Rare manifestations and malignancies in tuberous sclerosis complex: findings from the TuberOus SClerosis registry to increAse disease awareness (TOSCA)

Sauter, M.; Belousova, E.; Benedik, M. P.; Carter, T.; Cottin, V.; Curatolo, P.; Dahlin, M.; D'Amato, L.; D'Augeres, G. B.; de Vries, P. J.; Ferreira, J. C.; Feucht, M.; Fladrowski, C.; Hertzberg, C.; Jozwiak, S.; Lawson, J. A.; Macaya, A.; Marques, R.; Nabbout, R.; O'Callaghan, F.; Qin, J.; Sander, V.; Shah, S.; Takahashi, Y.; Touraine, R.; Youroukos, S.; Zonnenberg, B.; Jansen, A.; Kingswood, J. C.; Shinohara, N.; Horie, S.; Kubota, M.; Tohyama, J.; Imai, K.; Kaneda, M.; Kaneko, H.; Uchida, Y.; Kirino, T.; Endo, S.; Inoue, Y.; Uruno, K.; Serdaroglu, A.; Yapici, Z.; Anlar, B.; Altunbasak, S.; Lvova, O.; Belyaev, O. V.; Agranovich, O.; Levitina, E. V.; Maksimova, Y. V.; Karas, A.; Jiang, Y.; Zou, L.; Xu, K.; Zhang, Y.; Luan, G.; Zhang, Y.; Wang, Y.; Jin, M.; Ye, D.; Liao, W.; Zhou, L.; Liu, J.; Liao, J.; Yan, B.; Deng, Y.; Jiang, L.; Liu, Z.; Huang, S.; Li, H.; Kim, K.; Chen, P. -L.; Lee, H. -F.; Tsai, J. -D.; Chi, C. -S.; Huang, C. -C.; Riney, K.; Yates, D.; Kwan, P.; Likasitwattanakul, S.; Nabangchang, C.; Chomtho, L. T. K.; Katanyuwong, K.; Sriudomkajorn, S.; Wilmshurst, J.; Segel, R.; Gilboa, T.; Tzadok, M.; Valevski, A. F.; Papathanasopoulos, P.; Papavasiliou, A. S.; Giannakodimos, S.; Gatzonis, S.; Pavlou, E.; Tzoufi, M.; Vergeer, A. M. H.; Dhooghe, M.; Verhelst, H.; Roelens, F.; Nassogne, M. C.; Defresne, P.; De Waele, L.; Leroy, P.; Demonceau, N.; Legros, B.; Van Bogaert, P.; Ceulemans, B.; Dom, L.; Castelnau, P.; De Saint Martin, A.; Riquet, A.; Milh, M.; Cances, C.; Pedespan, J. -M.; Ville, D.; Roubertie, A.; Auvin, S.; Berquin, P.; Richelme, C.; Allaire, C.; Gueden, S.; Tich, S. N. T.; Godet, B.; Rojas, M. L. R. F.; Planas, J. C.; Bermejo, A. M.; Dura, P. S.; Aparicio, S. R.; Gonzalez, M. J. M.; Pison, J. L.; Barca, M. O. B.; Laso, E. L.; Luengo, O. A.; Rodriguez, F. J. A.; Dieguez, I. M.; Salas, A. C.; Carrera, I. M.; Salcedo, E. M.; Petri, M. E. Y.; Candela, R. C.; da Conceicao Carrilho, I.; Vieira, J. P.; da Silva Oliveira Monteiro, J. P.; de Oliveira Ferreira Leao, M. J. S.; Luis, C. S. M. R.; Mendonca, C. P.; Endziniene, M.; Strautmanis, J.; Talvik, I.; Canevini, M. P.; Gambardella, A.; Pruna, D.; Buono, S.; Fontana, E.; Bernardina, B. D.; Burloiu, C.; Cosma, I. S. B.; Vintan, M. A.; Popescu, L.; Zitterbart, K.; Payerova, J.; Bratsky, L.; Zilinska, Z.; Gruber-Sedlmayr, U.; Baumann, M.; Haberlandt, E.; Rostasy, K.; Pataraia, E.; Elmslie, F.; Johnston, C. A.; Crawford, P.; Uldall, P.; Uvebrant, P.; Rask, O.; Bjoernvold, M.; Brodtkorb, E.; Sloerdahl, A.; Solhoff, R.; Jaatun, M. S. G.; Mandera, M.; Radzikowska, E. J.; Wysocki, M.; Fischereder, M.; Kurlemann, G.; Wilken, B.; Wiemer-Kruel, A.; Budde, K.; Marquard, K.; Knuf, M.; Hahn, A.; Hartmann, H.; Merkenschlager, A.; Trollmann, R.

