Bristol Myers Squibb, Eisai, Genmab, Janssen, Merck, Novartis and Roche and was principal investigator of clinical trials for Abbvie, Amgen, Cytovation, Eisai, Imcheck Therapeutics, Molecular Partners Ag, Merck, Ose Pharma, Pierre Fabre, Sanofi Aventis, Sotio A.S, Transgene. Dr Michot: Principal/sub-Investigator of Clinical trials for Amgen, Astex, AstraZeneca, Medimmune, Roche, Sanofi, Xencor, BMS, Seattle Genetics, Regeneron. Pr Lambotte: paid expert testimony and consultancy fees from BMS France, MSD, Astra Zeneca; expert testimony for Janssen., Gilead. Pr Marabelle has worked as a clinical investigator and has participated to scientific advisory boards or has consulted for the following companies commercialising anti-PD(L)1 antibodies: Bristol Myers Squibb, Merck Sharp & Dohme, Astra Zeneca, Roche/Genentech, Sanofi, Merck Serono and Pfizer. No other disclosures were reported., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2023

125. Effect of bariatric surgery on cancer risk: results from an emulated target trial using population-based data.

Author

Lazzati A, Epaud S, Ortala M, Katsahian S, and Lanoy E

Subjects

Humans, Obesity complications, Obesity surgery, Proportional Hazards Models, Weight Loss, Bariatric Surgery methods, Neoplasms complications, Neoplasms etiology, Obesity, Morbid surgery

Abstract

Background: The impact of weight loss induced by bariatric surgery on cancer occurrence is controversial. To study the causal effect of bariatric surgery on cancer risk from an observational database, a target-trial emulation technique was used to mimic an RCT., Methods: Data on patients admitted between 2010 and 2019 with a diagnosis of obesity were extracted from a national hospital discharge database. Criteria for inclusion included eligibility criteria for bariatric surgery and the absence of cancer in the 2 years following inclusion. The intervention arms were bariatric surgery versus no surgery. Outcomes were the occurrence of any cancer and obesity-related cancer; cancers not related to obesity were used as negative controls., Results: A total of 1 140 347 patients eligible for bariatric surgery were included in the study. Some 288 604 patients (25.3 per cent) underwent bariatric surgery. A total of 48 411 cancers were identified, including 4483 in surgical patients and 43 928 among patients who did not receive bariatric surgery. Bariatric surgery was associated with a decrease in the risk of obesity-related cancer (hazard ratio (HR) 0.89, 95 per cent c.i. 0.83 to 0.95), whereas no significant effect of surgery was identified with regard to cancers not related to obesity (HR 0.96, 0.91 to 1.01)., Conclusion: When emulating a target trial from observational data, a reduction of 11 per cent in obesity-related cancer was found after bariatric surgery., (© The Author(s) 2022. Published by Oxford University Press on behalf of BJS Society Ltd. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com.)

Published

2022

126. Convalescent plasma improves overall survival in patients with B-cell lymphoid malignancy and COVID-19: a longitudinal cohort and propensity score analysis.

Author

Hueso T, Godron AS, Lanoy E, Pacanowski J, Levi LI, Gras E, Surgers L, Guemriche A, Meynard JL, Pirenne F, Idri S, Tiberghien P, Morel P, Besson C, Duléry R, Lamure S, Hermine O, Gagneux-Brunon A, Freymond N, Grabar S, and Lacombe K

Subjects

Antibodies, Viral, Humans, Immunization, Passive, Propensity Score, SARS-CoV-2, COVID-19 Serotherapy, COVID-19 therapy, Neoplasms

Abstract

Patients with hematological malignancy and COVID-19 display a high mortality rate. In such patients, immunosuppression due to underlying disease and previous specific treatments impair humoral response, limiting viral clearance. Thus, COVID-19 convalescent plasma (CCP) therapy appears as a promising approach through the transfer of neutralizing antibodies specific to SARS-CoV-2. We report the effect of CCP in a cohort of 112 patients with hematological malignancy and COVID-19 and a propensity score analysis on subgroups of patients with B-cell lymphoid disease treated (n = 81) or not (n = 120) with CCP between May 1, 2020 and April 1, 2021. The overall survival of the whole cohort was 65% (95% CI = 56-74.9) and 77.5% (95% CI = 68.5-87.7) for patients with B-cell neoplasm. Prior anti-CD20 monoclonal antibody therapy was associated with better overall survival, whereas age, high blood pressure, and COVID-19 severity were associated with a poor outcome. After an inverse probability of treatment weighting approach, we observed in anti-CD20-exposed patients with B-cell lymphoid disease a decreased mortality of 63% (95% CI = 31-80) in the CCP-treated group compared to the CCP-untreated subgroup, confirmed in the other sensitivity analyses. Convalescent plasma may be beneficial in COVID-19 patients with B-cell neoplasm who are unable to mount a humoral immune response., (© 2022. The Author(s), under exclusive licence to Springer Nature Limited.)

Published

2022

127. Trend of antibiotic consumption and its association with influenza-like illnesses in France between 2004 and 2018.

Author

Yaacoub S, Lanoy E, Hider-Mlynarz K, Saleh N, and Maison P

Subjects

Drug Utilization, France epidemiology, Humans, Macrolides, Anti-Bacterial Agents therapeutic use, Influenza, Human drug therapy, Influenza, Human epidemiology

Abstract

Background: Antibiotic consumption has been reported to be driven by the treatment of respiratory tract infections. Our objectives were to describe the trend of antibiotic consumption in France compared with that of other European countries; to describe the evolution of each antibiotic class in France; and to explore the relationship between antibiotic consumption and incidence of influenza-like illnesses., Methods: In this observational study, antibiotic consumption was reported as defined daily doses per 1000 inhabitants per day in the community and hospital sectors in descriptive and graphical formats, using data from the European Surveillance of Antimicrobial Consumption Network database. The total consumption and the consumption of different classes of antibiotics in France according to time and influenza-like illnesses were studied using multiple linear regression models., Results: The total consumption of antibiotics in France was constant over the 15 years. It was driven by the community sector (92.8%) and was higher than the consumption of other European Union countries (P-value < 0.001). The beta-lactam penicillins were the most consumed antibiotic class and the only class that increased with time. The multiple linear regression models showed a positive correlation between antibiotic consumption in the community sector and incidence of influenza-like illnesses [B = 0.170, 95% CI (0.088-0.252)]. Similar significant results were shown between other antibiotic classes used in the management of influenza-like illnesses (other beta-lactams, and macrolides, lincosamides and streptogramins) and influenza-like illnesses., Conclusion: Our results suggest that antibiotics used in the management of respiratory tract infections might be involved in the irrational use of antibiotics., (© The Author(s) 2021. Published by Oxford University Press on behalf of the European Public Health Association. All rights reserved.)

