Your search keyword '"GNA11"' showing total 106 results

1. Early-onset hypertension associated with extensive cutaneous capillary malformations harboring postzygotic variants in GNAQ and GNA11.

Author

Davies, Olivia, Davies, Olivia, Ng, Ashley, Tran, Jennifer, Blumenthal, Shoshana, Arkin, Lisa, Nopper, Amy, Cottrell, Catherine, Garzon, Maria, Siegel, Dawn, Frieden, Ilona, Drolet, Beth, Davies, Olivia, Davies, Olivia, Ng, Ashley, Tran, Jennifer, Blumenthal, Shoshana, Arkin, Lisa, Nopper, Amy, Cottrell, Catherine, Garzon, Maria, Siegel, Dawn, Frieden, Ilona, and Drolet, Beth

Abstract

BACKGROUND AND OBJECTIVES: Cutaneous capillary malformations (CMs) describe a group of vascular birthmarks with heterogeneous presentations. CMs may present as an isolated finding or with other associations, including glaucoma and leptomeningeal angiomatosis (i.e., Sturge-Weber syndrome) or pigmentary birthmarks (i.e., phakomatosis pigmentovascularis). The use of targeted genetic sequencing has revealed that postzygotic somatic variations in GNAQ and GNA11 at codon 183 are associated with CMs. We report five patients with early-onset hypertension and discuss possible pathogenesis of hypertension. METHODS: Twenty-nine patients with CMs, confirmed GNAQ/11 postzygotic variants, and documented past medical history were identified from a multi-institutional vascular anomalies study. Early-onset hypertension was defined as hypertension before the age of 55 years. Clinical data were reviewed for evidence of hypertension, such as documentation of diagnosis or elevated blood pressure measurements. RESULTS: Five of the 29 patients identified as having GNAQ/11 postzygotic variants had documented early-onset hypertension. Three individuals harbored a GNAQ p.R183Q variant, and two individuals harbored a GNA11 p.R183C variant. All individuals had extensive cutaneous CMs involving the trunk and covering 9%-56% of their body surface area. The median age of hypertension diagnosis was 15 years (range 11-24 years), with three individuals having renal abnormalities on imaging. CONCLUSIONS: Early-onset hypertension is associated with extensive CMs harboring somatic variations in GNAQ/11. Here, we expand on the GNAQ/11 phenotype and hypothesize potential mechanisms driving hypertension. We recommend serial blood pressure measurements in patients with extensive CMs on the trunk and extremities to screen for early-onset hypertension.

Published

2022

2. Somatic mutations of GNA11 and GNAQ in CTNNB1-mutant aldosterone-producing adenomas presenting in puberty, pregnancy or menopause

Author

Zhou, Junhua, Azizan, Elena A. B., Cabrera, Claudia P., Fernandes-Rosa, Fabio L., Boulkroun, Sheerazed, Argentesi, Giulia, Cottrell, Emily, Amar, Laurence, Wu, Xilin, O'Toole, Sam, Goodchild, Emily, Marker, Alison, Senanayake, Russell, Garg, Sumedha, Åkerström, Tobias, Backman, Samuel, Jordan, Suzanne, Polubothu, Satyamaanasa, Berney, Daniel M., Gluck, Anna, Lines, Kate E., Thakker, Rajesh V., Tuthill, Antoinette, Joyce, Caroline, Kaski, Juan Pablo, Karet Frankl, Fiona E., Metherell, Lou A., Teo, Ada E. D., Gurnell, Mark, Parvanta, Laila, Drake, William M., Wozniak, Eva, Klinzing, David, Kuan, Jyn Ling, Tiang, Zenia, Gomez Sanchez, Celso E., Hellman, Per, Foo, Roger S. Y., Mein, Charles A., Kinsler, Veronica A., Björklund, Peyman, Storr, Helen L., Zennaro, Maria-Christina, Brown, Morris J., Zhou, Junhua, Azizan, Elena A. B., Cabrera, Claudia P., Fernandes-Rosa, Fabio L., Boulkroun, Sheerazed, Argentesi, Giulia, Cottrell, Emily, Amar, Laurence, Wu, Xilin, O'Toole, Sam, Goodchild, Emily, Marker, Alison, Senanayake, Russell, Garg, Sumedha, Åkerström, Tobias, Backman, Samuel, Jordan, Suzanne, Polubothu, Satyamaanasa, Berney, Daniel M., Gluck, Anna, Lines, Kate E., Thakker, Rajesh V., Tuthill, Antoinette, Joyce, Caroline, Kaski, Juan Pablo, Karet Frankl, Fiona E., Metherell, Lou A., Teo, Ada E. D., Gurnell, Mark, Parvanta, Laila, Drake, William M., Wozniak, Eva, Klinzing, David, Kuan, Jyn Ling, Tiang, Zenia, Gomez Sanchez, Celso E., Hellman, Per, Foo, Roger S. Y., Mein, Charles A., Kinsler, Veronica A., Björklund, Peyman, Storr, Helen L., Zennaro, Maria-Christina, and Brown, Morris J.

Abstract

Sequence analysis identifies gain-of-function somatic mutations in GNA11 or GNAQ in CTNNB1-mutant aldosterone-producing adenomas. Most patients with these mutations presented during puberty, pregnancy or menopause, with elevated LHCGR expression. Most aldosterone-producing adenomas (APAs) have gain-of-function somatic mutations of ion channels or transporters. However, their frequency in aldosterone-producing cell clusters of normal adrenal gland suggests a requirement for codriver mutations in APAs. Here we identified gain-of-function mutations in both CTNNB1 and GNA11 by whole-exome sequencing of 3/41 APAs. Further sequencing of known CTNNB1-mutant APAs led to a total of 16 of 27 (59%) with a somatic p.Gln209His, p.Gln209Pro or p.Gln209Leu mutation of GNA11 or GNAQ. Solitary GNA11 mutations were found in hyperplastic zona glomerulosa adjacent to double-mutant APAs. Nine of ten patients in our UK/Irish cohort presented in puberty, pregnancy or menopause. Among multiple transcripts upregulated more than tenfold in double-mutant APAs was LHCGR, the receptor for luteinizing or pregnancy hormone (human chorionic gonadotropin). Transfections of adrenocortical cells demonstrated additive effects of GNA11 and CTNNB1 mutations on aldosterone secretion and expression of genes upregulated in double-mutant APAs. In adrenal cortex, GNA11/Q mutations appear clinically silent without a codriver mutation of CTNNB1.

Published

2021

3. GNAQ and GNA11 mutant nonuveal melanoma: a subtype distinct from both cutaneous and uveal melanoma

Author

Livingstone, E., Zaremba, A., Horn, S., Ugurel, S., Casalini, B., Schlaak, M., Hassel, J. C., Herbst, R., Utikal, J. S., Weide, B., Gutzmer, R., Meier, F., Koelsche, C., Hadaschik, E., Sucker, A., Reis, H., Merkelbach-Bruse, S., Siewert, M., Sahm, F., von Deimling, A., Cosgarea, I., Zimmer, L., Schadendorf, D., Schilling, B., Griewank, K. G., Livingstone, E., Zaremba, A., Horn, S., Ugurel, S., Casalini, B., Schlaak, M., Hassel, J. C., Herbst, R., Utikal, J. S., Weide, B., Gutzmer, R., Meier, F., Koelsche, C., Hadaschik, E., Sucker, A., Reis, H., Merkelbach-Bruse, S., Siewert, M., Sahm, F., von Deimling, A., Cosgarea, I., Zimmer, L., Schadendorf, D., Schilling, B., and Griewank, K. G.

Abstract

Background GNAQ and GNA11 mutant nonuveal melanoma represent a poorly characterized rare subgroup of melanoma with a gene mutation profile similar to uveal melanoma. Objectives To characterize these tumours in terms of clinical behaviour and genetic characteristics. Methods Patients with nonuveal GNAQ/11 mutated melanoma were identified from the prospective multicentre tumour tissue registry ADOREG, Tissue Registry in Melanoma (TRIM) and additional cooperating skin cancer centres. Extensive data on patient, tumour and treatment characteristics were collected retrospectively. Targeted sequencing was used to determine tumour mutational burden. Immunohistochemistry staining was performed for programmed death-ligand 1 and BRCA1-associated protein (BAP)1. Existing whole-exome cutaneous and uveal melanoma data were analysed for mutation type and burden. Results We identified 18 patients with metastatic GNAQ/11 mutant nonuveal melanoma. Tumours had a lower tumour mutational burden and fewer ultraviolet signature mutations than cutaneous melanomas. In addition to GNAQ and GNA11 mutations (nine each), six splicing factor 3b subunit 1 (SF3B1), three eukaryotic translation initiation factor 1A X-linked (EIF1AX) and four BAP1 mutations were detected. In contrast to uveal melanoma, GNAQ/11 mutant nonuveal melanomas frequently metastasized lymphatically and concurrent EIF1AX, SF3B1 and BAP1 mutations showed no apparent association with patient prognosis. Objective response to immunotherapy was poor with only one partial response observed in 10 treated patients (10%). Conclusions Our findings suggest that GNAQ/11 mutant nonuveal melanomas are a subtype of melanoma that is both clinically and genetically distinct from cutaneous and uveal melanoma. As they respond poorly to available treatment regimens, novel effective therapeutic approaches for affected patients are urgently needed. What is already known about this topic? The rare occurrence of GNAQ/11 mutations in nonuveal melanom

