Your search keyword '"Letouzé E"' showing total 123 results

1. Les mutations d’ARMC5 et KDM1A sont associées à des profils différentiels d’expression de récepteurs illégitimes dans l’hyperplasie macronodulaire bilatérale des surrénales

Author

Bouys, L., primary, Florian, V., additional, Vaczlavik, A., additional, Giannone, G., additional, Jouinot, A., additional, Armignacco, R., additional, Cavalcante, I., additional, Berthon, A., additional, Letouzé, E., additional, Vaduva, P., additional, Barat, M., additional, Bonnet-Serrano, F., additional, Perlemoine, K., additional, Ribes, C., additional, Sibony, M., additional, North, M.O., additional, Espiard, S., additional, Haissaguerre, M., additional, Tauveron, I., additional, Guignat, L., additional, Groussin, L., additional, Dousset, B., additional, Reincke, M., additional, Fragoso, M., additional, Stratakis, C., additional, Pasmant, E., additional, Libé, R., additional, Assié, G., additional, Ragazzon, B., additional, and Bertherat, J., additional

Published

2022

2. Towards a “Lyon molecular signature” to individualize the treatment of rectal cancer. Prognostic analysis of a prospective cohort of 94 rectal cancers T1-2-3 Nx MO to be the basis of a molecular signature

Author

Gérard, J.-P., Baulieux, J., Doyen, J., Gal, J., Letouze, E., Olschwang, S., Chapet, O., and Romestaing, P.

Published

2012

3. HLA-D and PLA2R1 risk alleles associate with recurrent primary membranous nephropathy in kidney transplant recipients

Author

Berchtold, L., Letouzé, E., Alexander, M.P., Canaud, G., Logt, A. van de, Hamilton, P., Mousson, C., Vuiblet, V., Moyer, A.M., Guibert, S. de, Mrázová, P., Levi, C., Dubois, V., Cruzado, J.M., Torres, A. Cedillo, Gandhi, M.J., Yousfi, N., Tesar, V., OndrejViklický, ., Hourmant, M., Moulin, B., Rieu, P., Choukroun, G., Legendre, C., Wetzels, J., Brenchley, P., Castan, J.A. Ballarín, Debiec, H., Ronco, P., Berchtold, L., Letouzé, E., Alexander, M.P., Canaud, G., Logt, A. van de, Hamilton, P., Mousson, C., Vuiblet, V., Moyer, A.M., Guibert, S. de, Mrázová, P., Levi, C., Dubois, V., Cruzado, J.M., Torres, A. Cedillo, Gandhi, M.J., Yousfi, N., Tesar, V., OndrejViklický, ., Hourmant, M., Moulin, B., Rieu, P., Choukroun, G., Legendre, C., Wetzels, J., Brenchley, P., Castan, J.A. Ballarín, Debiec, H., and Ronco, P.

Abstract

Item does not contain fulltext, Recurrence of primary membranous nephropathy after transplantation occurs in up to 44% of patients and is driven by PLA2R antibody. Here, we asked whether genetic determinants could improve risk prediction. First, we sequenced PLA2R1 and HLA-D loci in 248 patients with primary membranous nephropathy and identified two independent single nucleotide polymorphisms (SNPs) at risk for primary membranous nephropathy at each locus. These were rs9271188 (intergenic between HLA-DRB1 and HLA-DQA1,) and rs9275086 (intergenic between HLA-DQB1 and HLA-DQA2) at the HLA-D locus along with rs6726925 and rs13018963 at the PLA2R1 locus. Then we investigated whether primary membranous nephropathy at-risk variants were associated with recurrence in a retrospective cohort of 105 donor-recipient pairs and a replication cohort of 40 pairs. Seven SNPs located between HLA-DRB1 and HLA-DQA1 in linkage disequilibrium with rs9271188, and three SNPs in the PLA2R1 region predicted recurrence when presented by the donor, but not when presented by the recipient. The two SNPs in the HLA-D region most strongly associated with recurrence (rs9271705 and rs9271550) were confirmed in the replication cohort. A genetic risk score based on the two best predictors at each locus (rs9271705, rs9271550, rs17830558, and rs3828323) identified a group of patients with high risk of recurrence. Thus, our results suggest that the graft contributes to recurrence of primary membranous nephropathy through the disease susceptibility HLA-D and PLA2R1 SNPs in an autoimmune milieu. Further studies are needed before implementation of genetic testing for these in donor selection.

Published

2021

4. Analyzing the Effect of Time in Migration Measurement Using Georeferenced Digital Trace Data

Author

Fiorio, L., Zagheni, E., Abel, G., Hill, J., Pestre, G., Letouzé, E., Cai, J., Fiorio, L., Zagheni, E., Abel, G., Hill, J., Pestre, G., Letouzé, E., and Cai, J.

Abstract

Georeferenced digital trace data offer unprecedented flexibility in migration estimation. Because of their high temporal granularity, many migration estimates can be generated from the same data set by changing the definition parameters. Yet despite the growing application of digital trace data to migration research, strategies for taking advantage of their temporal granularity remain largely underdeveloped. In this paper, we provide a general framework for converting digital trace data into estimates of migration transitions and for systematically analyzing their variation along a quasi-continuous time scale, analogous to a survival function. From migration theory, we develop two simple hypotheses regarding how we expect our estimated migration transition functions to behave. We then test our hypotheses on simulated data and empirical data from three platforms in two internal migration contexts: geotagged Tweets and Gowalla check-ins in the United States, and cell-phone call detail records in Senegal. Our results demonstrate the need for evaluating the internal consistency of migration estimates derived from digital trace data before using them in substantive research. At the same time, however, common patterns across our three empirical data sets point to an emergent research agenda using digital trace data to study the specific functional relationship between estimates of migration and time and how this relationship varies by geography and population characteristics.

Published

2021

5. Characterizing the Mobile Phone Use Patterns of Refugee-Hosting Provinces in Turkey

Author

Frydenlund, Erika, Sener, Meltem Y., Gore, Ross, Boshuijzen - van Burken, Christine, Bozdag, Engin, de Kock, Christa, Salah, A.A., Pentland, A., Lepri, B., Letouzé, E., and Philosophy & Ethics

Subjects

rechtvaardigheid en sterke instellingen, SDG 16 - Peace, SDG 16 – Vrede, business.industry, Turkish, Refugee, media_common.quotation_subject, SDG 16 - Peace, Justice and Strong Institutions, Internet privacy, Compassion, Justice and Strong Institutions, language.human_language, Mobile phone, Political science, language, Social media, business, Proxy (statistics), media_common

Abstract

We use coarse-grained mobile phone data from a large Turkish mobile phone provider and cross-reference this data with social media data and a qualitatively composed violent events list to explore the integration of refugees in Turkey. The data provides grounds for fruitful future research. It suggests that border communities with the refugee-sending country have much different communications patterns than non-border communities. Additionally, proximity to refugee camps may increase negative sentiment on social media toward refugees, which we suggest may be a proxy for understanding “compassion fatigue.” These findings provide directions for future research on integration.

Published

2019

6. Introduction to the Data for Refugees Challenge on Mobility of Syrian Refugees in Turkey

Author

Salah, A.A., Pentland, Alex, Lepri, Bruno, Letouzé, E, de Montjoye, Yves-Alexandre, Dong, Xiaowen, Vinck, Patrick, Salah, A.A., Pentland, Alex, Lepri, Bruno, Letouzé, E, de Montjoye, Yves-Alexandre, Dong, Xiaowen, and Vinck, Patrick

Abstract

The Data for Refugees (D4R) Challenge was a nonprofit challenge initiated to improve the conditions of the Syrian refugees in Turkey by providing a special database to scientific community for enabling research on urgent problems concerning refugees, including health, education, unemployment, safety, and social integration. The collected database was based on anonymized mobile Call Detail Record (CDR) of phone calls and SMS messages of Türk Telekom customers. It indicated broad activity and mobility patterns of refugees and citizens in Turkey for 1 year. The data collection period was from January 1, 2017 to December 31, 2017. The project was initiated by Türk Telekom, in partnership with the Turkish Academic and Research Council (TÜBİTAK) and Boğaziçi University, and in collaboration with several academic and nongovernmental organizations, including UNHCR Turkey, UNICEF, and International Organization for Migration. This chapter describes the Challenge in detail, providing a history of its evolution, as well as a description of the data shared with the participants of the Challenge.

Published

2019

7. Introduction to the Data for Refugees Challenge on Mobility of Syrian Refugees in Turkey

Author

Social and Affective Computing, Sub Social and Affective Computing, Salah, A.A., Pentland, Alex, Lepri, Bruno, Letouzé, E, de Montjoye, Yves-Alexandre, Dong, Xiaowen, Vinck, Patrick, Social and Affective Computing, Sub Social and Affective Computing, Salah, A.A., Pentland, Alex, Lepri, Bruno, Letouzé, E, de Montjoye, Yves-Alexandre, Dong, Xiaowen, and Vinck, Patrick

Published

2019

8. L’étude génomique de l’hyperplasie macronodulaire bilatérale primitive des surrénales (HMBPS) révèle 3 groupes aux caractéristiques clinico-pathologiques distinctes, un lié à ARMC5 et un deuxième à un nouveau gène responsable du syndrome de Cushing dépendant de l’alimentation : LSD1/KDM1A, étendant le spectre des causes génétiques du syndrome de Cushing surrénalien

Author

Vaczlavik, A., Bouys, L., Violon, F., Giannone, G., Jouinot, A., Armignacco, R., Cavalcante, I., Berthon, A., Letouze, E., Vaduva, P., Barat, M., Bonnet, F., Perlemoine, K., Ribes, C., Sibony, M., North, M.O., Espiard, S., Emy, P., Haissaguerre, M., Tauveron, I., Guignat, L., Groussin, L., Dousset, B., Lefebvre, H., Reincke, M., Fragoso, M.C., Stratakis, C.A., Pasmant, E., Libé, R., Assié, G., Ragazzon, B., and Bertherat, J.