Published

2021

128. Intratumoral Immunotherapy: From Trial Design to Clinical Practice.

Author

Champiat S, Tselikas L, Farhane S, Raoult T, Texier M, Lanoy E, Massard C, Robert C, Ammari S, De Baère T, and Marabelle A

Subjects

Clinical Trials as Topic, Combined Modality Therapy methods, Humans, Injections, Intralesional, Neoplasms immunology, Neoplasms mortality, Oncolytic Viruses immunology, Progression-Free Survival, Tumor Escape drug effects, Tumor Microenvironment drug effects, Tumor Microenvironment immunology, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Cancer Vaccines administration & dosage, Immunotherapy methods, Neoplasms therapy, Oncolytic Virotherapy methods

Abstract

Systemic immunotherapies such as immune checkpoint blockade targeted at PD(L)1 and CTLA4 have demonstrated their ability to provide durable tumor responses and long-term overall survival benefits for some patients in several solid tumor types. However, a majority of patients remain resistant to these treatments and a significant proportion of them develop severe autoimmune and inflammatory adverse events. Preclinical studies have demonstrated that intratumoral injections of immunostimulatory products (oncolytics, pattern recognition receptor agonists,…) that are able to trigger type I IFN release and enhance tumor antigen presentation on immune cells could generate a strong antitumor immunity and overcome the resistance to systemic immune checkpoint blockade therapies. The intratumoral immunotherapy strategies that are currently in clinical development offer a unique therapeutic and exploratory setting to better understand the immune contexture across tumor lesions of patients with metastatic cancer. Also these local therapeutic products could turn cold tumors into hot and improve the response rates to cancer immunotherapies while diminishing their systemic exposure and toxicities. Intratumoral immunotherapies could prime or boost the immunity against tumors and therefore radically change the combinatorial therapeutic strategies currently pursued for metastatic and local cancers to improve their long-term survival. We aimed to review and discuss the scientific rationale for intratumoral immunotherapy, the challenges raised by this strategy in terms of drug development within clinical trials and the current state-of-the-art regarding the clinical practice of this innovative approach., (©2020 American Association for Cancer Research.)

Published

2021

129. Impact of young age on platinum response in women with epithelial ovarian cancer: Results of a large single-institution registry.

Author

Michels J, Genestie C, Dunant A, Caron O, Lanoy E, Colomba E, Pommeret F, Rey A, Gouy S, Duvillard P, Teuff GL, Larue C, Savoye AM, Lhommé C, Leary A, Morice P, and Pautier P

Subjects

Adolescent, Adult, Age Factors, Aged, Aged, 80 and over, Carcinoma, Ovarian Epithelial pathology, Carcinoma, Ovarian Epithelial surgery, Cohort Studies, Female, Follow-Up Studies, Humans, Middle Aged, Neoplasm Staging, Organoplatinum Compounds administration & dosage, Ovarian Neoplasms pathology, Ovarian Neoplasms surgery, Progression-Free Survival, Retrospective Studies, Survival Rate, Treatment Outcome, Young Adult, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Carcinoma, Ovarian Epithelial drug therapy, Ovarian Neoplasms drug therapy

Abstract

Objective: In young women, EOC is a rare disease with an uncertain genetic and biological substrate., Methods: We report a long follow-up of EOC patients treated at Gustave Roussy between 1990 and 2009. We matched young patients aged ≤30 years to randomly selected older patients aged ≥40 years according to known prognostic factors (i.e. FIGO stage, histology and surgical residual disease) and the date of diagnosis with a threshold at the year 2000 to balance the treatment procedures., Results: EOC was diagnosed in 68 patients aged ≤30 years matched with 111 patients aged ≥40 years. Low-grade (LG) (i.e. serous and endometrioid) (52%, n = 35) and mucinous (i.e. 23%, n = 16 infiltrative and 12% n = 8 expansile) tumors are prevalent. High-grade (HG) tumors are rare (7%, n = 5). Early stage diseases (53%, n = 36 FIGO I/II) are predominant. Response to platinum based chemotherapy is observed to be inferior in young patients as compared to matched older patients (ORR, 29 vs 84% p = 0.0002). For HG tumors the PFS is of 0% at 5 and 10 years in younger as compared to 30% in older patients. No difference in PFS (median 4.9 vs 9.8 ms, p = 0.58) and OS (not reached vs 15.3 ms, p = 0.47) is found overall among younger and older patients respectively. The median follow-up was 72 months (range, 11-288 months). No genetic abnormalities were found., Conclusions: Young EOC patients are most often diagnosed at an early FIGO stage with LG serous or mucinous histology. Tumors are significantly more resistant to platinum-based chemotherapy in younger patients., Competing Interests: Declaration of Competing Interest Dr. Pautier reports support from Roche, Astra Zeneca, non-financial support from MSD, Clovis, GSK, outside the submitted work. Dr. Leary reports support from Tesaro, Clovis, Astra Zeneca, MSD, Merck Serono, Seattle Genetics, Gridstone, Biocad, Ability, Gamamabs and grants from Merus, Gamamabs, Sanofi, Inivata. Drs Michels, Genestie, Dunant, Caron, Colomba, Pommeret, Rey, Gouy, Duvillard, Le Teuff, Savoye, Lhommé, Morice report no conflict of interest. All authors contributed equally to this practice statement., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2021

130. Infectious complications in patients treated with immune checkpoint inhibitors.

Author

Karam JD, Noel N, Voisin AL, Lanoy E, Michot JM, and Lambotte O

Subjects

Aged, Female, Humans, Immunosuppressive Agents therapeutic use, Male, Middle Aged, Retrospective Studies, Antineoplastic Agents, Immunological adverse effects, Immune Checkpoint Inhibitors adverse effects, Infections chemically induced, Infections epidemiology, Neoplasms drug therapy

Abstract

Objective: Immune checkpoint inhibitor (ICI) antibodies constitute a new generation of cancer treatments, associated with immune-related adverse events (irAEs). A previous retrospective study of patients with metastatic melanoma (treated mostly with anti-CTLA4 antibodies) reported a serious infection rate of 7.3%. The main risk factors were corticoids and infliximab use. We sought to describe infections and risk factors among patients receiving anti-PD-1/PD-L1 ICIs., Patients and Methods: We reviewed 200 medical records sampled randomly from a French prospective registry, which collates patients treated with anti-PD-1/PD-L1 ICIs. We recorded demographic data, the occurrence of irAEs, immunosuppressant use, and the outcome., Results: Thirty-six patients (18%) experienced an infection by a median (interquartile range) of 47 (19.2-132) days after initiation of the ICI. Twenty-one patients (58.3%) had a lung infection, seven (19.4%) had a skin infection, seven (19.4%) had a urinary tract infection, and all of them received antibiotics. The infection was generally mild, and the patients were treated as outpatient. There were no infection-related deaths and no opportunistic infection. Sixty percent of the patients were being treated for metastatic melanoma and 35.5% for non-small cell lung cancer, and 106 irAEs (mostly grade II) were reported. Forty-seven patients received steroids for cancer symptoms or irAEs, and five received immunosuppressants during the immunotherapy. We did not observe any association between corticosteroid or immunosuppressant use and the occurrence of an infection., Conclusion: The infection rate in patients treated with an anti-PD-1/PD-L1 ICI was 18%, without any severe or opportunistic infection. The occurrence of an infection was not associated with corticosteroid or immunosuppressant use., Competing Interests: Conflict of interest statement Dr. Olivier Lambotte reports paid expert testimony and consultancy fees from BMS France, MSD, Astra Zeneca, and Incyte; consultancy fees from Genzyme; and expert testimony for Janssen. Dr. Nicolas Noël reports speaker fees from MSD and Janssen outside the scope of the submitted work. Dr. Jean-Marie Michot reports fees from Celgene, Bristol-Myers Squibb, AstraZeneca, and Janssen; non-financial support from AstraZeneca, Roche, Novartis, Gilead, Celgene, and Bristol-Myers Squibb. The remaining authors declare no conflicts of interest., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published

2020

131. Dose escalation phase 1 study of radiotherapy in combination with anti-cytotoxic-T-lymphocyte-associated antigen 4 monoclonal antibody ipilimumab in patients with metastatic melanoma.