Published

2020

4. GNAQ and GNA11 mutant nonuveal melanoma: a subtype distinct from both cutaneous and uveal melanoma

Author

Livingstone, E., Zaremba, A., Horn, S., Ugurel, S., Casalini, B., Schlaak, M., Hassel, J. C., Herbst, R., Utikal, J. S., Weide, B., Gutzmer, R., Meier, F., Koelsche, C., Hadaschik, E., Sucker, A., Reis, H., Merkelbach-Bruse, S., Siewert, M., Sahm, F., von Deimling, A., Cosgarea, I., Zimmer, L., Schadendorf, D., Schilling, B., Griewank, K. G., Livingstone, E., Zaremba, A., Horn, S., Ugurel, S., Casalini, B., Schlaak, M., Hassel, J. C., Herbst, R., Utikal, J. S., Weide, B., Gutzmer, R., Meier, F., Koelsche, C., Hadaschik, E., Sucker, A., Reis, H., Merkelbach-Bruse, S., Siewert, M., Sahm, F., von Deimling, A., Cosgarea, I., Zimmer, L., Schadendorf, D., Schilling, B., and Griewank, K. G.

Abstract

Background GNAQ and GNA11 mutant nonuveal melanoma represent a poorly characterized rare subgroup of melanoma with a gene mutation profile similar to uveal melanoma. Objectives To characterize these tumours in terms of clinical behaviour and genetic characteristics. Methods Patients with nonuveal GNAQ/11 mutated melanoma were identified from the prospective multicentre tumour tissue registry ADOREG, Tissue Registry in Melanoma (TRIM) and additional cooperating skin cancer centres. Extensive data on patient, tumour and treatment characteristics were collected retrospectively. Targeted sequencing was used to determine tumour mutational burden. Immunohistochemistry staining was performed for programmed death-ligand 1 and BRCA1-associated protein (BAP)1. Existing whole-exome cutaneous and uveal melanoma data were analysed for mutation type and burden. Results We identified 18 patients with metastatic GNAQ/11 mutant nonuveal melanoma. Tumours had a lower tumour mutational burden and fewer ultraviolet signature mutations than cutaneous melanomas. In addition to GNAQ and GNA11 mutations (nine each), six splicing factor 3b subunit 1 (SF3B1), three eukaryotic translation initiation factor 1A X-linked (EIF1AX) and four BAP1 mutations were detected. In contrast to uveal melanoma, GNAQ/11 mutant nonuveal melanomas frequently metastasized lymphatically and concurrent EIF1AX, SF3B1 and BAP1 mutations showed no apparent association with patient prognosis. Objective response to immunotherapy was poor with only one partial response observed in 10 treated patients (10%). Conclusions Our findings suggest that GNAQ/11 mutant nonuveal melanomas are a subtype of melanoma that is both clinically and genetically distinct from cutaneous and uveal melanoma. As they respond poorly to available treatment regimens, novel effective therapeutic approaches for affected patients are urgently needed. What is already known about this topic? The rare occurrence of GNAQ/11 mutations in nonuveal melanom

Published

2020

5. Prognostic impact of chromosomal aberrations and GNAQ, GNA11 and BAP1 mutations in uveal melanoma

Author

Staby, Kjersti M, Gravdal, Karsten, Mørk, Sverre J, Heegaard, Steffen, Vintermyr, Olav K, Krohn, Jørgen, Staby, Kjersti M, Gravdal, Karsten, Mørk, Sverre J, Heegaard, Steffen, Vintermyr, Olav K, and Krohn, Jørgen

Abstract

PURPOSE: To evaluate clinico-pathological and molecular prognostic factors in a well-defined series of posterior uveal melanoma (UM) with focus on chromosomal aberrations and mutations in the GNAQ, GNA11 and BRCA1-associated protein 1 (BAP1) genes.METHODS: Formalin-fixed paraffin-embedded (FFPE) tissue samples were obtained from 50 consecutive eyes enucleated for UM between 1993 and 2005. The material was tested for loss of chromosome 3 and gain of chromosome 8q gene signatures by selective molecular gene markers using multiplex ligation-dependent probe amplification (MLPA), and for DNA mutations in the GNAQ, GNA11 and BAP1 genes.RESULTS: After a mean follow-up of 83 months (range, 8-205 months), 21 patients had died of metastatic UM and 16 patients of other causes. Tumour diameter, ciliary body involvement, mixed/epithelioid cell types, mitotic index, Ki-67 proliferation index, loss of chromosome 3 and gain of chromosome 8q showed statistically significant associations with metastatic disease. There were no significant differences in the prevalence of GNAQ and GNA11 mutations between patients with or without metastatic disease. Mutational analysis of the BAP1 gene was performed in 32 primary UM and in five UM liver metastases. Nine different BAP1 missense mutations were identified. BAP1 mutations were not more common in metastasizing than in nonmetastasizing UM.CONCLUSION: The molecular gene markers showing loss of chromosome 3 and gain of 8q gene signatures were associated with an increased risk of metastatic disease. BRCA1-associated protein 1 (BAP1) gene mutation status had no prognostic significance. The frequency and spectrum of BAP1 mutations in UM may be more dependent on ethnicity and demographic variables than hitherto considered.

Published

2018

6. GNAQ and GNA11 mutations and downstream YAP activation in choroidal nevi

Author

Vader, M.J.C. (M. J.C.), Madigan, M.C. (M. C.), Versluis, M. (Mieke), Suleiman, H.M. (H. M.), Gezgin, G. (Gülçin), Gruis, N.A. (Nelleke A.), Out-Luiting, J.J. (Jacoba), Bergman, W. (Wilma), Verdijk, R.M. (Robert), Jager, M.J. (Martine), Velden, P.A. (Pieter) van der, Vader, M.J.C. (M. J.C.), Madigan, M.C. (M. C.), Versluis, M. (Mieke), Suleiman, H.M. (H. M.), Gezgin, G. (Gülçin), Gruis, N.A. (Nelleke A.), Out-Luiting, J.J. (Jacoba), Bergman, W. (Wilma), Verdijk, R.M. (Robert), Jager, M.J. (Martine), and Velden, P.A. (Pieter) van der

Abstract

Background: Mutations in GNAQ/11 genes are considered an early event in the development of uveal melanoma that may derive from a pre-existing nevus. The Hippo pathway, by way of YAP activation, rather than MAP kinase, has a role in the oncogenic capacity of GNAQ/11 mutations.Methods: We investigated 16 nevi from 13 human eyes for driver GNAQ/11 mutations using droplet digital PCR and determined whether nevi are clonal by quantifying mutant nevus cell fractions. Immunohistochemistry was performed on 15 nevi to analyse YAP activation.Results: For 15 out of 16 nevi, a GNAQ/11 mutation was detected in the nevus cells albeit at a low frequency with a median of 13%. Nuclear YAP, a transcriptional co-activator in the Hippo tumour-suppressor pathway, was detected in 14/15 nevi.Conclusions: Our analysis suggests that a mutation in GNAQ/11 occurs in a subset of choroidal nevus cells. We hypothesise that GNAQ/11 mutant-driven extracellular mitogenic signalling involving YAP activation leads to accumulation of wild-type nevus cells.

Published

2017

7. GNAQ and GNA11 mutations and downstream YAP activation in choroidal nevi

Author

Vader, MJC, Madigan, MC, Versluis, M, Suleiman, HM, Gezgin, G, Gruis, NA, Out-Luiting, JJ, Bergman, W, Verdijk, Rob, Jager, MJ, Van der Velden, PA, Vader, MJC, Madigan, MC, Versluis, M, Suleiman, HM, Gezgin, G, Gruis, NA, Out-Luiting, JJ, Bergman, W, Verdijk, Rob, Jager, MJ, and Van der Velden, PA

Published

2017

8. Patient survival in uveal melanoma is not affected by oncogenic mutations in GNAQ and GNA11

Author

Koopmans, A.E. (Anna), Vaarwater, J. (Jolanda), Paridaens, A.D.A. (Dion), Naus, N.C. (Nicole), Kiliç, E. (Emine), Klein, J.E.M.M. (Annelies) de, Koopmans, A.E. (Anna), Vaarwater, J. (Jolanda), Paridaens, A.D.A. (Dion), Naus, N.C. (Nicole), Kiliç, E. (Emine), and Klein, J.E.M.M. (Annelies) de

Abstract

Background:Mutations in GNAQ and GNA11, encoding the oncogenic G-protein alpha subunit q and 11, respectively, occur frequently in the majority of uveal melanomas. Methods:Exons 4 and 5 from GNAQ and GNA11 were amplified and sequenced from 92 ciliary body and choroidal melanomas. The mutation status was correlated with disease-free survival (DFS) and other parameters. Results:None of the tumours harboured a GNAQ exon 4 mutation. A GNAQ mutation in exon 5 codon 209 was found in 46 out of 92 (50.0%) of the tumours. Only 1 out of 92 (1.1%) melanomas showed a mutation in GNA11 exon 4 codon 183, whereas 39 out of 92 (42.4%) harboured a mutation in exon 5 of GNA11 codon 209. Six tumours did not show any mutations in exons 4 and 5 of these genes. Univariate analyses showed no correlation between DFS and the mutation status. Conclusion:GNAQ and GNA11 mutations are, in equal matter, not associated with patient outcome.British Journal of Cancer advance online publication 18 June 2013; doi:10.1038/bjc.2013.299 www.bjcancer.com.