doi:10.1186/s13023-021-01917-y

Background: Tuberous sclerosis complex (TSC) is a rare multisystem autosomal dominant disorder caused by pathogenic variants in either the TSC1 or TSC2 gene. Common manifestations of TSC have been grouped into major and minor clinical diagnostic criteria and assessed in clinical routine workup. However, case studies point towards the existence of rare disease manifestations and to the potential association of TSC with malignant tumors. In this study we sought to characterize rare manifestations and malignancies using a large cohort of patients. Methods: TuberOus SClerosis registry to increAse disease awareness (TOSCA) is a multicenter, international disease registry collecting clinical manifestations and characteristics of patients with TSC, both retrospectively and prospectively. We report rates and characteristics of rare manifestations and malignancies in patients with TSC who had enrolled in the TOSCA registry. We also examined these manifestations by age, sex, and genotype (TSC1 or TSC2). Results: Overall, 2211 patients with TSC were enrolled in the study. Rare manifestations were reported in 382 (17.3%) study participants and malignancies in 65 (2.9%). Of these rare manifestations, the most frequent were bone sclerotic foci (39.5%), scoliosis (23%), thyroid adenoma (5.5%), adrenal angiomyolipoma (4.5%), hemihypertrophy and pancreatic neuroendocrine tumors (pNET; both 3.1%). These rare manifestations were more commonly observed in adults than children (66.2% vs. 22.7%), in females versus males (58.4% vs. 41.6%; except for scoliosis: 48.9% vs. 51.1%), and in those with TSC2 versus TSC1 (67.0% vs. 21.1%; except for thyroid adenoma: 42.9% vs. 57.1%). In the 65 individuals with reported malignancies, the most common were renal cell carcinoma (47.7%), followed by breast (10.8%) and thyroid cancer (9.2%). Although malignancies were more common in adult patients, 26.1% were reported in children and 63.1% in individuals < 40 years. TSC1 mutations were over-represented in individuals with malignancies compared to the overall TOSCA cohort (32.1% vs. 18.5%). Conclusion: Rare manifestations were observed in a significant proportion of individuals with TSC. We recommend further examination of rare manifestations in TSC. Collectively, malignancies were infrequent findings in our cohort. However, compared to the general population, malignant tumors occurred earlier in age and some tumor types were more common.

Rare manifestations and malignancies in tuberous sclerosis complex: findings from the TuberOus SClerosis registry to increAse disease awareness (TOSCA)

Sauter M.;Belousova E.;Benedik M. P.;Carter T.;Cottin V.;Curatolo P.;Dahlin M.;D'Amato L.;d'Augeres G. B.;de Vries P. J.;Ferreira J. C.;Feucht M.;Fladrowski C.;Hertzberg C.;Jozwiak S.;Lawson J. A.;Macaya A.;Marques R.;Nabbout R.;O'Callaghan F.;Qin J.;Sander V.;Shah S.;Takahashi Y.;Touraine R.;Youroukos S.;Zonnenberg B.;Jansen A.;Kingswood J. C.;Shinohara N.;Horie S.;Kubota M.;Tohyama J.;Imai K.;Kaneda M.;Kaneko H.;Uchida Y.;Kirino T.;Endo S.;Inoue Y.;Uruno K.;Serdaroglu A.;Yapici Z.;Anlar B.;Altunbasak S.;Lvova O.;Belyaev O. V.;Agranovich O.;Levitina E. V.;Maksimova Y. V.;Karas A.;Jiang Y.;Zou L.;Xu K.;Zhang Y.;Luan G.;Zhang Y.;Wang Y.;Jin M.;Ye D.;Liao W.;Zhou L.;Liu J.;Liao J.;Yan B.;Deng Y.;Jiang L.;Liu Z.;Huang S.;Li H.;Kim K.;Chen P. -L.;Lee H. -F.;Tsai J. -D.;Chi C. -S.;Huang C. -C.;Riney K.;Yates D.;Kwan P.;Likasitwattanakul S.;Nabangchang C.;Chomtho L. T. K.;Katanyuwong K.;Sriudomkajorn S.;Wilmshurst J.;Segel R.;Gilboa T.;Tzadok M.;Valevski A. F.;Papathanasopoulos P.;Papavasiliou A. S.;Giannakodimos S.;Gatzonis S.;Pavlou E.;Tzoufi M.;Vergeer A. M. H.;Dhooghe M.;Verhelst H.;Roelens F.;Nassogne M. C.;Defresne P.;De Waele L.;Leroy P.;Demonceau N.;Legros B.;Van Bogaert P.;Ceulemans B.;Dom L.;Castelnau P.;De Saint Martin A.;Riquet A.;Milh M.;Cances C.;Pedespan J. -M.;Ville D.;Roubertie A.;Auvin S.;Berquin P.;Richelme C.;Allaire C.;Gueden S.;Tich S. N. T.;Godet B.;Rojas M. L. R. F.;Planas J. C.;Bermejo A. M.;Dura P. S.;Aparicio S. R.;Gonzalez M. J. M.;Pison J. L.;Barca M. O. B.;Laso E. L.;Luengo O. A.;Rodriguez F. J. A.;Dieguez I. M.;Salas A. C.;Carrera I. M.;Salcedo E. M.;Petri M. E. Y.;Candela R. C.;da Conceicao Carrilho I.;Vieira J. P.;da Silva Oliveira Monteiro J. P.;de Oliveira Ferreira Leao M. J. S.;Luis C. S. M. R.;Mendonca C. P.;Endziniene M.;Strautmanis J.;Talvik I.;Canevini M. P.;Gambardella A.;Pruna D.;Buono S.;Fontana E.;Bernardina B. D.;Burloiu C.;Cosma I. S. B.;Vintan M. A.;Popescu L.;Zitterbart K.;Payerova J.;Bratsky L.;Zilinska Z.;Gruber-Sedlmayr U.;Baumann M.;Haberlandt E.;Rostasy K.;Pataraia E.;Elmslie F.;Johnston C. A.;Crawford P.;Uldall P.;Uvebrant P.;Rask O.;Bjoernvold M.;Brodtkorb E.;Sloerdahl A.;Solhoff R.;Jaatun M. S. G.;Mandera M.;Radzikowska E. J.;Wysocki M.;Fischereder M.;Kurlemann G.;Wilken B.;Wiemer-Kruel A.;Budde K.;Marquard K.;Knuf M.;Hahn A.;Hartmann H.;Merkenschlager A.;Trollmann R.