Published

2021

9. Characterization of the transcriptional and metabolic responses of pediatric high grade gliomas to mTOR-HIF-1a

Author

Nguyen, A., Moussallieh, F. M., Mackay, A., Cicek, A. E., Coca, A., Chenard, M. P., Weingertner, N., Lhermitte, B., Letouzé, E., Guérin, E., Pencreach, E., Jannier, S., Guenot, D., Namer, I. J., Jones, C., and Entz-Werlé, N.

Subjects

Pediatric, Targets, mTor, HIF1alpha, High grade glioma

Abstract

Pediatric high grade glioma (pHGGs), including sus-tentorial and diffuse intrinsic pontine gliomas, are known to have a very dismal prognosis. For instance, even an increased knowledge on molecular biology driving this brain tumor entity, there is no treatment able to cure those patients. Therefore, we were focusing on a translational pathway able to increase the cell resistance to treatment and to reprogram metabolically tumor cells, which are, then, adapting easily to a hypoxic microenvironment. To establish, the crucial role of the hypoxic pathways in pHGGs, we, first, assessed their protein and transcriptomic deregulations in a pediatric cohort of pHGGs and in pHGG’s cell lines, cultured in both normoxic and hypoxic conditions. Secondly, based on the concept of a bi-therapy targeting in pHGGs mTORC1 (rapamycin) and HIF-1α (irinotecan), we hypothesized that the balanced expressions between RAS/ERK, PI3K/AKT and HIF-1α/HIF-2α/MYC proteins or genes may provide a modulation of the cell response to this double targeting. Finally, we could evidence three protein, genomic and metabolomic profiles of response to rapamycin combined with irinotecan. The pattern of highly sensitive cells to mTOR/HIF-1α targeting was linked to a MYC/ERK/HIF-1α over-expression and the cell resistance to a major hyper-expression of HIF-2α.

Published

2017

10. Génomique intégrée des Hyperplasies Macronodulaires Bilatérales primitives des Surrénales (HMBS)

Author

Vaczlavik, A., Bouys, L., Letouze, E., Heurtier, V., Bonnet, F., Letourneur, F., Perlemoine, K., Espiard, S., Guignat, L., Assie, G., Ragazzon, B., and Bertherat, J.

Published

2020

11. Genotype-Phenotype Correlation of CTNNB1 Mutations Reveals Different B-Catenin Activation Levels in Hepatocellular Tumors with High Activity Associated with Malignancy

Author

Rebouissou, S., primary, Franconi, A., additional, Calderaro, J., additional, Letouzé, E., additional, Imbeaud, S., additional, Pilati, C., additional, Nault, J.-C., additional, Couchy, G., additional, Laurent, A., additional, Balabaud, C., additional, Bioulac-Sage, P., additional, and Zucman-Rossi, J., additional

Published

2016

12. G05 : Exome sequencing of 243 liver tumors identifies new mutational signatures and potential therapeutic targets

Author

Schulze, K., primary, Imbeaud, S., additional, Letouzé, E., additional, Alexandrov, L.B., additional, Calderaro, J., additional, Rebouissou, S., additional, Couchy, G., additional, Meiller, C., additional, Soysouvanh, F., additional, Calatayud, A.-L., additional, Pinyol, R., additional, Pelletier, L., additional, Balabaud, C., additional, Laurent, A., additional, Blanc, J.-F., additional, Mazzaferro, V., additional, Calvo, F., additional, Villanueva, A., additional, Nault, J.-C., additional, Bioulac-Sage, P., additional, Stratton, M.R., additional, Llovet, J.M., additional, and Zucman-Rossi, J., additional

Published

2015

13. P0266 : Adeno-Associated Virus 2 (AAV2) induces recurrent insertional mutagenesis in Human Hepatocellular Carcinomas

Author

Nault, J.C., primary, Datta, S., additional, Franconi, A., additional, Imbeaud, S., additional, Mallet, M., additional, Couchy, G., additional, Letouzé, E., additional, Pilati, C., additional, Verret, B., additional, Blanc, J.F., additional, Balabaud, C., additional, Calderaro, J., additional, Laurent, A., additional, Lextexier, M., additional, Bioulac-Sage, P., additional, Calvo, F., additional, and Zucman-Rossi, J., additional

Published

2015

14. Genome-Wide Paternal Uniparental Disomy as a Cause of Beckwith-Wiedemann Syndrome Associated with Recurrent Virilizing Adrenocortical Tumors

Author

Bertoin, F., additional, Letouzé, E., additional, Grignani, P., additional, Patey, M., additional, Rossignol, S., additional, Libé, R., additional, Pasqual, C., additional, Lardière-Deguelte, S., additional, Hoeffel-Fornes, C., additional, Gaillard, D., additional, Previderè, C., additional, Delemer, B., additional, and Lalli, E., additional

Published

2014

15. Recherche pangénomique des gènes impliqués dans les corticosurrénalomes

Author

Assié, G., primary, Letouzé, E., additional, Jouinot, A., additional, Barreau, O., additional, Fassnacht, M., additional, Luscap, W., additional, Omeiri, H., additional, Rodriguez, S., additional, Perlemoine, K., additional, René-Corail, F., additional, Elarouci, N., additional, Sbiera, S., additional, Kroiss, M., additional, Waldmann, J., additional, Quinkler, M., additional, Mannelli, M., additional, Mantero, F., additional, Papathomas, T., additional, Allolio, B., additional, De Krijger, R., additional, Tabarin, A., additional, Kerlan, V., additional, Baudin, E., additional, Tissier, F., additional, Dousset, B., additional, Groussin, L., additional, Amar, L., additional, Clauser, E., additional, Bertagna, X., additional, Ragazzon, B., additional, Beuschlein, F., additional, Libé, R., additional, De Reyniès, A., additional, and Bertherat, J., additional

Published

2014

16. SNP array profiling of childhood adrenocortical tumors reveals distinct pathways of tumorigenesis and highlights candidate driver genes

Author

Letouzé, E. (Eric), Rosati, R. (Roberto), Komechen, H. (Heloisa), Doghman, M. (Mabrouka), Marisa, L. (Laetitia), Flück, C. (Christa), Krijger, R.R. (Ronald) de, Noesel, M.M. (Max) van, Mas, J.-C. (Jean-Christophe), Pianovski, M.A.D. (Mara A.), Zambetti, G.P. (Gerard), Figueiredo, E.G. (Eberval), Lalli, E. (Enzo), Letouzé, E. (Eric), Rosati, R. (Roberto), Komechen, H. (Heloisa), Doghman, M. (Mabrouka), Marisa, L. (Laetitia), Flück, C. (Christa), Krijger, R.R. (Ronald) de, Noesel, M.M. (Max) van, Mas, J.-C. (Jean-Christophe), Pianovski, M.A.D. (Mara A.), Zambetti, G.P. (Gerard), Figueiredo, E.G. (Eberval), and Lalli, E. (Enzo)

Abstract

Context: Childhood adrenocortical tumors (ACT) are rare malignancies, except in southern Brazil, where a higher incidence rate is associated to a high frequency of the founder R337H TP53 mutation. To date, copy number alterations in these tumors have only been analyzed by low-resolution comparative genomic hybridization. Objective: We analyzed an international series of 25 childhood ACT using high-resolution single nucleotide polymorphism arrays to: 1) detect focal copynumberalterations highlighting candidate driver genes; and 2) compare genetic alterations between Brazilian patients carrying the R337H TP53 mutation and non-Brazilian patients. Results: We identified 16 significantly recurrent chromosomal alterations (q-value < 0.05), the mostfrequent being -4q34, +9q33-q34, +19p, loss of heterozygosity (LOH) ofchromosome17and 11p15. Focal amplifications and homozygous deletions comprising well-known oncogenes (MYC, MDM2, PDGFRA, KIT, MCL1, BCL2L1) and tumor suppressors (TP53, RB1, RPH3AL) were identified. In addition, eight focal deletions were detected at 4q34, defining a sharp peak region around the noncodingRNALINC00290 gene. Although non-Brazilian tumors with a mutated TP53 were similar to Brazilian tumors, those with a wild-type TP53 displayed distinct genomic profiles, with significantly fewer rearrangements (P = 0.019). In particular, three alterations (LOH of chromosome 17, +9q33-q34, and -4q34) were significantly more frequent in TP53-mutated samples. Finally, two of four TP53 wild-type tumors displayed as sole rearrangement a copy-neutral LOH of the imprinted region at 11p15, supporting a major role for this region in ACT development. Conclusions: Our findings highlight potential driver genes and cellular pathways implicated in childhood ACT and demonstrate the existence of different oncogenic routes in this pathology. Copyright

Published

2012

17. FRI-088 - Genotype-Phenotype Correlation of CTNNB1 Mutations Reveals Different B-Catenin Activation Levels in Hepatocellular Tumors with High Activity Associated with Malignancy

Author

Rebouissou, S., Franconi, A., Calderaro, J., Letouzé, E., Imbeaud, S., Pilati, C., Nault, J.-C., Couchy, G., Laurent, A., Balabaud, C., Bioulac-Sage, P., and Zucman-Rossi, J.

Published

2016

18. PS116 - Prospective Evidence That Hepatocellular Carcinoma Surveillance in Patients with Compensated Viral Cirrhosis Increases the Probability of Curative Treatment and Survival Taking into Account Lead-Time Bias (Anrs Co12 Cirvir Cohort)

Author

Costentin, C., Layese, R., Bourcier, V., Corvi, L., Petro-Sanchez, V., Marcellin, P., Guyader, D., Pol, S., Larrey, D., de Ledinghen, V., Ouzan, D., Zoulim, F., zarski, J.P., Roulot, D., Tran, A., Bronowicki, J.-P., Riachi, G., Cales, P., Péron, J.M., Alric, L., Bourlière, M., Mathurin, P., Sutton, A., Letouze, E., Zucman-Rossi, J., Roudot-Thoraval, F., and Nahon, P.

Published

2016

19. Disomie paternelle pangénomique en mosaïque : nouveau mécanisme de tumorigénèse surrénalienne dans le syndrome de Beckwith–Wiedemann ?