Published

2013

9. GNA11 and N-RAS mutations: alternatives for MAPK pathway activating GNAQ mutations in primary melanocytic tumours of the central nervous system

Author

Gessi, Marco, Hammes, J, Lauriola, Libero, Dörner, E, Kirfel, J, Kristiansen, G, Zur Muehlen, A, Denkhaus, D, Waha, A, Pietsch, T., Lauriola, Libero (ORCID:0000-0003-0481-5138), Gessi, Marco, Hammes, J, Lauriola, Libero, Dörner, E, Kirfel, J, Kristiansen, G, Zur Muehlen, A, Denkhaus, D, Waha, A, Pietsch, T., and Lauriola, Libero (ORCID:0000-0003-0481-5138)

Abstract

Aim: Primary melanocytic tumours are uncommon neoplasms of the central nervous system. Although similarities with uveal melanomas have been hypothesized, data on their molecular features are limited. Methods: In this study, we investigated the mutational status of BRAF (V600E) , KIT, GNAQ, GNA11, N-RAS and H-RAS in a series of 19 primary melanocytic tumours of the CNS. Results: We identified six cases harbouring mutations in the hotspot codon 209 of the GNAQ gene and two cases with mutations in the hotspot codon 209 of the GNA11 gene. Two mutations in codon 61 of N-RAS were also found. In the SSCP analysis, no shifts corresponding to BRAF(V600E) mutations or suggesting activating mutations in the KIT gene were observed. Conclusions: In primary melanocytic tumours of the CNS, GNA11 and N-RAS mutations represent a mechanism of MAPK pathway activation alternative to the common GNAQ mutations. On the other hand, BRAF(V600E) mutations and activating KIT mutations seem to be absent or very rare in these tumours. © 2012 The Authors. Neuropathology and Applied Neurobiology © 2012 British Neuropathological Society.

Published

2012

10. GNA11- und GNAQ Mutationsanalyse bei unklaren Malignomen - ein neuer diagnostischer Marker für Metastasen des uvealen Melanoms?

Author

Böhm, MRR, Tsianakas, A, Spieker, T, Grenzebach, UH, Merté, RL, Eter, N, Böhm, MRR, Tsianakas, A, Spieker, T, Grenzebach, UH, Merté, RL, and Eter, N

Published

2012

11. MAPK pathway activation by GNAQ and GNA11 mutations in melanocytic tumors of the central nervous system.

Author

Gessi, M, Hammes, J, Lauriola, L, Dörner, E, Kirfel, J, Kristiansen, G, zur Muehlen, A, Denkhaus, D, Waha, A, Pietsch, T, Gessi, M, Hammes, J, Lauriola, L, Dörner, E, Kirfel, J, Kristiansen, G, zur Muehlen, A, Denkhaus, D, Waha, A, and Pietsch, T

Published

2012

12. GNA11- und GNAQ Mutationsanalyse bei unklaren Malignomen - ein neuer diagnostischer Marker für Metastasen des uvealen Melanoms?

Author

Böhm, MRR, Tsianakas, A, Spieker, T, Grenzebach, UH, Merté, RL, Eter, N, Böhm, MRR, Tsianakas, A, Spieker, T, Grenzebach, UH, Merté, RL, and Eter, N

Published

2012

13. MAPK pathway activation by GNAQ and GNA11 mutations in melanocytic tumors of the central nervous system.

Author

Gessi, M, Hammes, J, Lauriola, L, Dörner, E, Kirfel, J, Kristiansen, G, zur Muehlen, A, Denkhaus, D, Waha, A, Pietsch, T, Gessi, M, Hammes, J, Lauriola, L, Dörner, E, Kirfel, J, Kristiansen, G, zur Muehlen, A, Denkhaus, D, Waha, A, and Pietsch, T

Published

2012

14. Prognostic Values of G-Protein Mutations in Metastatic Uveal Melanoma

Author

Terai, Mizue, Shimada, Ayako, I Chervoneva, Hulse, Liam, Danielson, Meggie, Swensen, Jeff, Orloff, Marlana, Wedegaertner, Philip B, Benovic, Jeffrey L, Aplin, A E, Sato, Takami, Terai, Mizue, Shimada, Ayako, I Chervoneva, Hulse, Liam, Danielson, Meggie, Swensen, Jeff, Orloff, Marlana, Wedegaertner, Philip B, Benovic, Jeffrey L, Aplin, A E, and Sato, Takami

Abstract

Uveal melanoma is the most common primary ocular malignancy in adults, characterized by gene mutations in G protein subunit alpha q (GNAQ) and G protein subunit alpha 11 (GNA11). Although they are considered to be driver mutations, their role in MUM remains elusive. We investigated key somatic mutations of MUM and their impact on patients’ survival after development of systemic metastasis (Met-to-Death). Metastatic lesions from 87 MUM patients were analyzed by next generation sequencing (NGS). GNA11 (41/87) and GNAQ (39/87) mutations were most predominantly seen in MUM. Most GNA11 mutations were Q209L (36/41), whereas GNAQ mutations comprised Q209L (14/39) and Q209P (21/39). Epigenetic pathway mutations BAP1 (42/66), SF3B1 (11/66), FBXW7 (2/87), PBRM1 (1/66), and SETD2 (1/66) were found. No specimen had the EIF1AX mutation. Interestingly, Met-to-Death was longer in patients with GNAQ Q209P compared to GNAQ/GNA11 Q209L mutations, suggesting the difference in mutation type in GNAQ/GNA11 might determine the prognosis of MUM. Structural alterations of the GNAQ/GNA11 protein and their impact on survival of MUM patients should be further investigated.

Published

2021

15. Extracutaneous manifestations in phacomatosis cesioflammea and cesiomarmorata: Case series and literature review.

Author

Kumar, Akash, Kumar, Akash, Zastrow, Diane B, Kravets, Elijah J, Beleford, Daniah, Ruzhnikov, Maura RZ, Grove, Megan E, Dries, Annika M, Kohler, Jennefer N, Waggott, Daryl M, Yang, Yaping, Huang, Yong, Undiagnosed Diseases Network, Mackenzie, Katherine M, Eng, Christine M, Fisher, Paul G, Ashley, Euan A, Teng, Joyce M, Stevenson, David A, Shieh, Joseph T, Wheeler, Matthew T, Bernstein, Jonathan A, Kumar, Akash, Kumar, Akash, Zastrow, Diane B, Kravets, Elijah J, Beleford, Daniah, Ruzhnikov, Maura RZ, Grove, Megan E, Dries, Annika M, Kohler, Jennefer N, Waggott, Daryl M, Yang, Yaping, Huang, Yong, Undiagnosed Diseases Network, Mackenzie, Katherine M, Eng, Christine M, Fisher, Paul G, Ashley, Euan A, Teng, Joyce M, Stevenson, David A, Shieh, Joseph T, Wheeler, Matthew T, and Bernstein, Jonathan A

Abstract

Phacomatosis pigmentovascularis (PPV) comprises a family of rare conditions that feature vascular abnormalities and melanocytic lesions that can be solely cutaneous or multisystem in nature. Recently published work has demonstrated that both vascular and melanocytic abnormalities in PPV of the cesioflammea and cesiomarmorata subtypes can result from identical somatic mosaic activating mutations in the genes GNAQ and GNA11. Here, we present three new cases of PPV with features of the cesioflammea and/or cesiomarmorata subtypes and mosaic mutations in GNAQ or GNA11. To better understand the risk of potentially occult complications faced by such patients we additionally reviewed 176 cases published in the literature. We report the frequency of clinical findings, their patterns of co-occurrence as well as published recommendations for surveillance after diagnosis. Features assessed include: capillary malformation; dermal and ocular melanocytosis; glaucoma; limb asymmetry; venous malformations; and central nervous system (CNS) anomalies, such as ventriculomegaly and calcifications. We found that ocular findings are common in patients with phacomatosis cesioflammea and cesiomarmorata. Facial vascular involvement correlates with a higher risk of seizures (p = .0066). Our genetic results confirm the role of mosaic somatic mutations in GNAQ and GNA11 in phacomatosis cesioflammea and cesiomarmorata. Their clinical and molecular findings place these conditions on a clinical spectrum encompassing other GNAQ and GNA11 related disorders and inform recommendations for their management.