Author

Boutros C, Chaput-Gras N, Lanoy E, Larive A, Mateus C, Routier E, Sun R, Tao YG, Massard C, Bahleda R, Schwob D, Ibrahim N, Khoury Abboud RM, Caramella C, Lancia A, Cassard L, Roy S, Soria JC, Robert C, and Deutsch E

Subjects

Adult, Aged, Aged, 80 and over, Antineoplastic Combined Chemotherapy Protocols pharmacology, Dose-Response Relationship, Radiation, Humans, Ipilimumab pharmacology, Maximum Tolerated Dose, Middle Aged, Antineoplastic Combined Chemotherapy Protocols therapeutic use, CTLA-4 Antigen metabolism, Ipilimumab therapeutic use, Melanoma drug therapy

Abstract

Background: A synergy between radiotherapy and anti-cytotoxic-T-lymphocyte-associated antigen 4 (anti-CTLA-4) monoclonal antibody has been demonstrated preclinically. The Mel-Ipi-Rx phase 1 study aimed to determine the maximum tolerated dose (MTD) and safety profile of radiotherapy combined with ipilimumab in patients with metastatic melanoma., Patients and Methods: A 3+3 dose escalation design was used with 9, 15, 18 and 24 Gy dose of radiotherapy at week 4 combined with 10 mg/kg ipilimumab every 3 weeks for four doses. Patients with evidence of clinical benefit at week 12 were eligible for maintenance with ipilimumab 10 mg/kg every 12 weeks starting at week 24 until severe toxicity or disease progression. The database lock occurred on April 30, 2019. Tumor growth rate of irradiated lesions and non-irradiated lesions were analyzed to assess the systemic immunologic antitumor response. Blood immune monitoring was performed before and during treatment to determine if radiotherapy could modify ipilimumab pharmacodynamics., Results: 19 patients received ipilimumab between August 2011 and July 2015. Nine patients received the four doses of ipilimumab. All patients received the combined radiotherapy. Grade 3 adverse events occurred in nine patients, the most common being colitis and hepatitis. No drug-related death occurred. Dose limiting toxicity occurred in two of six patients in the cohort receiving 15 Gy. The MTD was 9 Gy. Two patients had complete response, three had partial response response and seven had stable disease, giving an objective response rate of 31% and a clinical benefit rate of 75% at week 24. The median duration of follow-up was 5.8 years (Q1=4.5; Q3=6.8). The median overall survival (95% CI) was estimated at 0.9 years (0.5-2). The median progression-free survival (PFS) (95% CI) was 0.4 (0.2-1.4). Radiotherapy combined with ipilimumab was associated with increased CD4+ and CD8+ICOS+ T cells. Increased CD8+ was significantly associated with PFS., Conclusion: When combined with ipilimumab at 10 mg/kg, the MTD of radiotherapy was 9 Gy. This combination of ipilimumab and radiotherapy appears to be associated with antitumor activity. Increased CD8+ was significantly associated with PFS. Thus, immune biomarkers may be useful for early response evaluation., Trial Registration Number: NCT01557114., Competing Interests: Competing interests: CB has acted as a board advisor for BMS, has been a speaker for Merck and has received travel fees from Amgen and Pfizer. NC-G has received research grants from Cytune Pharma, GSK and Sanofi. She has acted as a board advisor for AstraZeneca and has been a speaker for Sanofi and AstraZeneca. CM has acted as consultant of BMS and Merck. ER has acted as a consultant for BMS, Novartis and Roche, and has received travel fees from BMS and Novartis. RS has received travel fees from AstraZeneca. CM has acted as a consultant from Amgen, Astellas, Astra Zeneca, Bayer, BeiGene, BMS, Celgene, Debiopharm, Genentech, Ipsen, Janssen, Lilly, MedImmune, MSD, Novartis, Pfizer, Roche, Sanofi and Orion. He is the principal or subinvestigator of clinical trials for Abbvie, Aduro, Agios, Amgen, Argen-x, Astex, AstraZeneca, Aveopharmaceuticals, Bayer, Beigene, Blueprint, BMS, BoeringerIngelheim, Celgene, Chugai, Clovis, DaiichiSankyo, Debiopharm, Eisai, Eos, Exelixis, Forma, Gamamabs, Genentech, Gortec, GSK, H3 biomedecine, Incyte, InnatePharma, Janssen, Kura Oncology, Kyowa, Lilly, Loxo, Lysarc, LytixBiopharma, Medimmune, Menarini, Merus, MSD, Nanobiotix, NektarTherapeutics, Novartis, Octimet, Oncoethix, OncopeptidesAB, Orion, Pfizer, Pharmamar, Pierre Fabre, Roche, Sanofi, Servier, Sierra Oncology, Taiho, Takeda, Tesaro and Xencor. J-CS has received consultancy fees from AstraZeneca, Astex, Clovis, GSK, GamaMabs, Lilly, MSD, Mission Therapeutics, Merus, Pfizer, PharmaMar, Pierre Fabre, Roche/Genentech, Sanofi, Servier, Symphogen and Takeda. He has been a full-time employee of MedImmune since September 2017. He is a shareholder of AstraZeneca and Gritstone. CR has acted as a consultant of Amgen, BMS, GSK, Merck, Novartis and Roche. ED has received research grants from Roche, Servier, AstraZeneca, Merck Serono, BMS, MSD, Amgen, Accuray and Boerhinger. He has received personal fees from Roche, AstraZeneca, Merck Serono, Amgen, Accuray and Boerhinger., (© Author(s) (or their employer(s)) 2020. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2020

132. Integrating expert's knowledge constraint of time dependent exposures in structure learning for Bayesian networks.

Author

Asvatourian V, Leray P, Michiels S, and Lanoy E

Subjects

Bayes Theorem, Causality, Computer Simulation, Humans, Algorithms

Abstract

Learning a Bayesian network is a difficult and well known task that has been largely investigated. To reduce the number of candidate graphs to test, some authors proposed to incorporate a priori expert knowledge. Most of the time, this a priori information between variables influences the learning but never contradicts the data. In addition, the development of Bayesian networks integrating time such as dynamic Bayesian networks allows identifying causal graphs in the context of longitudinal data. Moreover, in the context where the number of strongly correlated variables is large (i.e. oncology) and the number of patients low; if a biomarker has a mediated effect on another, the learning algorithm would associate them wrongly and vice versa. In this article we propose a method to use the a priori expert knowledge as hard constraints in a structure learning method for Bayesian networks with a time dependant exposure. Based on a simulation study and an application, where we compared our method to the state of the art PC-algorithm, the results showed a better recovery of the true graphs when integrating hard constraints a priori expert knowledge even for small level of information., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

133. One or Two Immune Checkpoint Inhibitors?

Author

Robert C, Lanoy E, and Besse B

Subjects

Antineoplastic Agents therapeutic use, Antineoplastic Combined Chemotherapy Protocols, Humans, Lung Neoplasms immunology, Melanoma immunology, Antibodies, Monoclonal therapeutic use, Ipilimumab therapeutic use, Lung Neoplasms drug therapy, Melanoma drug therapy

Abstract

The combination of ipilimumab and nivolumab was evaluated versus standard treatments in melanoma and lung cancer. Analysis of these trials highlights the differences in outcomes and potential predictive biomarkers across tumor types as well as the multiple remaining questions concerning the optimal use of immune checkpoint inhibitors., (Copyright © 2019 Elsevier Inc. All rights reserved.)