Author

Bertoin, F., primary, Patey, M., additional, Letouzé, E., additional, Gaillard, D., additional, Libé, R., additional, Delemer, B., additional, and Lalli, E., additional

Published

2013

20. PD-0608: Risk of metastasis and death in rectal cancer is increased with 8p deletion but not with gene expression

Author

Doyen, J., primary, Letouzé, E., additional, Marisa, L., additional, De Reyniès, A., additional, Milano, G., additional, Etienne-Grimaldi, M., additional, Selves, J., additional, Chapet, O., additional, Olschwang, S., additional, and Gérard, J., additional

Published

2013

21. Genome-Wide Paternal Uniparental Disomy as a Cause of Beckwith-Wiedemann Syndrome Associated with Recurrent Virilizing Adrenocortical Tumors.

Author

Bertoin, F., Letouzé, E., Grignani, P., Patey, M., Rossignol, S., Libé, R., Pasqual, C., Lardière-Deguelte, S., Hoeffel-Fornes, C., Gaillard, D., Previderè, C., Delemer, B., and Lalli, E.

Subjects

*BECKWITH-Wiedemann syndrome, *FIBROADENOMAS, *LOSS of heterozygosity, *DISEASE relapse, *HUMAN genome, *NEPHROBLASTOMA, TUMOR surgery

Abstract

Beckwith-Wiedemann syndrome (BWS) is an overgrowth syndrome characterized by fetal macrosomia, macroglossia, and abdominal wall defects. BWS patients are at risk to develop Wilms tumor, neuroblastoma, hepatoblastoma, and adrenal tumors. A young woman with BWS features, but with inconclusive genetic evidence for the disease, came to clinical observation for signs of virilization at the age of 16 years. An adrenocortical tumor was diagnosed and surgically resected. The tumor underwent 2 local relapses that were also surgically treated. The patient was also operated to remove a breast fibroadenoma. SNP arrays were used to analyze chromosome abnormalities in normal and tumor samples from the patient and her parents. The patient presented genome-wide mosaic paternal uniparental disomy (patUPD) both in the adrenocortical and the breast tumors, with different degrees of loss of heterozygosity (LOH). The more recent relapses of the adrenocortical tumor showed a loss of part of chromosome 17p that was absent in the first tumor. Analysis of a skin biopsy sample also showed mosaic patUPD with partial LOH, while no LOH was detected in leukocyte DNA. This case shows that virilizing adrenocortical tumors may be a clinical feature of patients with BWS. The SNP array technology is useful to diagnose genome-wide patUPD mosaicism in BWS patients with an inconclusive molecular diagnosis and underlines the tumorigenic potential of the absence of the maternal genome combined with an excess of the paternal genome. [ABSTRACT FROM AUTHOR]

Published

2015

22. L’Epidermal Growth Factor Receptor (EGFR) est une cible thérapeutique pour un sous-groupe de tumeurs de vessie agressives de phénotype de type basal

Author

Neuzillet, Y., Rebouissou, S., De Reynies, A., Lepage, M., Krucker, C., Chapeaublanc, E., Herault, A., Kamoun, A., Caillault, A., Letouze, E., Elarouci, N., Decoux, Y., Molinie, V., Vordos, D., Laplanche, A., Maille, P., Soyeux, P., Ofualuka, K., Reyal, F., Biton, A., Sibony, M., Paoletti, X., Southgate, J., Benhamou, S., Allory, Y., Radvanyi, F., and Lebret, T.

Published

2014

23. Étude par Reverse Phase Protein Array (RPPA) de l’activation de la voie PI3K/AKT dans le carcinome urothélial de la vessie

Author

Calderaro, J., de Koening, L., Bernard-Pierrot, I., Rebouissou, S., Letouze, E., Dubois, T., Maille, P., Soyeux, P., Vordos, D., de la Taille, A., Benhamou, S., Lebret, T., Radvanyi, F., and Allory, Y.

Published

2011

24. 170 oral TOWARDS A LYON MOLECULAR PROGNOSTIC SIGNATURE FOR RECTAL CANCER

Author

Doyen, J., Letouze, E., Romestaing, P., Chapet, O., and Gerard, J.P.

Published

2011

25. Integration of Syrian Refugees: Insights from D4R, Media Events and Housing Market Data

Author

Biagio Speciale, Simone Bertoli, Dino Pedreschi, Etienne Madinier, Hillel Rapoport, Michael Packard, Alina Sîrbu, Paolo Cintia, Fosca Giannotti, Caglar Ozden, Centre d'Études et de Recherches sur le Développement International - Clermont Auvergne (CERDI), Université Clermont Auvergne (UCA)-Centre National de la Recherche Scientifique (CNRS), Istituto di Scienza e Tecnologie dell'Informazione 'A. Faedo', The World Bank, University of Pisa - Università di Pisa, Paris School of Economics (PSE), Paris Jourdan Sciences Economiques (PJSE), Université Panthéon-Sorbonne (UP1)-École normale supérieure - Paris (ENS Paris)-Institut National de la Recherche Agronomique (INRA)-École des hautes études en sciences sociales (EHESS)-École des Ponts ParisTech (ENPC)-Centre National de la Recherche Scientifique (CNRS), Albert Ali Salah, Alex Pentland, Bruno Lepri, Emmanuel Letouzé, Salah A., Pentland A., Lepri B., Letouzé E., Bertoli, Simone, Cintia, Paolo, Giannotti, Fosca, Madinier, Etienne, Ozden, Caglar, Packard, Michael, Pedreschi, Dino, Rapoport, Hillel, Sîrbu, Alina, Speciale, Biagio, Centre d'Études et de Recherches sur le Développement International (CERDI), Université Clermont Auvergne [2017-2020] (UCA [2017-2020])-Centre National de la Recherche Scientifique (CNRS), CNR Istituto di Scienza e Tecnologie dell’Informazione 'A. Faedo' [Pisa] (CNR | ISTI), National Research Council of Italy | Consiglio Nazionale delle Ricerche (CNR), Université Paris 1 Panthéon-Sorbonne (UP1)-École normale supérieure - Paris (ENS-PSL), Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-École des hautes études en sciences sociales (EHESS)-École des Ponts ParisTech (ENPC)-Centre National de la Recherche Scientifique (CNRS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Georgetown University [Washington] (GU), Istituto di Biofisica [Pisa] (IBF), Salah A., Pentland A., Lepri B., Letouzé E., Centre National de la Recherche Scientifique (CNRS)-Université Clermont Auvergne [2017-2020] (UCA [2017-2020]), Consiglio Nazionale delle Ricerche [Roma] (CNR), École des Ponts ParisTech (ENPC)-École normale supérieure - Paris (ENS Paris), and Université Paris sciences et lettres (PSL)-Université Paris sciences et lettres (PSL)-Université Paris 1 Panthéon-Sorbonne (UP1)-Centre National de la Recherche Scientifique (CNRS)-École des hautes études en sciences sociales (EHESS)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)

Subjects

050402 sociology, Syrian refugees, Settore INF/01 - Informatica, 05 social sciences, We explore various means of quantifying integration using two of the D4R Challenge datasets. We propose various integration indices and discuss their output. We combine the data from the D4R Challenge with data from the GDELT Project and with data on transactions on the housing market in Turkey. We also describe research directions to be undertaken in the future using the D4R data, [SHS.ECO]Humanities and Social Sciences/Economics and Finance, 0504 sociology, 0502 economics and business, Market data, Regional science, Business, 050207 economics, Media event

Abstract

International audience; We explore various means of quantifying integration using two of the D4R Challenge datasets. We propose various integration indices and discuss their output. We combine the data from the D4R Challenge with data from the GDELT Project and with data on transactions on the housing market in Turkey. We also describe research directions to be undertaken in the future using the D4R data.

Published

2019

26. Role and timing of chromosome deletions in multiple myeloma.

Author

Minvielle S and Letouzé E

Subjects

Humans, Time Factors, Male, Female, Multiple Myeloma genetics, Multiple Myeloma pathology, Chromosome Deletion

Published

2024

27. Mechanisms of resistance to bispecific T-cell engagers in multiple myeloma and their clinical implications.

Author

Letouzé E, Moreau P, Munshi N, Samur M, Minvielle S, and Touzeau C

Subjects

Humans, Drug Resistance, Neoplasm, Immunotherapy methods, Tumor Microenvironment immunology, Animals, Multiple Myeloma therapy, Multiple Myeloma immunology, T-Lymphocytes immunology, T-Lymphocytes metabolism, Antibodies, Bispecific therapeutic use, Antibodies, Bispecific pharmacology

Abstract

Abstract: Bispecific T-cell engagers (TCEs) are revolutionizing patient care in multiple myeloma (MM). These monoclonal antibodies, that redirect T cells against cancer cells, are now approved for the treatment of triple-class exposed relapsed/refractory MM (RRMM). They are currently tested in earlier lines of the disease, including in first line. Yet, primary resistance occurs in about one-third of patients with RRMM, and most responders eventually develop acquired resistance. Understanding the mechanisms of resistance to bispecific TCE is thus essential to improve immunotherapies in MM. Here, we review recent studies investigating the clinical and molecular determinants of resistance to bispecific TCE. Resistance can arise from tumor-intrinsic or tumor-extrinsic mechanisms. Tumor-intrinsic resistance involves various alterations leading to the loss of the target antigen, such as chromosome deletions, point mutations, or epigenetic silencing. Loss of major histocompatibility complex (MHC) class I, preventing MHC class I: T-cell receptor (TCR) costimulatory signaling, was also reported. Tumor-extrinsic resistance involves abundant exhausted T-cell clones and several factors generating an immunosuppressive microenvironment. Importantly, some resistance mechanisms impair response to 1 TCE while preserving the efficacy of others. We next discuss the clinical implications of these findings. Monitoring the status of target antigens in tumor cells and their immune environment will be key to select the most appropriate TCE for each patient and to design combination and sequencing strategies for immunotherapy in MM., (© 2024 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved.)