Published

2019

16. Protein and mRNA Expression in Uveal Melanoma Cell Lines Are Related to GNA and BAP1 Mutation Status

Author

Gelmi, Maria Chiara, de Ru, Arnoud H., van Veelen, Peter A., Tjokrodirijo, Rayman T.N., Stern, Marc Henri, Houy, Alexandre, Verdijk, Robert M., Vu, T. H.Khanh, Ksander, Bruce R., Vaarwater, Jolanda, Kilic, Emine, Brosens, Erwin, Jager, Martine J., Gelmi, Maria Chiara, de Ru, Arnoud H., van Veelen, Peter A., Tjokrodirijo, Rayman T.N., Stern, Marc Henri, Houy, Alexandre, Verdijk, Robert M., Vu, T. H.Khanh, Ksander, Bruce R., Vaarwater, Jolanda, Kilic, Emine, Brosens, Erwin, and Jager, Martine J.

Abstract

Purpose: Cell lines are being used in preclinical uveal melanoma (UM) research. Because not all cell lines harbor typical GNAQ or GNA11 hotspot mutations, we aimed at better classifying them and determining whether we could find genetic causes to explain the protein and mRNA expression profiles of the cell lines. Methods: We studied protein and mRNA expression of 14 UM cell lines and determined the presence of single nucleotide variants and small insertions and deletions with next-generation sequencing and copy number alterations with a single nucleotide polymorphism array. The lists of differentially expressed proteins and genes were merged, and shared lists were created, keeping only terms with concordant mRNA and protein expression. Enrichment analyses were performed on the shared lists. Results:Cell lines Mel285 and Mel290 are separate from GNA-mutated cell lines and show downregulation of melanosome-related markers. Both lack typical UM mutations but each harbors four putatively deleterious variants in CTNNB1, PPP1R10, LIMCH1, and APC in Mel285 and ARID1A, PPP1R10, SPG11, and RNF43 in Mel290. The upregulated terms in Mel285 and Mel290 did not point to a convincing alternative origin. Mel285 shows loss of chromosomes 1p, 3p, partial 3q, 6, and partial 8p, whereas Mel290 shows loss of 1p and 6. Expression in the other 12 cell lines was related to BAP1 expression.Conclusions: Although Mel285 and Mel290 have copy number alterations that fit UM, multi-omics analyses show that they belong to a separate group compared to the other analyzed UM cell lines. Therefore, they may not be representative models to test potential therapeutic targets for UM.

Published

2024

17. Primary Meningeal Melanocytic Tumors of the Central Nervous System:A Review from the Ultra-Rare Brain Tumors Task Force of the European Network for Rare Cancers (EURACAN)

Author

Pellerino, Alessia, Verdijk, Robert M., Nichelli, Lucia, Andratschke, Nicolaus H., Idbaih, Ahmed, Goldbrunner, Roland, Pellerino, Alessia, Verdijk, Robert M., Nichelli, Lucia, Andratschke, Nicolaus H., Idbaih, Ahmed, and Goldbrunner, Roland

Abstract

Background: Primary meningeal melanocytic tumors are ultra-rare entities with distinct histological and molecular features compared with other melanocytic or pigmented lesions, such as brain and leptomeningeal metastases from metastatic melanoma. Methods: The European Network for Rare Cancers (EURACAN) Task Force on Ultra-Rare Brain Tumors (domain 10, subdomain 10) performed a literature review from January 1985 to December 2023 regarding the epidemiologic and clinical characteristics, histological and molecular features, radiological findings, and efficacy of local treatments (surgery and radiotherapy) and systemic treatments for these entities. Results: Molecular analysis can detect specific mutations, including GNAQ, GNA11, SF3B1, EIF1AX, BAP1, that are typically found in circumscribed primary meningeal melanocytic tumors and not in other melanocytic lesions, whereas NRAS and BRAF mutations are typical for diffuse primary meningeal melanocytic tumors. The neuroimaging of the whole neuroaxis suggests a melanocytic nature of a lesion, depicts its circumscribed or diffuse nature, but cannot predict the tumor’s aggressiveness. Gross-total resection is the first choice in the case of circumscribed meningeal melanocytoma and melanoma; conversely, meningeal biopsy may be reserved for patients with diffuse and multinodular leptomeningeal spread to achieve a definitive diagnosis. High-dose radiotherapy is rarely indicated in diffuse melanocytic tumors except as palliative treatment to alleviate symptoms. Last, a definitive advantage of a specific systemic treatment could not be concluded, as most of the data available derive from case reports or small cohorts. Conclusions: As primary meningeal melanocytic tumors are extremely rare, the correlations between the clinical characteristics, molecular profile, radiological findings at diagnosis and progression are weak, and poor evidence on the best

Published

2024

18. Somatic Loss-of-Function PIK3R1 and Activating Non-hotspot PIK3CA Mutations Associated with Capillary Malformation with Dilated Veins (CMDV)

Author

De Bortoli, Martina, Queisser, Angela, Pham, Van Cuong, Dompmartin, A., Helaers, Raphaël, Boutry, Simon, Claus, Cathy, De Roo, An Katrien, Hammer, Frank, Brouillard, Pascal, Abdelilah-Seyfried, Salim, Boon, Laurence L.M., Vikkula, Mikka, De Bortoli, Martina, Queisser, Angela, Pham, Van Cuong, Dompmartin, A., Helaers, Raphaël, Boutry, Simon, Claus, Cathy, De Roo, An Katrien, Hammer, Frank, Brouillard, Pascal, Abdelilah-Seyfried, Salim, Boon, Laurence L.M., and Vikkula, Mikka

Abstract

Common capillary malformations are red vascular skin lesions, most commonly associated with somatic activating GNAQ or GNA11 mutations. We focused on capillary malformations lacking such a mutation to identify previously unreported genetic causes. We used targeted next-generation sequencing on 82 lesions. Bioinformatic analysis allowed the identification of 9 somatic pathogenic variants in PIK3R1 and PIK3CA, encoding for the regulatory and catalytic subunits of phosphoinositide 3-kinase, respectively. Recharacterization of these lesions unraveled a common phenotype: a pale capillary malformation associated with visible dilated veins. Primary endothelial cells from 2 PIK3R1-mutated lesions were isolated, and PI3k-Akt-mTOR and RAS–RAF–MAPK signaling were assessed by western blot. This unveiled an abnormal increase in Akt phosphorylation, effectively reduced by PI3K pathway inhibitors, such as mTOR, Akt, and PIK3CA inhibitors. The effects of mutant PIK3R1 were further studied using zebrafish embryos. Endothelium-specific expression of PIK3R1 mutants resulted in abnormal development of the posterior capillary–venous plexus. In summary, capillary malformation associated with visible dilated veins emerges as a clinical entity associated with somatic pathogenic variants in PIK3R1 or PIK3CA (nonhotspot). Our findings suggest that the activated Akt signaling can be effectively reversed by PI3K pathway inhibitors. In addition, the proposed zebrafish model holds promise as a valuable tool for future drug screening aimed at developing patient-tailored treatments., SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2024

19. The Pediatric and Young Adult Choroidal and Ciliary Body Melanoma Genetic Study, A Survey by the European Ophthalmic Oncology Group

Author

van Poppelen, Natasha M., Cassoux, Nathalie, Turunen, Joni A., Naus, Nicole C., Verdijk, Robert M., Vaarwater, Jolanda, Cohen, Victoria, Papastefanou, Vasilios P., Kiratli, Hayyam, Saakyan, Svetlana V., Tsygankov, Alexander Y., Rospond-Kubiak, Iwona, Mudhar, Hardeep S., Salvi, Sachin M., Kiilgaard, Jens F., Heegaard, Steffen, Moulin, Alexandre P., Saornil, Maria A., Garciá-Alvarez, Ciro, Fili, Maria, Eide, Nils A., Meyer, Peter, Kivela, Tero T., de Klein, Annelies, Kilic, Emine, Al-Jamal, Ranaa T., van Poppelen, Natasha M., Cassoux, Nathalie, Turunen, Joni A., Naus, Nicole C., Verdijk, Robert M., Vaarwater, Jolanda, Cohen, Victoria, Papastefanou, Vasilios P., Kiratli, Hayyam, Saakyan, Svetlana V., Tsygankov, Alexander Y., Rospond-Kubiak, Iwona, Mudhar, Hardeep S., Salvi, Sachin M., Kiilgaard, Jens F., Heegaard, Steffen, Moulin, Alexandre P., Saornil, Maria A., Garciá-Alvarez, Ciro, Fili, Maria, Eide, Nils A., Meyer, Peter, Kivela, Tero T., de Klein, Annelies, Kilic, Emine, and Al-Jamal, Ranaa T.

Abstract

PURPOSE:To explore the genetic background of choroidal and ciliary body melanoma among children and young adults, with special focus on BAP1 germline variants in this age group. METHODS:Patients under the age of 25 and with confirmed choroidal or ciliary body melanoma were included in this retrospective, multicenter observational study. Nuclear BAP1 immunopositivity was used to evaluate the presence of functional BAP1 in the tumor. Next-generation sequencing using Ion Torrent platform was used to determine pathogenic variants of BAP1, EIF1AX, SF3B1, GNAQ and GNA11 and chromosome 3 status in the tumor or in DNA extracted from blood or saliva. Survival was analyzed using Kaplan-Meier estimates. RESULTS:The mean age at diagnosis was 17 years (range 5.0–24.8). A germline BAP1 pathogenic variant was identified in an 18-year-old patient, and a somatic variant, based mainly on immunohistochemistry, in 13 (42%) of 31 available specimens. One tumor had a somatic SF3B1 pathogenic variant. Disomy 3 and the absence of a BAP1 pathogenic variant in the tumor predicted the longest metastasis-free survival. Males showed longer metastasis-free survival than females (P = 0.018). CONCLUSIONS:We did not find a stronger-than-average BAP1 germline predisposition for choroidal and ciliary body melanoma among children and young adults compared to adults. Males had a more favorable survival and disomy 3, and the absence of a BAP1 mutation in the tumor tissue predicted the most favorable metastasis-free survival. A BAP1 germline pathogenic variant was identified in one patient (1%), and a somatic variant based mainly on immunohistochemistry in 13 (42%).