2021-01-01

Abstract

Background: Tuberous sclerosis complex (TSC) is a rare multisystem autosomal dominant disorder caused by pathogenic variants in either the TSC1 or TSC2 gene. Common manifestations of TSC have been grouped into major and minor clinical diagnostic criteria and assessed in clinical routine workup. However, case studies point towards the existence of rare disease manifestations and to the potential association of TSC with malignant tumors. In this study we sought to characterize rare manifestations and malignancies using a large cohort of patients. Methods: TuberOus SClerosis registry to increAse disease awareness (TOSCA) is a multicenter, international disease registry collecting clinical manifestations and characteristics of patients with TSC, both retrospectively and prospectively. We report rates and characteristics of rare manifestations and malignancies in patients with TSC who had enrolled in the TOSCA registry. We also examined these manifestations by age, sex, and genotype (TSC1 or TSC2). Results: Overall, 2211 patients with TSC were enrolled in the study. Rare manifestations were reported in 382 (17.3%) study participants and malignancies in 65 (2.9%). Of these rare manifestations, the most frequent were bone sclerotic foci (39.5%), scoliosis (23%), thyroid adenoma (5.5%), adrenal angiomyolipoma (4.5%), hemihypertrophy and pancreatic neuroendocrine tumors (pNET; both 3.1%). These rare manifestations were more commonly observed in adults than children (66.2% vs. 22.7%), in females versus males (58.4% vs. 41.6%; except for scoliosis: 48.9% vs. 51.1%), and in those with TSC2 versus TSC1 (67.0% vs. 21.1%; except for thyroid adenoma: 42.9% vs. 57.1%). In the 65 individuals with reported malignancies, the most common were renal cell carcinoma (47.7%), followed by breast (10.8%) and thyroid cancer (9.2%). Although malignancies were more common in adult patients, 26.1% were reported in children and 63.1% in individuals < 40 years. TSC1 mutations were over-represented in individuals with malignancies compared to the overall TOSCA cohort (32.1% vs. 18.5%). Conclusion: Rare manifestations were observed in a significant proportion of individuals with TSC. We recommend further examination of rare manifestations in TSC. Collectively, malignancies were infrequent findings in our cohort. However, compared to the general population, malignant tumors occurred earlier in age and some tumor types were more common.

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	Anno
	
			2021
		
	Parole chiave
	
			Malignancy
Rare manifestation
TOSCA
TSC
Tuberous sclerosis complex
Adult
Child
Female
Humans
Male
Mutation
Registries
Retrospective Studies
Tuberous Sclerosis Complex 1 Protein
Tuberous Sclerosis Complex 2 Protein
Adrenal Gland Neoplasms
Angiomyolipoma
Tuberous Sclerosis
		
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/20.500.12317/75071

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Rare manifestations and malignancies in tuberous sclerosis complex: findings from the TuberOus SClerosis registry to increAse disease awareness (TOSCA)

2021-01-01

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