Published

2024

28. Single-cell multiomics reveals the interplay of clonal evolution and cellular plasticity in hepatoblastoma.

Author

Roehrig A, Hirsch TZ, Pire A, Morcrette G, Gupta B, Marcaillou C, Imbeaud S, Chardot C, Gonzales E, Jacquemin E, Sekiguchi M, Takita J, Nagae G, Hiyama E, Guérin F, Fabre M, Aerts I, Taque S, Laithier V, Branchereau S, Guettier C, Brugières L, Fresneau B, Zucman-Rossi J, and Letouzé E

Subjects

Humans, Cell Plasticity genetics, Multiomics, Clonal Evolution genetics, Hepatoblastoma genetics, Liver Neoplasms genetics, Liver Neoplasms pathology

Abstract

Hepatoblastomas (HB) display heterogeneous cellular phenotypes that influence the clinical outcome, but the underlying mechanisms are poorly understood. Here, we use a single-cell multiomic strategy to unravel the molecular determinants of this plasticity. We identify a continuum of HB cell states between hepatocytic (scH), liver progenitor (scLP) and mesenchymal (scM) differentiation poles, with an intermediate scH/LP population bordering scLP and scH areas in spatial transcriptomics. Chromatin accessibility landscapes reveal the gene regulatory networks of each differentiation pole, and the sequence of transcription factor activations underlying cell state transitions. Single-cell mapping of somatic alterations reveals the clonal architecture of each tumor, showing that each genetic subclone displays its own range of cellular plasticity across differentiation states. The most scLP subclones, overexpressing stem cell and DNA repair genes, proliferate faster after neo-adjuvant chemotherapy. These results highlight how the interplay of clonal evolution and epigenetic plasticity shapes the potential of HB subclones to respond to chemotherapy., (© 2024. The Author(s).)

Published

2024

29. Preneoplastic liver colonization by 11p15.5 altered mosaic cells in young children with hepatoblastoma.

Author

Pilet J, Hirsch TZ, Gupta B, Roehrig A, Morcrette G, Pire A, Letouzé E, Fresneau B, Taque S, Brugières L, Branchereau S, Chardot C, Aerts I, Sarnacki S, Fabre M, Guettier C, Rebouissou S, and Zucman-Rossi J

Subjects

Humans, Child, Child, Preschool, Mosaicism, DNA Methylation, Genomic Imprinting, Tumor Microenvironment, Hepatoblastoma genetics, Beckwith-Wiedemann Syndrome diagnosis, Beckwith-Wiedemann Syndrome genetics, Beckwith-Wiedemann Syndrome pathology, Liver Neoplasms genetics

Abstract

Pediatric liver tumors are very rare tumors with the most common diagnosis being hepatoblastoma. While hepatoblastomas are predominantly sporadic, around 15% of cases develop as part of predisposition syndromes such as Beckwith-Wiedemann (11p15.5 locus altered). Here, we identify mosaic genetic alterations of 11p15.5 locus in the liver of hepatoblastoma patients without a clinical diagnosis of Beckwith-Wiedemann syndrome. We do not retrieve these alterations in children with other types of pediatric liver tumors. We show that mosaic 11p15.5 alterations in liver FFPE sections of hepatoblastoma patients display IGF2 overexpression and H19 downregulation together with an alteration of the liver zonation. Moreover, mosaic livers' microenvironment is enriched in extracellular matrix and angiogenesis. Spatial transcriptomics and single-nucleus RNAseq analyses identify a 60-gene signature in 11p15.5 altered hepatocytes. These data provide insights for 11p15.5 mosaicism detection and its functional consequences during the early steps of carcinogenesis., (© 2023. The Author(s).)

Published

2023

30. Author Correction: Acquired resistance to a GPRC5D-directed T-cell engager in multiple myeloma is mediated by genetic or epigenetic target inactivation.

Author

Derrien J, Gastineau S, Frigout A, Giordano N, Cherkaoui M, Gaborit V, Boinon R, Douillard E, Devic M, Magrangeas F, Moreau P, Minvielle S, Touzeau C, and Letouzé E

Published

2023

31. Acquired resistance to a GPRC5D-directed T-cell engager in multiple myeloma is mediated by genetic or epigenetic target inactivation.

Author

Derrien J, Gastineau S, Frigout A, Giordano N, Cherkaoui M, Gaborit V, Boinon R, Douillard E, Devic M, Magrangeas F, Moreau P, Minvielle S, Touzeau C, and Letouzé E

Subjects

Humans, Epigenesis, Genetic, Immunotherapy methods, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled immunology, T-Lymphocytes, Antibodies, Bispecific therapeutic use, Multiple Myeloma genetics, Multiple Myeloma therapy

Abstract

Bispecific antibodies targeting GPRC5D demonstrated promising efficacy in multiple myeloma, but acquired resistance usually occurs within a few months. Using a single-nucleus multi-omic strategy in three patients from the MYRACLE cohort (ClinicalTrials.gov registration: NCT03807128 ), we identified two resistance mechanisms, by bi-allelic genetic inactivation of GPRC5D or by long-range epigenetic silencing of its promoter and enhancer regions. Molecular profiling of target genes may help to guide the choice of immunotherapy and early detection of resistance in multiple myeloma., (© 2023. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2023

32. Discovering cryptic splice mutations in cancers via a deep neural network framework.

Author

Teboul R, Grabias M, Zucman-Rossi J, and Letouzé E

Abstract

Somatic mutations can disrupt splicing regulatory elements and have dramatic effects on cancer genes, yet the functional consequences of mutations located in extended splice regions is difficult to predict. Here, we use a deep neural network (SpliceAI) to characterize the landscape of splice-altering mutations in cancer. In our in-house series of 401 liver cancers, SpliceAI uncovers 1244 cryptic splice mutations, located outside essential splice sites, that validate at a high rate (66%) in matched RNA-seq data. We then extend the analysis to a large pan-cancer cohort of 17 714 tumors, revealing >100 000 cryptic splice mutations. Taking into account these mutations increases the power of driver gene discovery, revealing 126 new candidate driver genes. It also reveals new driver mutations in known cancer genes, doubling the frequency of splice alterations in tumor suppressor genes. Mutational signature analysis suggests mutational processes that could give rise preferentially to splice mutations in each cancer type, with an enrichment of signatures related to clock-like processes and DNA repair deficiency. Altogether, this work sheds light on the causes and impact of cryptic splice mutations in cancer, and highlights the power of deep learning approaches to better annotate the functional consequences of mutations in oncology., (© The Author(s) 2023. Published by Oxford University Press on behalf of NAR Cancer.)

Published

2023

33. Using Facebook advertising data to describe the socio-economic situation of Syrian refugees in Lebanon.

Author

Fatehkia M, Del Villar Z, Koebe T, Letouzé E, Lozano A, Al Feel R, Mrad F, and Weber I

Abstract

While the fighting in the Syrian civil war has mostly stopped, an estimated 5.6 million Syrians remain living in neighboring countries. Of these, an estimated 1.5 million are sheltering in Lebanon. Ongoing efforts by organizations such as UNHCR to support the refugee population are often ineffective in reaching those most in need. According to UNHCR's 2019 Vulnerability Assessment of Syrian Refugees Report (VASyR), only 44% of the Syrian refugee families eligible for multipurpose cash assistance were provided with help, as the others were not captured in the data. In this project, we are investigating the use of non-traditional data, derived from Facebook advertising data, for population level vulnerability assessment. In a nutshell, Facebook provides advertisers with an estimate of how many of its users match certain targeting criteria, e.g., how many Facebook users currently living in Beirut are "living abroad," aged 18-34, speak Arabic, and primarily use an iOS device. We evaluate the use of such audience estimates to describe the spatial variation in the socioeconomic situation of Syrian refugees across Lebanon. Using data from VASyR as ground truth, we find that iOS device usage explains 90% of the out-of-sample variance in poverty across the Lebanese governorates. However, evaluating predictions at a smaller spatial resolution also indicate limits related to sparsity, as Facebook, for privacy reasons, does not provide audience estimates for fewer than 1,000 users. Furthermore, comparing the population distribution by age and gender of Facebook users with that of the Syrian refugees from VASyR suggests an under-representation of Syrian women on the social media platform. This work adds to growing body of literature demonstrating the value of anonymous and aggregate Facebook advertising data for analysing large-scale humanitarian crises and migration events., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Fatehkia, del Villar, Koebe, Letouzé, Lozano, Al Feel, Mrad and Weber.)

Published

2022

34. Hepatocellular Carcinoma in Mongolia Delineates Unique Molecular Traits and a Mutational Signature Associated with Environmental Agents.

Author

Torrens L, Puigvehí M, Torres-Martín M, Wang H, Maeda M, Haber PK, Leonel T, García-López M, Esteban-Fabró R, Leow WQ, Montironi C, Torrecilla S, Varadarajan AR, Taik P, Campreciós G, Enkhbold C, Taivanbaatar E, Yerbolat A, Villanueva A, Pérez-Del-Pulgar S, Thung S, Chinburen J, Letouzé E, Zucman-Rossi J, Uzilov A, Neely J, Forns X, Roayaie S, Sia D, and Llovet JM

Subjects

Apolipoproteins B genetics, Coal, Female, Humans, Mongolia epidemiology, Mutation, Carcinoma, Hepatocellular etiology, Carcinoma, Hepatocellular genetics, Liver Neoplasms etiology, Liver Neoplasms genetics

Abstract

Purpose: Mongolia has the world's highest incidence of hepatocellular carcinoma (HCC), with ∼100 cases/100,000 inhabitants, although the reasons for this have not been thoroughly delineated., Experimental Design: We performed a molecular characterization of Mongolian (n = 192) compared with Western (n = 187) HCCs by RNA sequencing and whole-exome sequencing to unveil distinct genomic and transcriptomic features associated with environmental factors in this population., Results: Mongolian patients were younger, with higher female prevalence, and with predominantly HBV-HDV coinfection etiology. Mongolian HCCs presented significantly higher rates of protein-coding mutations (121 vs. 70 mutations per tumor in Western), and in specific driver HCC genes (i.e., APOB and TSC2). Four mutational signatures characterized Mongolian samples, one of which was novel (SBS Mongolia) and present in 25% of Mongolian HCC cases. This signature showed a distinct substitution profile with a high proportion of T>G substitutions and was significantly associated with a signature of exposure to the environmental agent dimethyl sulfate (71%), a 2A carcinogenic associated with coal combustion. Transcriptomic-based analysis delineated three molecular clusters, two not present in Western HCC; one with a highly inflamed profile and the other significantly associated with younger female patients., Conclusions: Mongolian HCC has unique molecular traits with a high mutational burden and a novel mutational signature associated with genotoxic environmental factors present in this country., (©2022 American Association for Cancer Research.)