Published

2024

20. GNA11‐mutated Sturge‐Weber Syndrome has distinct neurologica.

Author

UCL - SSS/DDUV/GEHU - Génétique, UCL - (SLuc) Centre de malformations vasculaires congénitales, Dompmartin, Anne, van der Vleuten, Carine J. M., Dekeuleneer, Valérie, Duprez, Thierry, Revencu, Nicole, Désir, Julie, te Loo, D. Maroeska W. M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Miikka, Boon, Laurence, UCL - SSS/DDUV/GEHU - Génétique, UCL - (SLuc) Centre de malformations vasculaires congénitales, Dompmartin, Anne, van der Vleuten, Carine J. M., Dekeuleneer, Valérie, Duprez, Thierry, Revencu, Nicole, Désir, Julie, te Loo, D. Maroeska W. M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Miikka, and Boon, Laurence

Abstract

Background: Sturge-Weber syndrome (SWS) is a neurocutaneous disorder characterized by clinical manifestations involving the brain, eye and skin. SWS is commonly caused by somatic mutations in G protein subunit Alpha Q (GNAQ). Subunit Alpha 11 (GNA11) mutations have been reported in 5 cases. It is not clear if their phenotypic features differ. Methods: Within two European multidisciplinary centers we looked for patients with clinical characteristics of SWS and a GNA11 mutation. Clinical and radiological data was collected retrospectively and prospectively. Results: We identified three patients with SWS associated with a somatic GNA11 mutation. They had disseminated capillary malformation (CM) and hyper- or hypotrophy of an extremity. At birth, the CMs of the face, trunk and limbs were pink and patchy, and slowly darkened with age evolving to purple color. Two of the patients had glaucoma. All had neurological symptoms and moderate brain atrophy at a lower degree of severity than classically associated with SWS. Susceptibility-Weighted Images (SWI) and contrast-enhanced (CE) Fluid Attenuated Inversion Recovery (FLAIR) MR views demonstrated best sensitivity to reveal the pial angiomas. Conclusions: We differentiate two distinct clinical/radiological phenotypes of SWS; GNAQ- and GNA11-SWS. The classical GNAQ-SWS is characterized by a homogeneous dark-red CM commonly associated with underlying soft tissue hypertrophy. The CM in GNA11-SWS is more reticulate and darkens with time; neurological picture is milder. SWI and post contrast FLAIR sequences appear to be necessary to demonstrate the leptomeningeal angiomatosis. Yet, anti-epileptic medication or future targeted therapies may be useful, like in classic SWS.

Published

2022

21. GNA11-mutated Sturge–Weber syndrome has distinct neurological and dermatological features

Author

UCL - SSS/DDUV/GEHU - Génétique, Dompmartin, Anne, van der Vleuten, Carine J. M., Dekeuleneer, Valérie, Duprez, Thierry, Revencu, Nicole, Désir, Julie, te Loo, D. Maroeska W. M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Miikka, Boon, Laurence, UCL - SSS/DDUV/GEHU - Génétique, Dompmartin, Anne, van der Vleuten, Carine J. M., Dekeuleneer, Valérie, Duprez, Thierry, Revencu, Nicole, Désir, Julie, te Loo, D. Maroeska W. M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Miikka, and Boon, Laurence

Abstract

Background and purpose: Sturge–Weber syndrome (SWS) is a neurocutaneous disorder characterized by clinical manifestations involving the brain, eye and skin. SWS is commonly caused by somatic mutations in G protein subunit Alpha Q (GNAQ). Five cases of subunit Alpha 11 (GNA11) mutations have been reported. We studied phenotypic features of GNA11-SWS and compared them with those of classic SWS. Methods: Within two European multidisciplinary centers we looked for patients with clinical characteristics of SWS and a GNA11 mutation. Clinical and radiological data were collected retrospectively and prospectively. Results: We identified three patients with SWS associated with a somatic GNA11 mutation. All had disseminated capillary malformation (CM) and hyper-or hypotrophy of an extremity. At birth, the CMs of the face, trunk and limbs were pink and patchy, and slowly darkened with age, evolving to a purple color. Two of the patients had glaucoma. All had neurological symptoms and moderate brain atrophy with a lower degree of severity than that classically associated with SWS. Susceptibility-weighted imaging (SWI) and contrast-enhanced fluid-attenuated inversion recovery (FLAIR) magnetic resonance imaging demonstrated the best sensitivity to reveal the pial angiomas. Conclusions: We have differentiated two distinct clinical/radiological phenotypes of SWS; GNAQ-and GNA11-SWS. The classic GNAQ-SWS is characterized by a homogeneous dark-red CM, commonly associated with underlying soft tissue hypertrophy. The CM in GNA11-SWS is more reticulate and darkens with time, and the neurological picture is milder. SWI and post-contrast FLAIR sequences appear to be necessary to demonstrate leptomeningeal angiomatosis. Anti-epileptic medication or future targeted therapies may be useful, as in classic SWS.

Published

2022

22. GNA11-mutated Sturge-Weber syndrome has distinct neurological and dermatological features

Author

Dompmartin, A., Vleuten, C.J.M. van der, Dekeuleneer, V., Duprez, T., Revencu, N., Désir, J., Loo, D.M.W.M. te, Flucke, U.E., Eijkelenboom, A., Schultze Kool, L.J., Vikkula, M., Boon, L., Dompmartin, A., Vleuten, C.J.M. van der, Dekeuleneer, V., Duprez, T., Revencu, N., Désir, J., Loo, D.M.W.M. te, Flucke, U.E., Eijkelenboom, A., Schultze Kool, L.J., Vikkula, M., and Boon, L.

Abstract

Item does not contain fulltext, BACKGROUND AND PURPOSE: Sturge-Weber syndrome (SWS) is a neurocutaneous disorder characterized by clinical manifestations involving the brain, eye and skin. SWS is commonly caused by somatic mutations in G protein subunit Alpha Q (GNAQ). Five cases of subunit Alpha 11 (GNA11) mutations have been reported. We studied phenotypic features of GNA11-SWS and compared them with those of classic SWS. METHODS: Within two European multidisciplinary centers we looked for patients with clinical characteristics of SWS and a GNA11 mutation. Clinical and radiological data were collected retrospectively and prospectively. RESULTS: We identified three patients with SWS associated with a somatic GNA11 mutation. All had disseminated capillary malformation (CM) and hyper- or hypotrophy of an extremity. At birth, the CMs of the face, trunk and limbs were pink and patchy, and slowly darkened with age, evolving to a purple color. Two of the patients had glaucoma. All had neurological symptoms and moderate brain atrophy with a lower degree of severity than that classically associated with SWS. Susceptibility-weighted imaging (SWI) and contrast-enhanced fluid-attenuated inversion recovery (FLAIR) magnetic resonance imaging demonstrated the best sensitivity to reveal the pial angiomas. CONCLUSIONS: We have differentiated two distinct clinical/radiological phenotypes of SWS; GNAQ- and GNA11-SWS. The classic GNAQ-SWS is characterized by a homogeneous dark-red CM, commonly associated with underlying soft tissue hypertrophy. The CM in GNA11-SWS is more reticulate and darkens with time, and the neurological picture is milder. SWI and post-contrast FLAIR sequences appear to be necessary to demonstrate leptomeningeal angiomatosis. Anti-epileptic medication or future targeted therapies may be useful, as in classic SWS.