Published

2019

134. Baseline gut microbiota predicts clinical response and colitis in metastatic melanoma patients treated with ipilimumab.

Author

Chaput N, Lepage P, Coutzac C, Soularue E, Le Roux K, Monot C, Boselli L, Routier E, Cassard L, Collins M, Vaysse T, Marthey L, Eggermont A, Asvatourian V, Lanoy E, Mateus C, Robert C, and Carbonnel F

Published

2019

135. No evidence for changes in skeletal muscle mass or weight during first-line chemotherapy for metastatic colorectal cancer.

Author

Antoun S, Bayar MA, Dyevre V, Lanoy E, Smolenschi C, and Ducreux M

Subjects

Aged, Antineoplastic Agents pharmacology, Body Composition drug effects, Body Weight drug effects, Female, Humans, Male, Middle Aged, Muscle, Skeletal drug effects, Prospective Studies, Survival Analysis, Tomography, X-Ray Computed, Treatment Outcome, Antineoplastic Agents adverse effects, Colorectal Neoplasms drug therapy, Muscle, Skeletal diagnostic imaging, Neoplasm Metastasis drug therapy

Abstract

Background: Studies over the past 10 years strongly support an association between skeletal muscle mass (SMM) depletion and outcome in metastatic colorectal cancer (mCRC). Factors influencing SMM changes over time are, however, poorly studied. We analyzed the impact of SMM on overall survival and chemotherapy toxicities in mCRC patients treated with first-line chemotherapy. Changes in weight and body composition were evaluated during follow-up., Methods: Patients enrolled in the randomized phase II ACCORD trial comparing two chemotherapy regimens were screened. Body composition parameters (SMM, adipose tissue) were assessed prospectively with computed tomography (CT) imaging, and toxicities were recorded. Mixed models were used to assess weight and BC changes during 4 months of treatment follow-up., Results: Among 145 patients included in ACCORD, 76 had available baseline CT scans and were included in the current study. Mean age was 60.6 ± 10.0 years, 50% were women, 82% had colon cancer, and 62% had two or more metastatic sites. At baseline, 49% had lost at least 5% of their initial weight, including 26% who had lost more than 10%; 53% had SMM depletion. In this homogenous cohort, there were no statistically significant associations between SMM depletion and overall survival, progression-free survival or chemotherapy toxicity. There were no decreases in weight or SMM during follow-up. Weight and SMM changes were not influenced by diarrhea either grade 3-4 or any grade (reported in 74% of patients). For patients with weight loss ≥10% at baseline, SMM increased significantly after 4 months of follow-up and after disease stabilization following chemotherapy (P = 0.008)., Conclusions: In a homogenous mCRC cohort, SMM depletion was not associated with survival or chemotherapy toxicity. Despite most patient experiencing diarrhea, no changes in weight or SMM were found during 4 months of follow-up. However, hypotheses deriving from our exploratory study have to be tested in further larger sample size studies., Trial Registration: Clinicaltrials.gov NCT00423696 (2011).

Published

2019

136. Long-Term Survival in Patients Responding to Anti-PD-1/PD-L1 Therapy and Disease Outcome upon Treatment Discontinuation.

Author

Gauci ML, Lanoy E, Champiat S, Caramella C, Ammari S, Aspeslagh S, Varga A, Baldini C, Bahleda R, Gazzah A, Michot JM, Postel-Vinay S, Angevin E, Ribrag V, Hollebecque A, Soria JC, Robert C, Massard C, and Marabelle A

Subjects

Adult, Aged, Aged, 80 and over, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized therapeutic use, B7-H1 Antigen immunology, B7-H1 Antigen metabolism, Clinical Trials, Phase I as Topic, Female, Humans, Male, Middle Aged, Neoplasms immunology, Neoplasms metabolism, Nivolumab therapeutic use, Outcome Assessment, Health Care methods, Programmed Cell Death 1 Receptor immunology, Programmed Cell Death 1 Receptor metabolism, Retrospective Studies, Survival Analysis, Withholding Treatment, Young Adult, Antineoplastic Agents, Immunological therapeutic use, B7-H1 Antigen antagonists & inhibitors, Cancer Survivors statistics & numerical data, Neoplasms drug therapy, Outcome Assessment, Health Care statistics & numerical data, Programmed Cell Death 1 Receptor antagonists & inhibitors

Abstract

Purpose: Anti-PD-(L)1 can provide overall survival (OS) benefits over conventional treatments for patients with many different cancer types. However, the long-term outcome of cancer patients responding to these therapies remains unknown. This study is an exploratory study that aimed to describe the long-term survival of patients responding to anti-PD-(L)1 monotherapy across multiple cancer types. Patients and Methods: Data from patients treated with an anti-PD-(L)1 monotherapy in a phase I trial at Gustave Roussy were retrospectively analyzed over a period of 5 years. All cancer types ( n = 19) were included. Clinical and biological factors associated with response, long-term survival, and secondary refractory disease were studied., Results: Among 262 eligible patients, the overall objective response rate was 29%. The median progression-free survival of responder patients (RP) at 3 months was 30 months, and the median OS of RP was not reached after a median follow-up of 34 months. In RPs, 3- and 5-year OS percentages were 84% and 64%, respectively. No death occurred in the 21 complete responders (CR) during the overall follow-up. However, many partial responders (PR) showed subsequent tumor relapses to treatment. Long responders (response ≥2 years) represented 11.8% of the overall population. These findings should be validated in further prospective studies., Conclusions: There are currently no differences in therapeutic strategies between CRs and PRs to anti-PD-(L)1. We found a striking difference in OS between these two types of responses. Our results are in favor of evaluating patient stratification strategies and intensification of treatments when tumor lesions of a partial responder to immunotherapy stop improving. See related commentary by Cohen and Flaherty, p. 910 ., (©2018 American Association for Cancer Research.)

Published

2019

137. What's next in using CT scans to better understand cachexia?

Author

Antoun S, Rossoni C, and Lanoy E

Subjects

Adipose Tissue physiopathology, Biomarkers, Body Composition, Cachexia etiology, Fatigue etiology, Fatigue physiopathology, Humans, Muscle Strength physiology, Muscle, Skeletal physiopathology, Neoplasms complications, Nutrition Assessment, Prospective Studies, Severity of Illness Index, Weight Loss physiology, Cachexia diagnostic imaging, Cachexia physiopathology, Sarcopenia diagnostic imaging, Sarcopenia physiopathology, Tomography, X-Ray Computed methods

Abstract

Purpose of Review: Cachexia (CAX), a protein metabolism disorder commonly associated with cancer, can be evaluated by computed tomography (CT) scan assessment of skeletal muscle mass (SMM), a parameter associated with patient outcome. This review analyzes current barriers for using CT scans of SMM in routine management for defining prognostic risk groups, and proposes new areas of research to reach a better understanding of CAX mechanisms., Recent Findings: Current research is focused on establishing a robust and relevant CAX staging system to reach a consensual definition. Previous biomarkers of CAX are poorly associated with outcome and do not exhibit clinical benefit. Systemic inflammatory marker, decrease in intake assessments, and/or nonnutritional criteria have been integrated to develop a multidimensional, highly complex CAX signature and CAX staging., Summary: A standardized definition of sarcopenia is essential, and its value in clinical practice should be evaluated in prospective interventional studies using skeletal muscle assessment. SMM loss may be a key element in defining early protein disorders occurring before weight loss and could be used as a trigger for initiating early nutritional support. Changes in SMM and body composition during follow-up are useful tools for exploring CAX mechanisms in terms of intrinsic factors or tumor evolution.