Published

2022

35. Bi-allelic hydroxymethylbilane synthase inactivation defines a homogenous clinico-molecular subtype of hepatocellular carcinoma.

Author

Molina L, Zhu J, Trépo E, Bayard Q, Amaddeo G, Blanc JF, Calderaro J, Ma X, Zucman-Rossi J, and Letouzé E

Subjects

Female, Heme, Humans, Hydroxymethylbilane Synthase genetics, Mutation, Oxygen, Porphobilinogen, beta Catenin genetics, Carcinoma, Hepatocellular complications, Carcinoma, Hepatocellular genetics, Liver Neoplasms complications, Liver Neoplasms genetics, Porphyria, Acute Intermittent etiology, Porphyria, Acute Intermittent genetics

Abstract

Background & Aims: Acute intermittent porphyria (AIP), caused by heterozygous germline mutations of the heme synthesis pathway enzyme HMBS (hydroxymethylbilane synthase), confers a high risk of hepatocellular carcinoma (HCC) development. Yet, the role of HMBS in liver tumorigenesis remains unclear., Methods: Herein, we explore HMBS alterations in a large series of 758 HCC cases, including 4 patients with AIP. We quantify the impact of HMBS mutations on heme biosynthesis pathway intermediates and we investigate the molecular and clinical features of HMBS-mutated tumors., Results: We identify recurrent bi-allelic HMBS inactivation, both in patients with AIP acquiring a second somatic HMBS mutation and in sporadic HCC with 2 somatic hits. HMBS alterations are enriched in truncating mutations, in particular in splice regions, leading to abnormal transcript structures. Bi-allelic HMBS inactivation results in a massive accumulation of its toxic substrate porphobilinogen and synergizes with CTNNB1-activating mutations, leading to the development of well-differentiated tumors with a transcriptomic signature of Wnt/β-catenin pathway activation and a DNA methylation signature related to ageing. HMBS-inactivated HCC mostly affects females, in the absence of fibrosis and classical HCC risk factors., Conclusions: These data identify HMBS as a tumor suppressor gene whose bi-allelic inactivation defines a homogenous clinical and molecular HCC subtype., Lay Summary: Heme (the precursor to hemoglobin, which plays a key role in oxygen transport around the body) synthesis occurs in the liver and involves several enzymes including hydroxymethylbilane synthase (HMBS). HMBS mutations cause acute intermittent porphyria, a disease caused by the accumulation of toxic porphyrin precursors. Herein, we show that HMBS inactivation is also involved in the development of liver cancers with distinct clinical and molecular characteristics., Competing Interests: Conflict of interest The authors declare that they have no competing interests. Please refer to the accompanying ICMJE disclosure forms for further details., (Copyright © 2022 European Association for the Study of the Liver. Published by Elsevier B.V. All rights reserved.)

Published

2022

36. Detection of acquired TERT amplification in addition to predisposing p53 and Rb pathways alterations in EGFR-mutant lung adenocarcinomas transformed into small-cell lung cancers.

Author

Mc Leer A, Foll M, Brevet M, Antoine M, Novello S, Mondet J, Cadranel J, Girard N, Giaj Levra M, Demontrond P, Audigier-Valette C, Letouzé E, Lantuéjoul S, Fernandez-Cuesta L, and Moro-Sibilot D

Subjects

Drug Resistance, Neoplasm genetics, ErbB Receptors genetics, Humans, Mutation, Protein Kinase Inhibitors therapeutic use, Retinoblastoma Protein metabolism, Tumor Suppressor Protein p53 genetics, Adenocarcinoma of Lung pathology, Carcinoma, Small Cell drug therapy, Lung Neoplasms pathology, Small Cell Lung Carcinoma drug therapy, Telomerase genetics, Telomerase therapeutic use

Abstract

Introduction: Among the different mechanisms of acquired resistance to EGFR tyrosine kinase inhibitors (TKIs) reported in EGFR-mutated lung adenocarcinoma (EGFR-LUAD) patients, histological transformation into small cell carcinoma (SCLC) occurs in 3-14% of resistant cases, regardless of the generation of EGFR-TKI. In recent studies, bi-allelic inactivation of TP53 and RB1 has been identified in a vast majority of transformed SCLCs. However, the molecular mechanisms driving this histologic transformation remain largely unknown, mainly due to the rarity of samples., Patients and Methods: Out of an initial cohort of 64 patients, tumor tissues of adequate quality and quantity for whole exome sequencing (WES) analysis were available for nine tumors for six patients: paired pre- and post-SCLC transformation samples for three Patients and post-SCLC transformation samples for three other patients., Results: Mutational analyses showed concurrent TP53 mutations and Rb pathway alterations in five of the six patients analyzed, confirming their suggested role as predisposing genetic alterations to SCLC transformation. In addition, TERT amplification was detected in four of the six patients and found to be an event acquired during SCLC transformation. Clonal history evolution analyses from the paired LUAD/SCLC samples showed different evolution patterns. In two patients, a large proportion of mutations were present in the most recent common ancestor cell of the initial LUAD and the transformed SCLC clones, whereas in the third patient, few clonal mutations were common between the LUAD and SCLC samples and the ancestor clone that lead to SCLC was present at low frequency in the initial LUAD., Conclusion: Despite varied clinical presentations and clonal history evolution patterns, in addition to p53 and Rb pathways alterations, TERT amplification emerged as another common genetic mechanism of EGFR-LUAD to SCLC transformation in our cohort, and could represent a candidate therapeutic target in this subset of SCLC tumors., (Copyright © 2022. Published by Elsevier B.V.)

Published

2022

37. Structure, Dynamics, and Impact of Replication Stress-Induced Structural Variants in Hepatocellular Carcinoma.

Author

Bayard Q, Cordier P, Péneau C, Imbeaud S, Hirsch TZ, Renault V, Nault JC, Blanc JF, Calderaro J, Desdouets C, Zucman-Rossi J, and Letouzé E

Subjects

Cyclins, Humans, Oncogenes, Whole Genome Sequencing, Carcinoma, Hepatocellular genetics, Carcinoma, Hepatocellular pathology, Liver Neoplasms genetics, Liver Neoplasms pathology

Abstract

Oncogene activation leads to replication stress and promotes genomic instability. Here we combine optical mapping and whole-genome sequencing (WGS) to explore in depth the nature of structural variants (SV) induced by replication stress in cyclin-activated hepatocellular carcinomas (CCN-HCC). In addition to classical tandem duplications, CCN-HCC displayed frequent intra-chromosomal and interchromosomal templated insertion cycles (TIC), likely resulting from template switching events. Template switching preferentially involves active topologically associated domains that are proximal to one another within the 3D genome. Template sizes depend on the type of cyclin activation and are coordinated within each TIC. Replication stress induced continuous accumulation of SVs during CCN-HCC progression, fostering the acquisition of new driver alterations and large-scale copy-number changes at TIC borders. Together, this analysis sheds light on the mechanisms, dynamics, and consequences of SV accumulation in tumors with oncogene-induced replication stress., Significance: Optical mapping and whole-genome sequencing integration unravels a unique signature of replication stress-induced structural variants that drive genomic evolution and the acquisition of driver events in CCN-HCC., (©2022 American Association for Cancer Research.)

Published

2022

38. H3K27me3 conditions chemotolerance in triple-negative breast cancer.

Author

Marsolier J, Prompsy P, Durand A, Lyne AM, Landragin C, Trouchet A, Bento ST, Eisele A, Foulon S, Baudre L, Grosselin K, Bohec M, Baulande S, Dahmani A, Sourd L, Letouzé E, Salomon AV, Marangoni E, Perié L, and Vallot C

Subjects

Humans, Lysine metabolism, Methylation, Neoplasm Recurrence, Local, Drug Resistance, Neoplasm genetics, Histones genetics, Histones metabolism, Triple Negative Breast Neoplasms drug therapy, Triple Negative Breast Neoplasms genetics

Abstract

The persistence of cancer cells resistant to therapy remains a major clinical challenge. In triple-negative breast cancer, resistance to chemotherapy results in the highest recurrence risk among breast cancer subtypes. The drug-tolerant state seems largely defined by nongenetic features, but the underlying mechanisms are poorly understood. Here, by monitoring epigenomes, transcriptomes and lineages with single-cell resolution, we show that the repressive histone mark H3K27me3 (trimethylation of histone H3 at lysine 27) regulates cell fate at the onset of chemotherapy. We report that a persister expression program is primed with both H3K4me3 (trimethylation of histone H3 at lysine 4) and H3K27me3 in unchallenged cells, with H3K27me3 being the lock to its transcriptional activation. We further demonstrate that depleting H3K27me3 enhances the potential of cancer cells to tolerate chemotherapy. Conversely, preventing H3K27me3 demethylation simultaneously to chemotherapy inhibits the transition to a drug-tolerant state, and delays tumor recurrence in vivo. Our results highlight how chromatin landscapes shape the potential of cancer cells to respond to initial therapy., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2022

39. Comprehensive characterization of viral integrations and genomic aberrations in HBV-infected intrahepatic cholangiocarcinomas.