Published

2022

23. GNA11-mutated Sturge–Weber syndrome has distinct neurological and dermatological features

Author

Dompmartin, A., van der Vleuten, Catharina Joanna Maria, Dekeuleneer, Valérie, Duprez, T., Revencu, Nicole, Désir, Julie, te Loo, Dunja Maroeska D.M.W.M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Mikka, Boon, Laurence Myriam, Dompmartin, A., van der Vleuten, Catharina Joanna Maria, Dekeuleneer, Valérie, Duprez, T., Revencu, Nicole, Désir, Julie, te Loo, Dunja Maroeska D.M.W.M., Flucke, Uta, Eijkelenboom, Astrid, Schultze Kool, Leo, Vikkula, Mikka, and Boon, Laurence Myriam

Abstract

Background and purpose: Sturge–Weber syndrome (SWS) is a neurocutaneous disorder characterized by clinical manifestations involving the brain, eye and skin. SWS is commonly caused by somatic mutations in G protein subunit Alpha Q (GNAQ). Five cases of subunit Alpha 11 (GNA11) mutations have been reported. We studied phenotypic features of GNA11-SWS and compared them with those of classic SWS. Methods: Within two European multidisciplinary centers we looked for patients with clinical characteristics of SWS and a GNA11 mutation. Clinical and radiological data were collected retrospectively and prospectively. Results: We identified three patients with SWS associated with a somatic GNA11 mutation. All had disseminated capillary malformation (CM) and hyper- or hypotrophy of an extremity. At birth, the CMs of the face, trunk and limbs were pink and patchy, and slowly darkened with age, evolving to a purple color. Two of the patients had glaucoma. All had neurological symptoms and moderate brain atrophy with a lower degree of severity than that classically associated with SWS. Susceptibility-weighted imaging (SWI) and contrast-enhanced fluid-attenuated inversion recovery (FLAIR) magnetic resonance imaging demonstrated the best sensitivity to reveal the pial angiomas. Conclusions: We have differentiated two distinct clinical/radiological phenotypes of SWS; GNAQ- and GNA11-SWS. The classic GNAQ-SWS is characterized by a homogeneous dark-red CM, commonly associated with underlying soft tissue hypertrophy. The CM in GNA11-SWS is more reticulate and darkens with time, and the neurological picture is milder. SWI and post-contrast FLAIR sequences appear to be necessary to demonstrate leptomeningeal angiomatosis. Anti-epileptic medication or future targeted therapies may be useful, as in classic SWS., SCOPUS: ar.j, DecretOANoAutActif, info:eu-repo/semantics/published

Published

2022

24. Molecular genetics of conjunctival melanoma and prognostic value of tert promoter mutation analysis

Author

N.M. (Natasha) van Poppelen, J.A. (Jolique) van Ipenburg, Q.C.C. (Quincy) van den Bosch, J.W.C. (Jolanda) Witteman - Vaarwater, T. (Tom) Brands, HJFMM (Bert) Eussen, F.J. (Frank) Magielsen, H.J. (Erik jan) Dubbink, A.D.A. (Dion) Paridaens, E. (Erwin) Brosens, N.C. (Nicole) Naus, J.E.M.M. (Annelies) de Klein, E. (Emine) Kiliç, R.M. (Rob) Verdijk, N.M. (Natasha) van Poppelen, J.A. (Jolique) van Ipenburg, Q.C.C. (Quincy) van den Bosch, J.W.C. (Jolanda) Witteman - Vaarwater, T. (Tom) Brands, HJFMM (Bert) Eussen, F.J. (Frank) Magielsen, H.J. (Erik jan) Dubbink, A.D.A. (Dion) Paridaens, E. (Erwin) Brosens, N.C. (Nicole) Naus, J.E.M.M. (Annelies) de Klein, E. (Emine) Kiliç, and R.M. (Rob) Verdijk

Abstract

The aim of this study was exploration of the genetic background of conjunctival melanoma (CM) and correlation with recurrent and metastatic disease. Twenty-eight CM from the Rotterdam Ocular Melanoma Study group were collected and DNA was isolated from the formalin-fixed paraffin embedded tissue. Targeted next-generation sequencing was performed using a panel covering GNAQ, GNA11, EIF1AX, BAP1, BRAF, NRAS, c-KIT, PTEN, SF3B1, and TERT genes. Recurrences and metastasis were present in eight (29%) and nine (32%) CM cases, respectively. TERT promoter mutations were most common (54%), but BRAF (46%), NRAS (21%), BAP1 (18%), PTEN (14%), c-KIT (7%), and SF3B1 (4%) mutations were also observed. No mutations in GNAQ, GNA11, and EIF1AX were found. None of the mutations was significantly associated with recurrent disease. Presence of a TERT promoter mutation was associated with metastatic disease (p-value = 0.008). Based on our molecular findings, CM comprises a separate entity within melanoma, although there are overlapping molecular features with uveal melanoma, such as the presence of BAP1 and SF3B1 mutations. This warrants careful interpretation of molecular data, in the light of clinical findings. About three quarter of CM contain drug-targetable mutations, and TERT promoter mutations are correlated to metastatic disease in CM.

Published

2021

25. Mutational Characterization of Cutaneous Melanoma Supports Divergent Pathways Model for Melanoma Development

Author

Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, European Academy of Dermatology and Venereology, Millán-Esteban, David, Peña-Chilet, María, García-Casado, Zaida, Manrique-Silva, Esperanza, Requena, Celia, Bañuls, José, López-Guerrero, José Antonio, Rodríguez-Hernández, Aranzazu, Traves, Víctor, Dopazo, Joaquín, Virós, Amaya, Kumar, Rajiv, Nagore, Eduardo, Ministerio de Ciencia e Innovación (España), Instituto de Salud Carlos III, Asociación Española Contra el Cáncer, European Academy of Dermatology and Venereology, Millán-Esteban, David, Peña-Chilet, María, García-Casado, Zaida, Manrique-Silva, Esperanza, Requena, Celia, Bañuls, José, López-Guerrero, José Antonio, Rodríguez-Hernández, Aranzazu, Traves, Víctor, Dopazo, Joaquín, Virós, Amaya, Kumar, Rajiv, and Nagore, Eduardo

Abstract

[Simple Summary] The divergent pathway model established at least two approaches for melanoma development. One was related to a propensity to melanocytic proliferation (nevogenic), and the other was associated with an accumulation of solar damage (CSD). We conducted a retrospective study to examine whether this model had a molecular support using sequencing and bioinformatic tools on a set of cutaneous melanomas corresponding to these two groups. We found that the nevogenic melanomas were associated with mutations in BRAF, while the CSD melanomas were associated with mutations in NF1, ROS1, GNA11, and RAC1. We concluded that nevogenic and CSD melanomas constitute two different biological entities., [Abstract] According to the divergent pathway model, cutaneous melanoma comprises a nevogenic group with a propensity to melanocyte proliferation and another one associated with cumulative solar damage (CSD). While characterized clinically and epidemiologically, the differences in the molecular profiles between the groups have remained primarily uninvestigated. This study has used a custom gene panel and bioinformatics tools to investigate the potential molecular differences in a thoroughly characterized cohort of 119 melanoma patients belonging to nevogenic and CSD groups. We found that the nevogenic melanomas had a restricted set of mutations, with the prominently mutated gene being BRAF. The CSD melanomas, in contrast, showed mutations in a diverse group of genes that included NF1, ROS1, GNA11, and RAC1. We thus provide evidence that nevogenic and CSD melanomas constitute different biological entities and highlight the need to explore new targeted therapies.

Published

2021

26. Molecular genetics of conjunctival melanoma and prognostic value of tert promoter mutation analysis

Author

van Poppelen, Natasha M., van Ipenburg, Jolique A., van den Bosch, Quincy, Vaarwater, Jolanda, Brands, Tom, Eussen, Bert, Magielsen, Frank, Dubbink, Hendrikus J., Paridaens, Dion, Brosens, Erwin, Naus, Nicole, de Klein, Annelies, Kiliç, Emine, Verdijk, Robert M., van Poppelen, Natasha M., van Ipenburg, Jolique A., van den Bosch, Quincy, Vaarwater, Jolanda, Brands, Tom, Eussen, Bert, Magielsen, Frank, Dubbink, Hendrikus J., Paridaens, Dion, Brosens, Erwin, Naus, Nicole, de Klein, Annelies, Kiliç, Emine, and Verdijk, Robert M.

Abstract

The aim of this study was exploration of the genetic background of conjunctival melanoma (CM) and correlation with recurrent and metastatic disease. Twenty-eight CM from the Rotterdam Ocular Melanoma Study group were collected and DNA was isolated from the formalin-fixed paraffin embedded tissue. Targeted next-generation sequencing was performed using a panel covering GNAQ, GNA11, EIF1AX, BAP1, BRAF, NRAS, c-KIT, PTEN, SF3B1, and TERT genes. Recurrences and metastasis were present in eight (29%) and nine (32%) CM cases, respectively. TERT promoter mutations were most common (54%), but BRAF (46%), NRAS (21%), BAP1 (18%), PTEN (14%), c-KIT (7%), and SF3B1 (4%) mutations were also observed. No mutations in GNAQ, GNA11, and EIF1AX were found. None of the mutations was significantly associated with recurrent disease. Presence of a TERT promoter mutation was associated with metastatic disease (p-value = 0.008). Based on our molecular findings, CM comprises a separate entity within melanoma, although there are overlapping molecular features with uveal melanoma, such as the presence of BAP1 and SF3B1 mutations. This warrants careful interpretation of molecular data, in the light of clinical findings. About three quarter of CM contain drug-targetable mutations, and TERT promoter mutations are correlated to metastatic disease in CM.