Published

2018

138. Estimating causal effects of time-dependent exposures on a binary endpoint in a high-dimensional setting.

Author

Asvatourian V, Coutzac C, Chaput N, Robert C, Michiels S, and Lanoy E

Subjects

Biomarkers analysis, Humans, Outcome Assessment, Health Care methods, Outcome Assessment, Health Care statistics & numerical data, Time Factors, Algorithms, Computer Simulation, Data Interpretation, Statistical, Models, Statistical

Abstract

Background: Recently, the intervention calculus when the DAG is absent (IDA) method was developed to estimate lower bounds of causal effects from observational high-dimensional data. Originally it was introduced to assess the effect of baseline biomarkers which do not vary over time. However, in many clinical settings, measurements of biomarkers are repeated at fixed time points during treatment and, therefore, this method needs to be extended. The purpose of this paper is to extend the first step of the IDA, the Peter Clarks (PC)-algorithm, to a time-dependent exposure in the context of a binary outcome., Methods: We generalised the so-called "PC-algorithm" to take into account the chronological order of repeated measurements of the exposure and proposed to apply the IDA with our new version, the chronologically ordered PC-algorithm (COPC-algorithm). The extension includes Firth's correction. A simulation study has been performed before applying the method for estimating causal effects of time-dependent immunological biomarkers on toxicity, death and progression in patients with metastatic melanoma., Results: The simulation study showed that the completed partially directed acyclic graphs (CPDAGs) obtained using COPC-algorithm were structurally closer to the true CPDAG than CPDAGs obtained using PC-algorithm. Also, causal effects were more accurate when they were estimated based on CPDAGs obtained using COPC-algorithm. Moreover, CPDAGs obtained by COPC-algorithm allowed removing non-chronological arrows with a variable measured at a time t pointing to a variable measured at a time t´ where t´ < t. Bidirected edges were less present in CPDAGs obtained with the COPC-algorithm, supporting the fact that there was less variability in causal effects estimated from these CPDAGs. In the example, a threshold of the per-comparison error rate of 0.5% led to the selection of an interpretable set of biomarkers., Conclusions: The COPC-algorithm provided CPDAGs that keep the chronological structure present in the data and thus allowed to estimate lower bounds of the causal effect of time-dependent immunological biomarkers on early toxicity, premature death and progression.

Published

2018

139. Tolerance and outcomes of stereotactic radiosurgery combined with anti-programmed cell death-1 (pembrolizumab) for melanoma brain metastases.

Author

Nardin C, Mateus C, Texier M, Lanoy E, Hibat-Allah S, Ammari S, Robert C, and Dhermain F

Subjects

Adult, Aged, Aged, 80 and over, Antibodies, Monoclonal, Humanized adverse effects, Antineoplastic Agents, Immunological adverse effects, Antineoplastic Agents, Immunological therapeutic use, Brain Neoplasms secondary, Chemoradiotherapy, Female, Humans, Male, Middle Aged, Neoplasm Metastasis, Radiosurgery adverse effects, Retrospective Studies, Skin Neoplasms pathology, Treatment Outcome, Antibodies, Monoclonal, Humanized therapeutic use, Brain Neoplasms drug therapy, Brain Neoplasms radiotherapy, Radiosurgery methods, Skin Neoplasms drug therapy, Skin Neoplasms radiotherapy

Abstract

Anti-programmed cell death-1 (anti-PD1) antibodies are currently the first-line treatment for patients with metastatic BRAF wild-type melanoma, alone or combined with the anti-CTLA4 monoclonal antibody, ipilimumab. To date, data on safety and the outcomes of patients treated with the anti-PD1 monoclonal antibodies, pembrolizumab (PB), or nivolumab, combined with stereotactic radiosurgery (SRS), for melanoma brain metastases (MBM) are scarce. We retrospectively reviewed all patients with MBM treated with PB combined with SRS between 2012 and 2015. The primary endpoint was neurotoxicity. The secondary endpoints were local, distant intracranial controls and overall survival (OS). Among 74 patients with MBM treated with SRS, 25 patients with a total of 58 MBM treated with PB combined with SRS within 6 months were included. Radiation necrosis, occurring within a median time of 6.5 months, was observed for four MBM (6.8%) in four patients. No other significant SRS-related adverse event was observed. After a median follow-up of 8.4 months, local control was achieved in 46 (80%) metastases and 17 (68%) patients. Perilesional oedema and intratumour haemorrhage appearing or increasing after SRS were associated with local progression (P<0.001). The median OS was 15.3 months (95% confidence interval: 4.6-26). The timing between SRS and PB administration did not seem to influence the risk of radiation necrosis, intracranial control or OS. SRS combined with PB was well tolerated and achieved local control in 80% of the lesions. Prolonged OS was observed compared with that currently yielded in this population of patients. Prospective studies are required to explore further the optimal ways to combine immunotherapy and SRS.

Published

2018

140. Safety and efficacy of anti-programmed death 1 antibodies in patients with cancer and pre-existing autoimmune or inflammatory disease.

Author

Danlos FX, Voisin AL, Dyevre V, Michot JM, Routier E, Taillade L, Champiat S, Aspeslagh S, Haroche J, Albiges L, Massard C, Girard N, Dalle S, Besse B, Laghouati S, Soria JC, Mateus C, Robert C, Lanoy E, Marabelle A, and Lambotte O

Subjects

Adult, Aged, Aged, 80 and over, Antibodies, Monoclonal adverse effects, Antineoplastic Agents, Immunological adverse effects, Autoimmune Diseases diagnosis, Autoimmune Diseases mortality, Disease-Free Survival, Female, France, Humans, Inflammation diagnosis, Inflammation mortality, Male, Middle Aged, Neoplasms diagnosis, Neoplasms immunology, Neoplasms mortality, Programmed Cell Death 1 Receptor immunology, Prospective Studies, Registries, Risk Factors, Time Factors, Treatment Outcome, Young Adult, Antibodies, Monoclonal therapeutic use, Antineoplastic Agents, Immunological therapeutic use, Autoimmune Diseases immunology, Inflammation immunology, Neoplasms drug therapy, Programmed Cell Death 1 Receptor antagonists & inhibitors

Abstract

Objective: Patients with autoimmune or inflammatory disease (AID) are susceptible to immune-related adverse events (irAEs) when treated with immune check-point inhibitors (ICIs). We decided to analyse the safety and effectiveness of anti-PD-1 antibodies in AID patients and look for an association between the presence of pre-existing AID and the clinical outcome., Methods: In a prospective study of the REISAMIC registry of grade ≥2 irAEs occurring in ICI-treated patients, we studied the associations between pre-existing AID on one hand and irAE-free survival, overall survival and best objective response rate on the other., Results: We identified 45 patients with 53 AIDs in REISAMIC. The cancer diagnoses included melanoma (n = 36), non-small-cell lung cancer (n = 6) and others (n = 3). The most frequent pre-existing AIDs were vitiligo (n = 17), psoriasis (n = 12), thyroiditis (n = 7), Sjögren syndrome (n = 4) and rheumatoid arthritis (n = 2). Twenty patients (44.4%) presented with at least one irAE: eleven of these were associated with a pre-existing AID ('AID flare'). Treatment with anti-PD-1 antibodies was maintained in 15 of the 20 patients with an irAE. The IrAE-free survival time was significantly shorter in AID patients (median: 5.4 months) than in AID-free patients (median: 13 months, p = 2.1 × 10 -4 ). The AID and AID-free groups did not differ significantly with regard to the overall survival time and objective response rate (p = 0.38 and 0.098, respectively)., Conclusion: In patients treated with anti-PD-1 antibody, pre-existing AID was associated with a significantly increased risk of irAEs. Our results indicate that cancer treatments with anti-PD-1 antibodies are just as effective in AID patients as they are in AID-free patients., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2018

141. In the immuno-oncology era, is anti-PD-1 or anti-PD-L1 immunotherapy modifying the sensitivity to conventional cancer therapies?