Author

An J, Kim D, Oh B, Oh YJ, Song J, Park N, Kim HI, Kang HJ, Oh JH, Kim W, Lee E, Sung CO, Song GW, Kim DG, Yu E, Letouzé E, Zucman-Rossi J, Lee HC, and Shim JH

Subjects

Bile Ducts, Intrahepatic pathology, Carcinogenesis, Genomics, Hepatitis B virus genetics, Humans, Virus Integration genetics, Bile Duct Neoplasms genetics, Bile Duct Neoplasms pathology, Carcinoma, Hepatocellular pathology, Cholangiocarcinoma genetics, Cholangiocarcinoma pathology, Liver Neoplasms genetics, Liver Neoplasms pathology

Abstract

Background and Aims: Despite the epidemiological association between intrahepatic cholangiocarcinoma (iCCA) and HBV infection, little is known about the relevant oncogenic effects. We sought to identify the landscape and mechanism of HBV integration, along with the genomic architecture of HBV-infected iCCA (HBV-iCCA) tumors., Approach and Results: We profiled a cohort of 108 HBV-iCCAs using whole-genome sequencing, deep sequencing, and RNA sequencing, together with preconstructed data sets of HBV-infected HCC (HBV-HCC; n = 167) and combined hepatocellular cholangiocarcinoma (HBV-cHCC/CCA; n = 59), and conventional (n = 154) and fluke-related iCCAs (n = 16). Platforms based on primary iCCA cell lines to evaluate the functional effects of chimeric transcripts were also used. We found that HBV had inserted at multiple sites in the iCCA genomes in 45 (41.7%) of the tumors. Recurrent viral integration breakpoints were found at nine different sites. The most common insertional hotspot (7 tumors) was in the TERT (telomerase reverse transcriptase) promoter, where insertions and mutations (11 tumors) were mutually exclusive, and were accompanied by promoter hyperactivity. Recurrent HBV integration events (5 tumors) were also detected in FAT2 (FAT atypical cadherin 2), and were associated with enrichment of epithelial-mesenchymal transition-related genes. A distinctive intergenic insertion (chr9p21.3), between DMRTA1 (DMRT like family A1) and LINC01239 (long intergenic non-protein coding RNA 1239), had oncogenic effects through activation of the mammalian target of rapamycin (mTOR)/4EBP/S6K pathway. Regarding the mutational profiles of primary liver cancers, the overall landscape of HBV-iCCA was closer to that of nonviral conventional iCCA, than to HBV-HCC and HBV-cHCC/CCA., Conclusions: Our findings provide insight into the behavior of iCCAs driven by various pathogenic mechanisms involving HBV integration events and associated genomic aberrations. This knowledge should be of use in managing HBV carriers., (© 2021 American Association for the Study of Liver Diseases.)

Published

2022

40. Hepatitis B virus integrations promote local and distant oncogenic driver alterations in hepatocellular carcinoma.

Author

Péneau C, Imbeaud S, La Bella T, Hirsch TZ, Caruso S, Calderaro J, Paradis V, Blanc JF, Letouzé E, Nault JC, Amaddeo G, and Zucman-Rossi J

Subjects

Carcinogenesis, Case-Control Studies, Cohort Studies, DNA, Viral isolation & purification, Female, Hepatitis B virus isolation & purification, Humans, Male, Carcinoma, Hepatocellular pathology, Carcinoma, Hepatocellular virology, Hepatitis B virus physiology, Liver Neoplasms pathology, Liver Neoplasms virology, Virus Integration physiology

Abstract

Objective: Infection by HBV is the main risk factor for hepatocellular carcinoma (HCC) worldwide. HBV directly drives carcinogenesis through integrations in the human genome. This study aimed to precisely characterise HBV integrations, in relation with viral and host genomics and clinical features., Design: A novel pipeline was set up to perform viral capture on tumours and non-tumour liver tissues from a French cohort of 177 patients mainly of European and African origins. Clonality of each integration event was determined with the localisation, orientation and content of the integrated sequence. In three selected tumours, complex integrations were reconstructed using long-read sequencing or Bionano whole genome mapping., Results: Replicating HBV DNA was more frequently detected in non-tumour tissues and associated with a higher number of non-clonal integrations. In HCC, clonal selection of HBV integrations was related to two different mechanisms involved in carcinogenesis. First, integration of viral enhancer nearby a cancer-driver gene may lead to a strong overexpression of oncogenes. Second, we identified frequent chromosome rearrangements at HBV integration sites leading to cancer-driver genes ( TERT, TP53, MYC ) alterations at distance. Moreover, HBV integrations have direct clinical implications as HCC with a high number of insertions develop in young patients and have a poor prognosis., Conclusion: Deep characterisation of HBV integrations in liver tissues highlights new HBV-associated driver mechanisms involved in hepatocarcinogenesis. HBV integrations have multiple direct oncogenic consequences that remain an important challenge for the follow-up of HBV-infected patients., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published

2022

41. KDM1A inactivation causes hereditary food-dependent Cushing syndrome.

Author

Vaczlavik A, Bouys L, Violon F, Giannone G, Jouinot A, Armignacco R, Cavalcante IP, Berthon A, Letouzé E, Vaduva P, Barat M, Bonnet F, Perlemoine K, Ribes C, Sibony M, North MO, Espiard S, Emy P, Haissaguerre M, Tauveron I, Guignat L, Groussin L, Dousset B, Reincke M, Fragoso MC, Stratakis CA, Pasmant E, Libé R, Assié G, Ragazzon B, and Bertherat J

Subjects

Armadillo Domain Proteins genetics, Histone Demethylases genetics, Humans, Hyperplasia, Phenotype, Cushing Syndrome diagnosis, Cushing Syndrome genetics, Cushing Syndrome surgery

Abstract

Purpose: This study aimed to investigate the genetic cause of food-dependent Cushing syndrome (FDCS) observed in patients with primary bilateral macronodular adrenal hyperplasia (PBMAH) and adrenal ectopic expression of the glucose-dependent insulinotropic polypeptide receptor. Germline ARMC5 alterations have been reported in about 25% of PBMAH index cases but are absent in patients with FDCS., Methods: A multiomics analysis of PBMAH tissues from 36 patients treated by adrenalectomy was performed (RNA sequencing, single-nucleotide variant array, methylome, miRNome, exome sequencing)., Results: The integrative analysis revealed 3 molecular groups with different clinical features, namely G1, comprising 16 patients with ARMC5 inactivating variants; G2, comprising 6 patients with FDCS with glucose-dependent insulinotropic polypeptide receptor ectopic expression; and G3, comprising 14 patients with a less severe phenotype. Exome sequencing revealed germline truncating variants of KDM1A in 5 G2 patients, constantly associated with a somatic loss of the KDM1A wild-type allele on 1p, leading to a loss of KDM1A expression both at messenger RNA and protein levels (P = 1.2 × 10 -12 and P < .01, respectively). Subsequently, KDM1A pathogenic variants were identified in 4 of 4 additional index cases with FDCS., Conclusion: KDM1A inactivation explains about 90% of FDCS PBMAH. Genetic screening for ARMC5 and KDM1A can now be offered for most PBMAH operated patients and their families, opening the way to earlier diagnosis and improved management., Competing Interests: Conflict of Interest The authors declare no conflicts of interest., (Copyright © 2021 American College of Medical Genetics and Genomics. All rights reserved.)

Published

2022

42. Accurate intercensal estimates of energy access to track Sustainable Development Goal 7.

Author

Pokhriyal N, Letouzé E, and Vosoughi S

Abstract

Intercensal estimates of access to electricity and clean cooking fuels at policy planning microregions in a country are essential for understanding their evolution and tracking progress towards Sustainable Development Goals (SDG) 7. Surveys are prohibitively expensive to get such intercensal microestimates. Existing works, mainly, focus on electrification rates, make predictions at the coarse spatial granularity, and generalize poorly to intercensal periods. Limited works focus on estimating clean cooking fuel access, which is one of the crucial indicators for measuring progress towards SDG 7. We propose a novel spatio-temporal multi-target Bayesian regression model that provides accurate intercensal microestimates for household electrification and clean cooking fuel access by combining multiple types of earth-observation data, census, and surveys. Our model's estimates are produced for Senegal for 2020 at policy planning microregions, and they explain 77% and 86% of variation in regional aggregates for electrification and clean fuels, respectively, when validated against the most recent survey. The diagnostic nature of our microestimates reveals a slow evolution and significant lack of clean cooking fuel access in both urban and rural areas in Senegal. It underscores the challenge of expanding energy access even in urban areas owing to their rapid population growth. Owing to the timeliness and accuracy of our microestimates, they can help plan interventions by local governments or track the attainment of SDGs when no ground-truth data are available., Supplementary Information: The online version contains supplementary material available at 10.1140/epjds/s13688-022-00371-5., Competing Interests: Competing interestsThe authors declare that they have no competing interests., (© The Author(s) 2022.)

Published

2022

43. Common genetic variation in alcohol-related hepatocellular carcinoma: a case-control genome-wide association study.

Author

Trépo E, Caruso S, Yang J, Imbeaud S, Couchy G, Bayard Q, Letouzé E, Ganne-Carrié N, Moreno C, Oussalah A, Féray C, Blanc JF, Clément B, Hillon P, Boursier J, Paradis V, Calderaro J, Gnemmi V, Nault JC, Guéant JL, Devière J, Archambeaud I, Vitellius C, Turlin B, Bronowicki JP, Gustot T, Sutton A, Ziol M, Nahon P, and Zucman-Rossi J

Subjects

Acyltransferases genetics, Adult, Aged, Aged, 80 and over, Case-Control Studies, Female, Genetic Variation, Genotype, Humans, Male, Middle Aged, Phospholipases A2, Calcium-Independent genetics, Polymorphism, Single Nucleotide, Wnt Proteins genetics, Wnt3A Protein genetics, Young Adult, Alcohol-Related Disorders genetics, Carcinoma, Hepatocellular genetics, Genetic Predisposition to Disease, Genome-Wide Association Study, Liver Neoplasms genetics