Published

2021

27. Genetics of ocular melanoma: Insights into genetics, inheritance and testing

Author

van Poppelen, Natasha, de Bruyn, Daniël, Bicer, Tolga, Verdijk, Rob, Naus, Nicole, Mensink, HW, Paridaens, Dion, de Klein, Annelies, Brosens, Erwin, Kiliç, Emine, van Poppelen, Natasha, de Bruyn, Daniël, Bicer, Tolga, Verdijk, Rob, Naus, Nicole, Mensink, HW, Paridaens, Dion, de Klein, Annelies, Brosens, Erwin, and Kiliç, Emine

Abstract

Ocular melanoma consists of posterior uveal melanoma, iris melanoma and conjunctival melanoma. These malignancies derive from melanocytes in the uveal tract or conjunctiva. The genetic profiles of these different entities differ from each other. In uveal melanoma, GNAQ and GNA11 gene mutations are frequently found and prognosis is based on mutation status of BAP1, SF3B1 and EIF1AX genes. Iris melanoma, also originating from the uvea, has similarities to the genetic makeups of both posterior uveal melanoma (UM) and conjunctival melanoma since mutations in GNAQ and GNA11 are less common and genes involved in conjunctival melanoma such as BRAF have been described. The genetic spectrum of conjunctival melanoma, however, includes frequent mutations in the BRAF, NRAS and TERT promoter genes, which are found in cutaneous melanoma as well. The BRAF status of the tumor is not correlated to prognosis, whereas the TERT promoter gene mutations are. Clinical presentation, histopathological characteristics and copy number alterations are associated with survival in ocular melanoma. Tissue material is needed to classify ocular melanoma in the different subgroups, which creates a need for the use of noninvasive techniques to prognosticate patients who underwent eye preserving treatment.

Published

2021

28. MicroRNA-1249 Targets G Protein Subunit Alpha 11 and Facilitates Gastric Cancer Cell Proliferation, Motility and Represses Cell Apoptosis

Author

Zhang,Hongzhu, Fu,Tingting, Zhang,Cuiping, Zhang,Hongzhu, Fu,Tingting, and Zhang,Cuiping

Abstract

Hongzhu Zhang,1,* Tingting Fu,1,* Cuiping Zhang2 1Department of Gastroenterology, Jinan Jigang Hospital, Jinan, Shandong, 250101, People’s Republic of China; 2Department of Gastroenterology, The Affiliated Hospital of Qingdao University, Qingdao, Shandong, 266000, People’s Republic of China*These authors contributed equally to this workCorrespondence: Cuiping ZhangDepartment of Gastroenterology, The Affiliated Hospital of Qingdao University, 16 Jiangsu Road, Shinan District, Qingdao, Shandong, 266000, People’s Republic of ChinaEmail zhangcuiping66@sohu.comAim: The purpose of our study was to investigate the effects of miR-1249 in gastric cancer.Methods: By analyzing the data obtained from TCGA database, the expression and prognosis of miR-1249 in gastric cancer patients were analyzed. Then, CCK8, colony forming and transwell assays were used to test cell proliferation and motility. The cell apoptosis was detected by flow cytometry. The Pearson correlation coefficient analyzed was applied to analyze the correlation between GNA11 and miR-1249. qRT-PCR and Western blotting assays were employed to detect the mRNA and protein levels.Results: We discovered that miR-1249 was highly expressed and was associated with a worse prognosis in gastric cancer patients. Besides, miR-1249 was up-regulated in gastric cancer cell lines (AGS, MKN45 and SNU1). More interestingly, miR-1249 exerted facilitating impacts on gastric cancer cell proliferation and motility, whereas miR-1249 acted as a suppressing effect on gastric cancer apoptosis. G protein subunit alpha 11 (GNA11) was a target gene of miR-1249 and was negatively correlated with miR-1249. Furthermore, GNA11 was negatively regulated by miR-1249. Additionally, GNA11 was lowly expressed in gastric cancer tissues and cell lines, as well as low GNA11 expression, was related to poor overall survival results in gastric cancer patients. The promoting influences of miR-1249 over-expression on AGS cell prol

Published

2021

29. Targeted next generation sequencing reveals unique mutation profile of primary melanocytic tumors of the central nervous system.

Author

Van De Nes, J, Gessi, M, Sucker, A, Möller, I, Stiller, M, Horn, S, Scholz, Sl, Pischler, C, Stadtler, N, Schilling, B, Zimmer, L, Hillen, U, Scolyer, Ra, Buckland, Me, Lauriola, Libero, Pietsch, T, Waha, A, Schadendorf, D, Murali, R, Griewank, Kg, Lauriola, Libero (ORCID:0000-0003-0481-5138), Van De Nes, J, Gessi, M, Sucker, A, Möller, I, Stiller, M, Horn, S, Scholz, Sl, Pischler, C, Stadtler, N, Schilling, B, Zimmer, L, Hillen, U, Scolyer, Ra, Buckland, Me, Lauriola, Libero, Pietsch, T, Waha, A, Schadendorf, D, Murali, R, Griewank, Kg, and Lauriola, Libero (ORCID:0000-0003-0481-5138)

Abstract

Melanocytic tumors originating in the central nervous system (MT-CNS) are rare tumors that generally have a favorable prognosis, however malignant tumors do occur. Pathogenetically MT-CNS are not well characterized. Similar to uveal melanoma and blue nevi, they frequently harbor activating GNAQ or GNA11 mutations. Rare NRAS mutations have also been reported. Other mutations have not yet been described. We analyzed 19 MT-CNS, 7 uveal melanomas and 19 cutaneous melanomas using a targeted next generation sequencing approach analyzing 29 genes known to be frequently mutated in other melanocytic tumors (in particular uveal and cutaneous melanomas). In concordance with previous studies, cutaneous melanoma samples showed frequent NRAS or BRAF mutations, as well as mutations in other genes (e.g. NF1, RAC1, PIK3CA, ARID1A). Metastasized uveal melanomas exhibited mutations in GNAQ, GNA11 and BAP1. In contrast, MT-CNS almost exclusively demonstrated mutations in GNAQ (71 %) or GNA11 (12 %). Interestingly both GNA11 mutations identified were detected in MT-CNS diagnosed as intermediate grade melanocytomas which also recurred. One of these recurrent cases also harbored an inactivating BAP1 mutation and was found to have lost one copy of chromosome 3. Our findings show that while MT-CNS do have GNAQ or GNA11 mutations, they rarely harbor other recurrent mutations found in uveal or cutaneous melanomas. Considering chromosome 3 and BAP1 loss are robust markers of poor prognosis in uveal melanoma, it will prove interesting to determine whether these genomic alterations are also of prognostic significance in MT-CNS.

Published

2016

30. BRCA-1 associated protein-1 y su relación con el melanoma uveal

Author

Murcia Nadal, Emilio, Diezhandino García, Patricia, Universidad de Valladolid. Facultad de Medicina, Murcia Nadal, Emilio, Diezhandino García, Patricia, and Universidad de Valladolid. Facultad de Medicina

Abstract

El melanoma uveal (MU) es un cáncer infrecuente con una incidencia de 2 casos/millón de habitantes, más común entre los 50 y los 70 años. Se localiza principalmente en la coroides y en un 30-40% de los casos son asintomáticos. Para su diagnóstico no es necesaria la biopsia, pero requiere de un estudio de extensión con TC o RM. Su tratamiento se basa en termoterapia, radioterapia y cirugía en casos seleccionados. El 50% de los casos desarrollará metástasis, mortales al año. Para su tumorogénesis es necesaria una 1ª mutación en GNAQ o GNA11 y una 2ª en BAP1, EIF1AX o SF3B1. BAP-1 es una proteína codificada en el cromosoma 3 con múltiples funciones, como la modificación de la cromatina, la regulación del ciclo y metabolismo celulares, y varias formas de muerte celular, como la apoptosis y la ferroptosis. Posee a su vez un papel en la inflamación y la respuesta inmunitaria. El MU presenta una alta tasa de metástasis, principalmente en hígado. Las mutaciones en BAP-1 se relacionan con un mayor riesgo de metástasis y un peor pronóstico. Las mutaciones germinales en BAP-1 pueden producir el síndrome de predisposición tumoral asociado a BAP-1 (TPDS1) con incremento de incidencia de varios cánceres, entre ellos el melanoma uveal, el melanoma cutáneo, y el cáncer de pulmón., Grado en Medicina

Published

2023

31. Sturge-Weber Syndrome: A Review of Pathophysiology, Genetics, Clinical Features, and Current Management Approache

Author

Sánchez-Espino,Luis Fernando, Ivars,Marta, Antoñanzas,Javier, Baselga,Eulalia, Sánchez-Espino,Luis Fernando, Ivars,Marta, Antoñanzas,Javier, and Baselga,Eulalia