Author

Aspeslagh S, Matias M, Palomar V, Dercle L, Lanoy E, Soria JC, and Postel-Vinay S

Subjects

Adult, Aged, B7-H1 Antigen immunology, Disease-Free Survival, Drug Resistance, Neoplasm, Female, Humans, Male, Middle Aged, Neoplasms immunology, Neoplasms mortality, Neoplasms pathology, Programmed Cell Death 1 Receptor immunology, Retrospective Studies, Signal Transduction drug effects, Time Factors, Treatment Outcome, Tumor Microenvironment, Young Adult, Antineoplastic Agents, Immunological therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, B7-H1 Antigen antagonists & inhibitors, Immunotherapy methods, Neoplasms drug therapy, Programmed Cell Death 1 Receptor antagonists & inhibitors

Abstract

Introduction: The advent of anti-programmed death receptor-1/ligand-1 antibodies (anti-PD(L)1) is profoundly changing the therapeutic strategy of oncology. As anti-PD(L)1 modulate tumour microenvironment, it might impact sensitivity to conventional cancer therapy (CCT). Therefore, we explored whether sensitivity to CCT was different before and after anti-PD(L)1 therapy., Methods: Patients who started anti-PD(L)1 treatment at Gustave Roussy Cancer Centre between February 2012 and December 2015, and who received at least one line of CCT immediately before and immediately after anti-PD(L)1, were eligible. We analysed progression-free survival (PFS) and overall response rate (ORR) of the CCT line immediately before (PFSpre/ORRpre) and after (PFSpost/ORRpost) anti-PD(L)1. PFS and ORR were compared using Wilcoxon signed rank and McNemar tests in a paired data subset for patients having received identical class of CCT pre and post anti-PD(L)1 therapy., Results: Among 118 eligible patients, 65% received anti-PD1 and 35% anti-PD-L1 agents. Median PFSpre versus PFSpost was 4.7 versus 3.5 months (p = 0.011), respectively; it was 5.7 versus 6.8 months (NS) for patients who derived clinical benefit from immunotherapy and 3.9 versus 3.0 months (p = 0.012) for patients who were primary resistant to anti-PD(L)1 therapy. Subgroup analysis did not reveal any significant difference in PFS or ORR before versus after anti-PD(L)1 therapy according to CCT class or to its ability to induce immunogenic cell death., Conclusion: Patients who derive benefit from immune therapies tend to have better PFS on conventional therapies after having received the anti-PD(L)1 agent. Further studies on larger data sets are warranted to confirm these findings., (Copyright © 2017 Elsevier Ltd. All rights reserved.)

Published

2017

142. Factors which modulate the rates of skeletal muscle mass loss in non-small cell lung cancer patients: a pilot study.

Author

Atlan P, Bayar MA, Lanoy E, Besse B, Planchard D, Ramon J, Raynard B, and Antoun S

Subjects

Carcinoma, Non-Small-Cell Lung pathology, Female, Humans, Lung Neoplasms pathology, Male, Middle Aged, Muscle, Skeletal pathology, Pilot Projects, Weight Loss, Carcinoma, Non-Small-Cell Lung complications, Lung Neoplasms complications, Muscle, Skeletal physiology

Abstract

Purpose: Advanced non-small cell lung cancer (NSCLC) is associated with weight loss which may reflect skeletal muscle mass (SMM) and/or total adipose tissue (TAT) depletion. This study aimed to describe changes in body composition (BC) parameters and to identify the factors unrelated to the tumor which modulate them., Methods: SMM, TAT, and the proportion of SMM to SMM + TAT were assessed with computed tomography. Estimates of each BC parameter at follow-up initiation and across time were derived from a mixed linear model of repeated measurements with a random intercept and a random slope. The same models were used to assess the independent effect of gender, age, body mass index (BMI), and initial values on changes in each BC parameter., Results: Sixty-four patients with stage III or IV NSCLC were reviewed. The mean ± SD decreases in body weight and SMM were respectively 59 ± 3 g/week (P < 0.03) and 7 mm 2 /m 2 /week (P = 0.0003). During follow-up, no changes were identified in TAT nor in muscle density or in the proportion of SMM to SMM + TAT, estimated at 37 ± 2% at baseline. SMM loss was influenced by initial BMI (P < 0.0001) and SMM values (P = 0.0002): the higher the initial BMI or SMM values, the greater the loss observed. Weight loss was greater when the initial weight was heavier (P < 0.0001)., Conclusion: Our results demonstrate that SMM wasting in NSCLC is lower when initial SMM and BMI values are low. These exploratory findings after our attempt to better understand the intrinsic factors associated with muscle mass depletion need to be confirmed in larger studies.

Published

2017

143. Transcriptional response to hypoxic stress in melanoma and prognostic potential of GBE1 and BNIP3.

Author

Buart S, Terry S, Noman MZ, Lanoy E, Boutros C, Fogel P, Dessen P, Meurice G, Gaston-Mathé Y, Vielh P, Roy S, Routier E, Marty V, Ferlicot S, Legrès L, Bouchtaoui ME, Kamsu-Kom N, Muret J, Deutsch E, Eggermont A, Soria JC, Robert C, and Chouaib S

Abstract

Gradients of hypoxia occur in most solid tumors and cells found in hypoxic regions are associated with the most aggressive and therapy-resistant fractions of the tumor. Despite the ubiquity and importance of hypoxia responses, little is known about the variation in the global transcriptional response to hypoxia in melanoma. Using microarray technology, whole genome gene expression profiling was first performed on established melanoma cell lines. From gene set enrichment analyses, we derived a robust 35 probes signature (hypomel for HYPOxia MELanoma) associated with hypoxia-response pathways, including 26 genes up regulated, and 9 genes down regulated. The microarray data were validated by RT-qPCR for the 35 transcripts. We then validated the signature in hypoxic zones from 8 patient specimens using laser microdissection or macrodissection of Formalin fixed-paraffin-embedded (FFPE) material, followed with RT-qPCR. Moreover, a similar hypoxia-associated gene expression profile was observed using NanoString technology to analyze RNAs from FFPE melanoma tissues of a cohort of 19 patients treated with anti-PD1. Analysis of NanoString data from validation sets using Non-Negative Matrix Factorization (NMF) analysis (26 genes up regulated in hypoxia) and dual clustering (samples and genes) further revealed that the increased level of BNIP3 (Bcl-2 adenovirus E1B 19 kDa-interacting protein 3)/GBE1 (glycogen branching enzyme1) differential pair correlates with the lack of response of melanoma patients to anti-PD1 (pembrolizumab) immunotherapy. These studies suggest that through elevated glycogenic flux and induction of autophagy, hypoxia is a critical molecular program that could be considered as a prognostic factor for melanoma., Competing Interests: CONFLICTS OF INTEREST We declare no competing financial interests.