Abstract

Background: Hepatocellular carcinoma is a frequent consequence of alcohol-related liver disease, with variable incidence among heavy drinkers. We did a genome-wide association study (GWAS) to identify common genetic variants for alcohol-related hepatocellular carcinoma., Methods: We conducted a two-stage case-control GWAS in a discovery cohort of 2107 unrelated European patients with alcohol-related liver disease aged 20-92 years recruited between Oct 22, 1993, and March 12, 2017. Cases were patients with alcohol-related hepatocellular carcinoma diagnosed by imaging or histology. Controls were patients with alcohol-related liver disease without hepatocellular carcinoma. We used an additive logistic regression model adjusted for the first ten principal components to assess genetic variants associated with alcohol-related hepatocellular carcinoma. We did another analysis with adjustment for age, sex, and liver fibrosis. New candidate associations (p<1 × 10 -6 ) and variants previously associated with alcohol-related hepatocellular carcinoma were evaluated in a validation cohort of 1933 patients with alcohol-related liver disease aged 29-92 years recruited between July 21, 1995, and May 2, 2019. We did a meta-analysis of the two case-control cohorts., Findings: The discovery cohort included 775 cases and 1332 controls. Of 7 962 325 variants assessed, we identified WNT3A-WNT9A (rs708113; p=1·11 × 10 -8 ) and found support for previously reported regions associated with alcohol-related hepatocellular carcinoma risk at TM6SF2 (rs58542926; p=6·02 × 10 -10 ), PNPLA3 (rs738409; p=9·29 × 10 -7 ), and HSD17B13 (rs72613567; p=2·49 × 10 -4 ). The validation cohort included 874 cases and 1059 controls and three variants were replicated: WNT3A-WNT9A (rs708113; p=1·17 × 10 -3 ), TM6SF2 (rs58542926; p=4·06 × 10 -5 ), and PNPLA3 (rs738409; p=1·17 × 10 -4 ). All three variants reached GWAS significance in the meta-analysis: WNT3A-WNT9A (odds ratio 0·73, 95% CI 0·66-0·81; p=3·93 × 10 -10 ), TM6SF2 (1·77, 1·52-2·07; p=3·84×10 -13 ), PNPLA3 (1·34, 1·22-1·47; p=7·30 × 10 -10 ). Adjustment for clinical covariates yielded similar results. We observed an additive effect of at-risk alleles on alcohol-related hepatocellular carcinoma. WNT3A-WNT9A rs708113 was not associated with liver fibrosis., Interpretation: WNT3A-WNT9A is a susceptibility locus for alcohol-related hepatocellular carcinoma, suggesting an early role of the Wnt-β-catenin pathway in alcohol-related hepatocellular carcinoma carcinogenesis., Funding: Ligue Nationale contre le Cancer, Bpifrance, INSERM, AFEF, CARPEM, Labex OncoImmunology, and Agence Nationale de la Recherche., Competing Interests: Declaration of interests ET received research support from Gilead. NG-C received honoraria from Roche, Gilead, and Ipsen, and support for travel and attending meetings from Gilead. CM received research support from Gilead; consulting fees from Gilead, AbbVie, Novartis, Surrozen, and Julius Clinical; support for travel and attending meetings from Gilead and AbbVie; honoraria from Bayer and Astellas; and acted as a scientific advisor to Gilead and Novartis. J-CN received research support from Bayer and Ipsen. J-PB received consulting fees from Bayer, Roche, and Ipsen; honoraria from Bayer, Ipsen, and Roche; support for travel and attending meetings from Bayer, Ipsen, and Roche; and acted as a scientific advisor to Roche. TG received research support from Gilead, honoraria from AbbVie, and acted as a scientific advisor to GoLiver Therapeutics and Promethera Biosciences. PN received research support from Bristol Myers Squibb, Eisai, and Roche; consulting fees from AstraZeneca, Bayer, Bristol Myers Squibb, Gilead, Eisai, Roche, Ipsen, and Exact Science; honoraria from AstraZeneca, Bayer, Bristol Myers Squibb, Gilead, Eisai, Roche, Ipsen, and Exact Science; support for travel and attending meetings from Ipsen and Roche; and acted as a scientific advisor to AstraZeneca, Bayer, Bristol Myers Squibb, Gilead, Eisai, Roche, Ipsen, and Exact Science. All other authors declare no competing interests., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

44. Integrated Genomic Analysis Identifies Driver Genes and Cisplatin-Resistant Progenitor Phenotype in Pediatric Liver Cancer.

Author

Hirsch TZ, Pilet J, Morcrette G, Roehrig A, Monteiro BJE, Molina L, Bayard Q, Trépo E, Meunier L, Caruso S, Renault V, Deleuze JF, Fresneau B, Chardot C, Gonzales E, Jacquemin E, Guerin F, Fabre M, Aerts I, Taque S, Laithier V, Branchereau S, Guettier C, Brugières L, Rebouissou S, Letouzé E, and Zucman-Rossi J

Subjects

Adolescent, Carcinoma, Hepatocellular drug therapy, Carcinoma, Hepatocellular genetics, Child, Child, Preschool, Female, Gene Expression Profiling, Genomics, Hepatoblastoma drug therapy, Hepatoblastoma genetics, Humans, Infant, Liver Neoplasms genetics, Male, Neoplasm Recurrence, Local, Phenotype, Antineoplastic Agents therapeutic use, Cisplatin therapeutic use, Drug Resistance, Neoplasm genetics, Liver Neoplasms drug therapy

Abstract

Pediatric liver cancers (PLC) comprise diverse diseases affecting infants, children, and adolescents. Despite overall good prognosis, PLCs display heterogeneous response to chemotherapy. Integrated genomic analysis of 126 pediatric liver tumors showed a continuum of driver mechanisms associated with patient age, including new targetable oncogenes. In 10% of patients with hepatoblastoma, all before three years old, we identified a mosaic premalignant clonal expansion of cells altered at the 11p15.5 locus. Analysis of spatial and longitudinal heterogeneity revealed an important plasticity between "hepatocytic," "liver progenitor," and "mesenchymal" molecular subgroups of hepatoblastoma. We showed that during chemotherapy, "liver progenitor" cells accumulated massive loads of cisplatin-induced mutations with a specific mutational signature, leading to the development of heavily mutated relapses and metastases. Drug screening in PLC cell lines identified promising targets for cisplatin-resistant progenitor cells, validated in mouse xenograft experiments. These data provide new insights into cisplatin resistance mechanisms in PLC and suggest alternative therapies. SIGNIFICANCE: PLCs are deadly when they resist chemotherapy, with limited alternative treatment options. Using a multiomics approach, we identified PLC driver genes and the cellular phenotype at the origin of cisplatin resistance. We validated new treatments targeting these molecular features in cell lines and xenografts. This article is highlighted in the In This Issue feature, p. 2355 ., (©2021 American Association for Cancer Research.)

Published

2021

45. A high-risk retinoblastoma subtype with stemness features, dedifferentiated cone states and neuronal/ganglion cell gene expression.

Author

Liu J, Ottaviani D, Sefta M, Desbrousses C, Chapeaublanc E, Aschero R, Sirab N, Lubieniecki F, Lamas G, Tonon L, Dehainault C, Hua C, Fréneaux P, Reichman S, Karboul N, Biton A, Mirabal-Ortega L, Larcher M, Brulard C, Arrufat S, Nicolas A, Elarouci N, Popova T, Némati F, Decaudin D, Gentien D, Baulande S, Mariani O, Dufour F, Guibert S, Vallot C, Rouic LL, Matet A, Desjardins L, Pascual-Pasto G, Suñol M, Catala-Mora J, Llano GC, Couturier J, Barillot E, Schaiquevich P, Gauthier-Villars M, Stoppa-Lyonnet D, Golmard L, Houdayer C, Brisse H, Bernard-Pierrot I, Letouzé E, Viari A, Saule S, Sastre-Garau X, Doz F, Carcaboso AM, Cassoux N, Pouponnot C, Goureau O, Chantada G, de Reyniès A, Aerts I, and Radvanyi F

Subjects

Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Cell Dedifferentiation genetics, Child, Preschool, DNA Methylation, Female, Gene Expression, Genetic Heterogeneity, Humans, Infant, Male, Mutation, N-Myc Proto-Oncogene Protein genetics, Neoplasm Metastasis, Retinal Cone Photoreceptor Cells metabolism, Retinal Ganglion Cells pathology, Retinal Neoplasms genetics, Retinal Neoplasms metabolism, Retinal Neoplasms pathology, Retinoblastoma genetics, Retinoblastoma metabolism, Retinoblastoma pathology, Retinal Cone Photoreceptor Cells pathology, Retinal Ganglion Cells metabolism, Retinal Neoplasms classification, Retinoblastoma classification

Abstract

Retinoblastoma is the most frequent intraocular malignancy in children, originating from a maturing cone precursor in the developing retina. Little is known on the molecular basis underlying the biological and clinical behavior of this cancer. Here, using multi-omics data, we demonstrate the existence of two retinoblastoma subtypes. Subtype 1, of earlier onset, includes most of the heritable forms. It harbors few genetic alterations other than the initiating RB1 inactivation and corresponds to differentiated tumors expressing mature cone markers. By contrast, subtype 2 tumors harbor frequent recurrent genetic alterations including MYCN-amplification. They express markers of less differentiated cone together with neuronal/ganglion cell markers with marked inter- and intra-tumor heterogeneity. The cone dedifferentiation in subtype 2 is associated with stemness features including low immune and interferon response, E2F and MYC/MYCN activation and a higher propensity for metastasis. The recognition of these two subtypes, one maintaining a cone-differentiated state, and the other, more aggressive, associated with cone dedifferentiation and expression of neuronal markers, opens up important biological and clinical perspectives for retinoblastomas., (© 2021. The Author(s).)

Published

2021

46. DNA Methylation Signatures Reveal the Diversity of Processes Remodeling Hepatocellular Carcinoma Methylomes.

Author

Meunier L, Hirsch TZ, Caruso S, Imbeaud S, Bayard Q, Roehrig A, Couchy G, Nault JC, Llovet JM, Blanc JF, Calderaro J, Zucman-Rossi J, and Letouzé E

Subjects

Aged, Carcinoma, Hepatocellular pathology, CpG Islands genetics, Datasets as Topic, Epigenesis, Genetic, Epigenome, Female, Gene Regulatory Networks, Humans, Liver Neoplasms pathology, Male, Middle Aged, Mutation, RNA-Seq, Carcinoma, Hepatocellular genetics, DNA Methylation, Genetic Heterogeneity, Liver Neoplasms genetics

Abstract

Background and Aims: DNA methylation patterns are highly rearranged in HCCs. However, diverse sources of variation are intermingled in cancer methylomes, precluding the precise characterization of underlying molecular mechanisms. We developed a computational framework (methylation signature analysis with independent component analysis [MethICA]) leveraging independent component analysis to disentangle the diverse processes contributing to DNA methylation changes in tumors., Approach and Results: Applied to a collection of 738 HCCs, MethICA unraveled 13 stable methylation components preferentially active in specific chromatin states, sequence contexts, and replication timings. These included signatures of general processes associated with sex and age but also signatures related to specific driver events and molecular subgroups. Catenin beta 1 mutations were major modulators of methylation patterns in HCC, characterized by a targeted hypomethylation of transcription factor 7-bound enhancers in the vicinity of Wnt target genes as well as a widespread hypomethylation of late-replicated partially methylated domains. By contrast, demethylation of early replicated highly methylated domains was a signature of replication stress, leading to an extensive hypomethylator phenotype in cyclin-activated HCC. Inactivating mutations of the chromatin remodeler AT-rich interactive domain-containing protein 1A were associated with epigenetic silencing of differentiation-promoting transcriptional networks, also detectable in cirrhotic liver. Finally, a hypermethylation signature targeting polycomb-repressed chromatin domains was identified in the G1 molecular subgroup with progenitor features., Conclusions: This study elucidates the diversity of processes remodeling HCC methylomes and reveals the epigenetic and transcriptional impact of driver alterations., (© 2021 American Association for the Study of Liver Diseases.)

Published

2021

47. Multi-site tumor sampling highlights molecular intra-tumor heterogeneity in malignant pleural mesothelioma.

Author

Meiller C, Montagne F, Hirsch TZ, Caruso S, de Wolf J, Bayard Q, Assié JB, Meunier L, Blum Y, Quetel L, Gibault L, Pintilie E, Badoual C, Humez S, Galateau-Sallé F, Copin MC, Letouzé E, Scherpereel A, Zucman-Rossi J, Le Pimpec-Barthes F, Jaurand MC, and Jean D

Subjects

Biopsy, Computational Biology methods, DNA Mutational Analysis methods, Disease Management, Disease Susceptibility, Gene Expression Profiling, Genetic Heterogeneity, High-Throughput Nucleotide Sequencing, Humans, Mesothelioma, Malignant diagnosis, Mesothelioma, Malignant metabolism, Molecular Diagnostic Techniques, Molecular Sequence Annotation, Mutation, Pleural Neoplasms diagnosis, Pleural Neoplasms metabolism, Precision Medicine methods, Precision Medicine standards, Prognosis, Tumor Microenvironment genetics, Exome Sequencing, Biomarkers, Tumor, Mesothelioma, Malignant etiology, Pleural Neoplasms etiology

Abstract

Background: Malignant pleural mesothelioma (MPM) is a heterogeneous cancer. Better knowledge of molecular and cellular intra-tumor heterogeneity throughout the thoracic cavity is required to develop efficient therapies. This study focuses on molecular intra-tumor heterogeneity using the largest series to date in MPM and is the first to report on the multi-omics profiling of a substantial series of multi-site tumor samples., Methods: Intra-tumor heterogeneity was investigated in 16 patients from whom biopsies were taken at distinct anatomical sites. The paired biopsies collected from apex, side wall, costo-diaphragmatic, or highest metabolic sites as well as 5 derived cell lines were screened using targeted sequencing. Whole exome sequencing, RNA sequencing, and DNA methylation were performed on a subset of the cohort for deep characterization. Molecular classification, recently defined histo-molecular gradients, and cell populations of the tumor microenvironment were assessed., Results: Sequencing analysis identified heterogeneous variants notably in NF2, a key tumor suppressor gene of mesothelial carcinogenesis. Subclonal tumor populations were shared among paired biopsies, suggesting a polyclonal dissemination of the tumor. Transcriptome analysis highlighted dysregulation of cell adhesion and extracellular matrix pathways, linked to changes in histo-molecular gradient proportions between anatomic sites. Methylome analysis revealed the contribution of epigenetic mechanisms in two patients. Finally, significant changes in the expression of immune mediators and genes related to immunological synapse, as well as differential infiltration of immune populations in the tumor environment, were observed and led to a switch from a hot to a cold immune profile in three patients., Conclusions: This comprehensive analysis reveals patient-dependent spatial intra-tumor heterogeneity at the genetic, transcriptomic, and epigenetic levels and in the immune landscape of the tumor microenvironment. Results support the need for multi-sampling for the implementation of molecular-based precision medicine., (© 2021. The Author(s).)

Published

2021

48. Corrigendum to Berchtold L, Letouzé E, Alexander MP, et al. HLA-D and PLA2R1 risk alleles associate with recurrent primary membranous nephropathy in kidney transplant recipients. Kidney Int. 2021;99:671-685.

Author

Berchtold L, Letouzé E, Alexander MP, Canaud G, Logt AV, Hamilton P, Mousson C, Vuiblet V, Moyer AM, Guibert S, Mrázová P, Levi C, Dubois V, Cruzado JM, Torres A, Gandhi MJ, Yousfi N, Tesar V, Viklický O, Hourmant M, Moulin B, Rieu P, Choukroun G, Legendre C, Wetzels J, Brenchley P, Ballarín Castan JA, Debiec H, and Ronco P

Published

2021

49. Loss of SDHB Promotes Dysregulated Iron Homeostasis, Oxidative Stress, and Sensitivity to Ascorbate.

Author

Goncalves J, Moog S, Morin A, Gentric G, Müller S, Morrell AP, Kluckova K, Stewart TJ, Andoniadou CL, Lussey-Lepoutre C, Bénit P, Thakker A, Vettore L, Roberts J, Rodriguez R, Mechta-Grigoriou F, Gimenez-Roqueplo AP, Letouzé E, Tennant DA, and Favier J

Subjects

Animals, Antioxidants pharmacology, Dioxygenases antagonists & inhibitors, Female, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mitochondria metabolism, Mitochondria pathology, Phenotype, Reactive Oxygen Species, Ascorbic Acid pharmacology, Homeostasis, Iron metabolism, Mutation, Oxidative Stress, Succinate Dehydrogenase physiology

Abstract

Succinate dehydrogenase is a key enzyme in the tricarboxylic acid cycle and the electron transport chain. All four subunits of succinate dehydrogenase are tumor suppressor genes predisposing to paraganglioma, but only mutations in the SDHB subunit are associated with increased risk of metastasis. Here we generated an Sdhd knockout chromaffin cell line and compared it with Sdhb- deficient cells. Both cell types exhibited similar SDH loss of function, metabolic adaptation, and succinate accumulation. In contrast, Sdhb -/- cells showed hallmarks of mesenchymal transition associated with increased DNA hypermethylation and a stronger pseudo-hypoxic phenotype compared with Sdhd -/- cells. Loss of SDHB specifically led to increased oxidative stress associated with dysregulated iron and copper homeostasis in the absence of NRF2 activation. High-dose ascorbate exacerbated the increase in mitochondrial reactive oxygen species, leading to cell death in Sdhb -/- cells. These data establish a mechanism linking oxidative stress to iron homeostasis that specifically occurs in Sdhb -deficient cells and may promote metastasis. They also highlight high-dose ascorbate as a promising therapeutic strategy for SDHB-related cancers. SIGNIFICANCE: Loss of different succinate dehydrogenase subunits can lead to different cell and tumor phenotypes, linking stronger 2-OG-dependent dioxygenases inhibition, iron overload, and ROS accumulation following SDHB mutation., (©2021 American Association for Cancer Research.)

Published

2021

50. HLA-D and PLA2R1 risk alleles associate with recurrent primary membranous nephropathy in kidney transplant recipients.

Author

Berchtold L, Letouzé E, Alexander MP, Canaud G, Logt AV, Hamilton P, Mousson C, Vuiblet V, Moyer AM, Guibert S, Mrázová P, Levi C, Dubois V, Cruzado JM, Torres A, Gandhi MJ, Yousfi N, Tesar V, OndrejViklický, Hourmant M, Moulin B, Rieu P, Choukroun G, Legendre C, Wetzels J, Brenchley P, Ballarín Castan JA, Debiec H, and Ronco P

Subjects

Alleles, Humans, Polymorphism, Single Nucleotide, Receptors, Phospholipase A2 genetics, Retrospective Studies, Glomerulonephritis, Membranous diagnosis, Glomerulonephritis, Membranous genetics, Kidney Transplantation adverse effects

Abstract

Recurrence of primary membranous nephropathy after transplantation occurs in up to 44% of patients and is driven by PLA2R antibody. Here, we asked whether genetic determinants could improve risk prediction. First, we sequenced PLA2R1 and HLA-D loci in 248 patients with primary membranous nephropathy and identified two independent single nucleotide polymorphisms (SNPs) at risk for primary membranous nephropathy at each locus. These were rs9271188 (intergenic between HLA-DRB1 and HLA-DQA1,) and rs9275086 (intergenic between HLA-DQB1 and HLA-DQA2) at the HLA-D locus along with rs6726925 and rs13018963 at the PLA2R1 locus. Then we investigated whether primary membranous nephropathy at-risk variants were associated with recurrence in a retrospective cohort of 105 donor-recipient pairs and a replication cohort of 40 pairs. Seven SNPs located between HLA-DRB1 and HLA-DQA1 in linkage disequilibrium with rs9271188, and three SNPs in the PLA2R1 region predicted recurrence when presented by the donor, but not when presented by the recipient. The two SNPs in the HLA-D region most strongly associated with recurrence (rs9271705 and rs9271550) were confirmed in the replication cohort. A genetic risk score based on the two best predictors at each locus (rs9271705, rs9271550, rs17830558, and rs3828323) identified a group of patients with high risk of recurrence. Thus, our results suggest that the graft contributes to recurrence of primary membranous nephropathy through the disease susceptibility HLA-D and PLA2R1 SNPs in an autoimmune milieu. Further studies are needed before implementation of genetic testing for these in donor selection., (Copyright © 2020. Published by Elsevier Inc.)

Published

2021