Published

2017

144. Patient-reported tolerability of adverse events in phase 1 trials.

Author

Henon C, Lissa D, Paoletti X, Thibault C, Le Tourneau C, Lanoy E, Hollebecque A, Massard C, Soria JC, and Postel-Vinay S

Abstract

Background: Phase I experts recommend revisiting dose-limiting toxicity (DLT) definition to include chronic and cumulative toxicities induced by new molecularly targeted therapies. Patient's assessment of late toxicities' tolerability is, however, unknown., Materials and Methods: A prospective survey on adverse events (AEs) tolerability on 23 National Cancer InstituteCommon Terminology Criteria for Adverse Event, Version 4 (NCI-CTCAE.v4) items was conducted at Gustave Roussy's Phase I department. Patients' maximum tolerability duration was recorded at baseline, during trial and at trial completion. Results were compared with the corresponding physicians' survey., Results: 52 patients enrolled in 27 Phase I trials between May 2014 and November 2015 completed 102 forms. At baseline, the most feared G2/G3 AEs were haematuria (74%), vomiting (71%) and hyperglycemia (64%)/dry mouth (94%), hyperglycemia (92%) and vomiting (92%). At trial completion, the most feared G2/G3 AEs were personality change (83.3%), haematuria (82%) and fever (80%)/dry mouth, fever and dizziness (100% each). Tolerability score did not differ over time. More previous treatments and occurrence of severe AEs were associated with better tolerability at study completion (p=0.0234 and p=0.0153, respectively, in multivariate analysis). Patient's tolerability differed from physician's assessment., Conclusion: AEs considered intolerable by patients are toxicities that directly impact their quality of life and differ from those feared by physicians or included in DLT definition. Patient-reported tolerability of AEs may help in optimising drug development., Competing Interests: Competing interests: None declared.

Published

2017

145. Baseline gut microbiota predicts clinical response and colitis in metastatic melanoma patients treated with ipilimumab.

Author

Chaput N, Lepage P, Coutzac C, Soularue E, Le Roux K, Monot C, Boselli L, Routier E, Cassard L, Collins M, Vaysse T, Marthey L, Eggermont A, Asvatourian V, Lanoy E, Mateus C, Robert C, and Carbonnel F

Subjects

Aged, Colitis microbiology, Female, Humans, Male, Melanoma complications, Melanoma microbiology, Melanoma pathology, Neoplasm Metastasis, Prospective Studies, RNA, Ribosomal, 16S genetics, Antineoplastic Agents, Immunological therapeutic use, Colitis complications, Intestines microbiology, Ipilimumab therapeutic use, Melanoma drug therapy, Microbiota

Abstract

Background: Ipilimumab, an immune checkpoint inhibitor targeting CTLA-4, prolongs survival in a subset of patients with metastatic melanoma (MM) but can induce immune-related adverse events, including enterocolitis. We hypothesized that baseline gut microbiota could predict ipilimumab anti-tumor response and/or intestinal toxicity., Patients and Methods: Twenty-six patients with MM treated with ipilimumab were prospectively enrolled. Fecal microbiota composition was assessed using 16S rRNA gene sequencing at baseline and before each ipilimumab infusion. Patients were further clustered based on microbiota patterns. Peripheral blood lymphocytes immunophenotypes were studied in parallel., Results: A distinct baseline gut microbiota composition was associated with both clinical response and colitis. Compared with patients whose baseline microbiota was driven by Bacteroides (cluster B, n = 10), patients whose baseline microbiota was enriched with Faecalibacterium genus and other Firmicutes (cluster A, n = 12) had longer progression-free survival (P = 0.0039) and overall survival (P = 0.051). Most of the baseline colitis-associated phylotypes were related to Firmicutes (e.g. relatives of Faecalibacterium prausnitzii and Gemmiger formicilis), whereas no colitis-related phylotypes were assigned to Bacteroidetes. A low proportion of peripheral blood regulatory T cells was associated with cluster A, long-term clinical benefit and colitis. Ipilimumab led to a higher inducible T-cell COStimulator induction on CD4+ T cells and to a higher increase in serum CD25 in patients who belonged to Faecalibacterium-driven cluster A., Conclusion: Baseline gut microbiota enriched with Faecalibacterium and other Firmicutes is associated with beneficial clinical response to ipilimumab and more frequent occurrence of ipilimumab-induced colitis., (© The Author 2017. Published by Oxford University Press on behalf of the European Society for Medical Oncology. All rights reserved. For permissions, please email: journals.permissions@oup.com.)

Published

2017

146. Statistical approaches for evaluating body composition markers in clinical cancer research.

Author

Bayar MA, Antoun S, and Lanoy E

Subjects

Biomarkers, Tumor metabolism, Biomedical Research methods, Confounding Factors, Epidemiologic, Humans, Neoplasms pathology, Outcome Assessment, Health Care, Body Composition physiology, Models, Statistical, Neoplasms therapy

Abstract

Introduction: The term 'morphomics' stands for the markers of body composition in muscle and adipose tissues. in recent years, as part of clinical cancer research, several associations between morphomics and outcome or toxicity were found in different treatment settings leading to a growing interest. we aim to review statistical approaches used to evaluate these markers and suggest practical statistical recommendations. Area covered: We identified statistical methods used recently to take into account properties of morphomics measurements. We also reviewed adjustment methods on major confounding factors such as gender and approaches to model morphomic data, especially mixed models for repeated measures. Finally, we focused on methods for determining a cut-off for a morphomic marker that could be used in clinical practice and how to assess its robustness. Expert commentary: From our review, we proposed 13 key points to strengthen analyses and reporting of clinical research assessing associations between morphomics and outcome or toxicity.

Published

2017

147. A Novel Spectroscopically Determined Pharmacodynamic Biomarker for Skin Toxicity in Cancer Patients Treated with Targeted Agents.

Author

Azan A, Caspers PJ, Bakker Schut TC, Roy S, Boutros C, Mateus C, Routier E, Besse B, Planchard D, Seck A, Kamsu Kom N, Tomasic G, Koljenović S, Noordhoek Hegt V, Texier M, Lanoy E, Eggermont AM, Paci A, Robert C, Puppels GJ, and Mir LM

Subjects

Aged, Area Under Curve, Biomarkers analysis, Erlotinib Hydrochloride adverse effects, Female, Humans, Imidazoles adverse effects, Indoles adverse effects, Male, Middle Aged, Oximes adverse effects, Pilot Projects, Protein Kinase Inhibitors adverse effects, Pyridones adverse effects, Pyrimidinones adverse effects, ROC Curve, Sensitivity and Specificity, Skin pathology, Sulfonamides adverse effects, Vemurafenib, Algorithms, Antineoplastic Agents adverse effects, Drug Eruptions diagnosis, Skin chemistry, Spectrum Analysis, Raman methods

Abstract

Raman spectroscopy is a noninvasive and label-free optical technique that provides detailed information about the molecular composition of a sample. In this study, we evaluated the potential of Raman spectroscopy to predict skin toxicity due to tyrosine kinase inhibitors treatment. We acquired Raman spectra of skin of patients undergoing treatment with MEK, EGFR, or BRAF inhibitors, which are known to induce severe skin toxicity; for this pilot study, three patients were included for each inhibitor. Our algorithm, based on partial least squares-discriminant analysis (PLS-DA) and cross-validation by bootstrapping, discriminated to variable degrees spectra from patient suffering and not suffering cutaneous adverse events. For MEK and EGFR inhibitors, discriminative power was more than 90% in the viable epidermis skin layer; whereas for BRAF inhibitors, discriminative power was 71%. There was a 81.5% correlation between blood drug concentration and Raman signature of skin in the case of EGFR inhibitors and viable epidermis skin layer. Our results demonstrate the power of Raman spectroscopy to detect apparition of skin toxicity in patients treated with tyrosine kinase inhibitors at levels not detectable via dermatological inspection and histological evaluation. Cancer Res; 77(2); 557-65. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published

2017

148. Sarcopenia is Associated with Chemotherapy Toxicity in Patients Undergoing Cytoreductive Surgery with Hyperthermic Intraperitoneal Chemotherapy for Peritoneal Carcinomatosis from Colorectal Cancer.

Author

Chemama S, Bayar MA, Lanoy E, Ammari S, Stoclin A, Goéré D, Elias D, Raynard B, and Antoun S

Subjects

Administration, Intravenous, Adult, Antineoplastic Combined Chemotherapy Protocols administration & dosage, Body Composition, Camptothecin administration & dosage, Camptothecin analogs & derivatives, Cytoreduction Surgical Procedures adverse effects, Female, Fluorouracil administration & dosage, Humans, Infusions, Parenteral, Irinotecan, Leucovorin administration & dosage, Male, Middle Aged, Neutropenia chemically induced, Operative Time, Organoplatinum Compounds administration & dosage, Oxaliplatin, Peritoneal Neoplasms secondary, Postoperative Complications etiology, Antineoplastic Combined Chemotherapy Protocols adverse effects, Colorectal Neoplasms pathology, Hyperthermia, Induced adverse effects, Peritoneal Neoplasms therapy, Sarcopenia complications

Abstract

Background: Despite the positive survival results of cytoreductive surgery (CRS) plus hyperthermic intraperitoneal chemotherapy (HIPEC), criticisms have been put forward regarding the safety of this treatment as a result of a high morbidity rate. Muscle depletion (sarcopenia) is associated with the occurrence of postoperative complications. The purpose of this study was to determine the association between sarcopenia and postoperative morbidity after CRS-HIPEC for peritoneal carcinomatosis from colorectal cancer by distinguishing the complications linked to CRS itself and those associated with chemotherapy (HIPEC) toxicities., Methods: Data concerning 97 consecutive patients who had undergone CRS-HIPEC were recorded. We analyzed the events occurring within 30 days after surgery that were prospectively recorded in a database. Sarcopenia was assessed using the L3 muscle index on computed tomography performed during the 2 months preceding surgery., Results: The sarcopenic patients experienced significantly more chemotherapy toxicities (57 vs. 26 %; p = 0.004) and especially neutropenia (36 vs. 17 %; p = 0.04) than their nonsarcopenic counterparts. There was no difference in complications linked to the CRS procedure between sarcopenic and nonsarcopenic patients. In the multivariate analysis, sarcopenia was the only parameter independently associated with the risk of chemotherapy toxicity (odds ratio 3.97; 95 % confidence interval 1.52-10.39; p = 0.005)., Conclusions: Despite the local administration of chemotherapy, systemic toxicity was observed in sarcopenic patients after CRS-HIPEC. This relationship favors new treatment strategies with white blood cell growth factors or chemotherapy dosing based on muscle value.

Published

2016

149. Safety profiles of anti-CTLA-4 and anti-PD-1 antibodies alone and in combination.

Author

Boutros C, Tarhini A, Routier E, Lambotte O, Ladurie FL, Carbonnel F, Izzeddine H, Marabelle A, Champiat S, Berdelou A, Lanoy E, Texier M, Libenciuc C, Eggermont AM, Soria JC, Mateus C, and Robert C

Subjects

Antineoplastic Combined Chemotherapy Protocols therapeutic use, CTLA-4 Antigen immunology, Humans, Immunotherapy methods, Lymphocyte Activation immunology, Molecular Targeted Therapy methods, Programmed Cell Death 1 Receptor immunology, Antibodies, Monoclonal, Humanized therapeutic use, CTLA-4 Antigen antagonists & inhibitors, Melanoma drug therapy, Programmed Cell Death 1 Receptor antagonists & inhibitors, Skin Neoplasms drug therapy

Abstract

Inhibition of immune checkpoints using anti-programmed cell death-1 (PD-1) or anti cytotoxic-T-lymphocyte-associated antigen 4 (CTLA-4) monoclonal antibodies has revolutionized the management of patients with advanced-stage melanoma and is among the most promising treatment approaches for many other cancers. Use of CTLA-4 and PD-1 inhibitors, either as single agents, or in combination, has been approved by the US FDA for the treatment of metastatic melanoma. Treatment with these novel immunotherapies results in a unique and distinct spectrum of adverse events, which are mostly related to activation of the immune system and are, therefore, an unwanted consequence of their mechanisms of action. Adverse effects of CTLA-4 and/or PD-1 inhibition are most commonly observed in the skin, gastrointestinal tract, liver and endocrine systems and include pruritus, rash, nausea, diarrhoea and thyroid disorders. In this Review, the authors describe the adverse event profile of checkpoint inhibitors targeting CTLA-4 and PD-1, used both as monotherapies and in combination and aim to provide some general guidelines, based upon the mechanisms of action of these therapies and on the management of these immune-related adverse events.

Published

2016

150. Cardiac troponin I elevation and overall survival among cancer patients receiving investigational compounds during phase I trials.

Author

Hollebecque A, Lanoy E, Troallen F, Soulat-Dufour L, Massard C, Bahleda R, Varga A, Gazzah A, Postel-Vinay S, Ribrag V, Deutsch E, Angevin E, Boccara F, Cohen A, Soria JC, and Ederhy S

Subjects

Antineoplastic Agents therapeutic use, Female, Heart Diseases chemically induced, Humans, Male, Middle Aged, Neoplasms complications, Neoplasms drug therapy, Poisson Distribution, Risk Factors, Survival Analysis, Antineoplastic Agents adverse effects, Heart Diseases metabolism, Neoplasms mortality, Troponin I metabolism

Abstract

Objective: To identify factors associated with troponin elevation and to measure the effect of elevated troponin on survival in cancer patients participating in phase I trials., Methods: Clinical characteristics, cardiovascular risk factors, and biological data from consecutive patients treated in phase I trials (January 2010-November 2012) were reviewed. Troponin value was measured for each patient before study-drug administration and then weekly. Cardiac troponin I was considered elevated if >0.06ng/mL. Incidence and relative risk of elevated troponin adjusted for potential confounding factors were estimated using multivariable Poisson regression models. A conditional Cox proportional hazards model was used to compare overall survival in patients with elevated troponin matched to patients without troponin elevation recruited in the same trial., Results: Of 463 patients, 42 (9%) experienced ≥1 episode of troponin I elevation after a median of 5weeks (interquartile range: 3-13) from drug initiation. Crude incidence of troponin elevation was 36/1000 person-months (95% confidence interval [CI]: 25-47). Troponin elevation was more frequent in patients exposed to antiangiogenic compounds versus other treatments (relative risk: 1.9, 95% CI: 1.1-3.3). Median overall survival from drug initiation was 9months (95% CI: 8-10), and 8months (95% CI: 2-13) in patients with troponin elevation. In the case-control analysis, risk of death was higher in patients with troponin elevation (hazard ratio: 2.9, 95% CI: 1.2-6.8)., Conclusion: Patients exposed to antiangiogenic compounds had a higher risk of troponin elevation, which was associated with a higher risk of death., (Copyright © 2016 Elsevier Ireland Ltd. All rights reserved.)

Published

2016