Abstract

Luis Fernando Sánchez-Espino,1 Marta Ivars,1 Javier Antoñanzas,2 Eulalia Baselga1 1Pediatric Dermatology Department, Barcelona Children’s Hospital Sant Joan de Dèu, Barcelona, Cataluña, Spain; 2Dermatology Department, Clínica Universidad de Navarra, Pamplona, Navarra, SpainCorrespondence: Eulalia Baselga, Department of Dermatology, Hospital Sant Joan de Deu, Passeig de Sant Joan de Déu, 2, Esplugues de Llobregat, Barcelona, 08950, Spain, Tel +34-686-68-9669, Email eulalia.baselga@sjd.esAbstract: Sturge-Weber syndrome (SWS) is a congenital, sporadic, and rare neurocutaneous disorder, characterized by the presence of a facial port-wine birthmark (PWB), glaucoma, and neurological manifestations including leptomeningeal angiomatosis and seizures. It is caused by a postzygotic, somatic, gain-of-function variant of the GNAQ gene, and more recently, the GNA11 gene in association with distinctive clinical features. Neuroimaging can help identify and stratify patients at risk for significant complications allowing closer follow-up; although no presymptomatic treatment has been demonstrated to be effective to date, these patients could benefit from early treatment and/or supportive interventions. Choroid plexus (CP) thickness measurements in brain magnetic resonance imaging (MRI) have a high sensitivity and specificity for early and incipient changes in SWS. In contrast, the absence of pathologic findings makes it possible to rule out associated neurological involvement and leads to periodical observation, with new imaging studies only in cases of new clinical signs/symptoms. Periodic ophthalmological examination is also recommended every 3 months during the first year and yearly afterwards to monitor for glaucoma and choroidal hemangiomas. Treatment for SWS depends on the extent and areas that are affected. These include laser surgery for PWB, anticonvulsants in the case of brain involvement, with either seizures or abnormal EEG, and medical treatment or surgery for

Published

2023

32. BRCA-1 associated protein-1 y su relación con el melanoma uveal

Author

Murcia Nadal, Emilio, Diezhandino García, Patricia, Universidad de Valladolid. Facultad de Medicina, Murcia Nadal, Emilio, Diezhandino García, Patricia, and Universidad de Valladolid. Facultad de Medicina

Abstract

El melanoma uveal (MU) es un cáncer infrecuente con una incidencia de 2 casos/millón de habitantes, más común entre los 50 y los 70 años. Se localiza principalmente en la coroides y en un 30-40% de los casos son asintomáticos. Para su diagnóstico no es necesaria la biopsia, pero requiere de un estudio de extensión con TC o RM. Su tratamiento se basa en termoterapia, radioterapia y cirugía en casos seleccionados. El 50% de los casos desarrollará metástasis, mortales al año. Para su tumorogénesis es necesaria una 1ª mutación en GNAQ o GNA11 y una 2ª en BAP1, EIF1AX o SF3B1. BAP-1 es una proteína codificada en el cromosoma 3 con múltiples funciones, como la modificación de la cromatina, la regulación del ciclo y metabolismo celulares, y varias formas de muerte celular, como la apoptosis y la ferroptosis. Posee a su vez un papel en la inflamación y la respuesta inmunitaria. El MU presenta una alta tasa de metástasis, principalmente en hígado. Las mutaciones en BAP-1 se relacionan con un mayor riesgo de metástasis y un peor pronóstico. Las mutaciones germinales en BAP-1 pueden producir el síndrome de predisposición tumoral asociado a BAP-1 (TPDS1) con incremento de incidencia de varios cánceres, entre ellos el melanoma uveal, el melanoma cutáneo, y el cáncer de pulmón., Grado en Medicina

Published

2023

33. Comprehensive molecular and clinicopathological analysis of vascular malformations: A study of 319 cases

Author

Broek, R.W. ten, Eijkelenboom, A., Vleuten, C.J.M. van der, Kamping, E.J., Kets, M., Verhoeven, B.H., Grünberg, K., Schultze Kool, L.J., Tops, B.B.J., Ligtenberg, M.J.L., Flucke, U.E., Broek, R.W. ten, Eijkelenboom, A., Vleuten, C.J.M. van der, Kamping, E.J., Kets, M., Verhoeven, B.H., Grünberg, K., Schultze Kool, L.J., Tops, B.B.J., Ligtenberg, M.J.L., and Flucke, U.E.

Abstract

Contains fulltext : 204299.pdf (publisher's version ) (Open Access), Vascular malformations are part of overgrowth syndromes characterized by somatic mosaic mutations or rarely by germline mutations. Due to their similarities and diversity, clinicopathological classification can be challenging. A comprehensive targeted Next Generation Sequencing screen using Unique Molecular Identifiers with a technical sensitivity of 1% mutant alleles was performed for frequently mutated positions in >/=21 genes on 319 formalin-fixed paraffin-embedded samples. In 132 out of 319 cases pathogenic mosaic mutations were detected affecting genes previously linked to vascular malformations e.g. PIK3CA (n=80), TEK (TIE2) (n=11), AKT1 (n=1), GNAQ (n=7), GNA11 (n=4), IDH1 (n=3), KRAS (n=9), and NRAS (n=1). Six cases harbored a combination of mutations in PIK3CA and in GNA11 (n=2), GNAQ (n=2), or IDH1 (n=2). Aberrations in PTEN and RASA1 with a variant allele frequency approaching 50% suggestive of germline origin were identified in six out of 102 cases tested; four contained a potential second hit at a lower allele frequency. Ninety-one of the total 142 pathogenic mutations were present at a variant allele frequency <10% illustrating the importance of sensitive molecular analysis. Clinicopathological characteristics showed a broad spectrum and overlap when correlated with molecular data. Sensitive screening of recurrently mutated genes in vascular malformations may help to confirm the diagnosis and reveals potential therapeutic options with a significant contribution of PIK3CA/mTOR and RAS-MAPK pathway mutations. The co-existence of two activating pathogenic mutations in parallel pathways illustrates potential treatment challenges and underlines the importance of multigene testing. Detected germline mutations have major clinical impact.

Published

2019

34. Comprehensive molecular and clinicopathological analysis of vascular malformations: A study of 319 cases

Author

Broek, R.W. ten, Eijkelenboom, A., Vleuten, C.J.M. van der, Kamping, E.J., Kets, M., Verhoeven, B.H., Grünberg, K., Schultze Kool, L.J., Tops, B.B.J., Ligtenberg, M.J.L., Flucke, U.E., Broek, R.W. ten, Eijkelenboom, A., Vleuten, C.J.M. van der, Kamping, E.J., Kets, M., Verhoeven, B.H., Grünberg, K., Schultze Kool, L.J., Tops, B.B.J., Ligtenberg, M.J.L., and Flucke, U.E.

Abstract

Contains fulltext : 204299.pdf (publisher's version ) (Open Access), Vascular malformations are part of overgrowth syndromes characterized by somatic mosaic mutations or rarely by germline mutations. Due to their similarities and diversity, clinicopathological classification can be challenging. A comprehensive targeted Next Generation Sequencing screen using Unique Molecular Identifiers with a technical sensitivity of 1% mutant alleles was performed for frequently mutated positions in >/=21 genes on 319 formalin-fixed paraffin-embedded samples. In 132 out of 319 cases pathogenic mosaic mutations were detected affecting genes previously linked to vascular malformations e.g. PIK3CA (n=80), TEK (TIE2) (n=11), AKT1 (n=1), GNAQ (n=7), GNA11 (n=4), IDH1 (n=3), KRAS (n=9), and NRAS (n=1). Six cases harbored a combination of mutations in PIK3CA and in GNA11 (n=2), GNAQ (n=2), or IDH1 (n=2). Aberrations in PTEN and RASA1 with a variant allele frequency approaching 50% suggestive of germline origin were identified in six out of 102 cases tested; four contained a potential second hit at a lower allele frequency. Ninety-one of the total 142 pathogenic mutations were present at a variant allele frequency <10% illustrating the importance of sensitive molecular analysis. Clinicopathological characteristics showed a broad spectrum and overlap when correlated with molecular data. Sensitive screening of recurrently mutated genes in vascular malformations may help to confirm the diagnosis and reveals potential therapeutic options with a significant contribution of PIK3CA/mTOR and RAS-MAPK pathway mutations. The co-existence of two activating pathogenic mutations in parallel pathways illustrates potential treatment challenges and underlines the importance of multigene testing. Detected germline mutations have major clinical impact.

Published

2019

35. Chromosomal rearrangements in uveal melanoma: Chromothripsis

Author

van Poppelen, N.M., Yavuzyigitoglu, S. (Serdar), Smit, K.N., Vaarwater, J. (Jolanda), Eussen, H.J.F.M.M. (Bert), Brands, T., Paridaens, D, Kiliç, E. (Emine), Klein, J.E.M.M. (Annelies) de, van Poppelen, N.M., Yavuzyigitoglu, S. (Serdar), Smit, K.N., Vaarwater, J. (Jolanda), Eussen, H.J.F.M.M. (Bert), Brands, T., Paridaens, D, Kiliç, E. (Emine), and Klein, J.E.M.M. (Annelies) de

Abstract

Uveal melanoma (UM) is the most common primary intraocular malignancy in the Western world. Recurrent mutations in GNAQ, GNA11, CYSLTR2, PLCB4, BAP1, EIF1AX, and SF3B1 are described as well as non-random chromosomal aberrations. Chromothripsis is a rare event in which chromosomes are shattered and rearranged and has been reported in a variety of cancers including UM. SNP arrays of 249 UM from patients who underwent enucleation, biopsy or endoresection were reviewed for the presence of chromothripsis. Chromothripsis was defined as ten or more breakpoints per chromosome involved. Genetic analysis of GNAQ, GNA11, BAP1, SF3B1, and EIF1AX was conducted using Sanger and next-generation sequencing. In addition, immunohistochemistry for BAP1 was performed. Chromothripsis was detected in 7 out of 249 tumors and the affected chromosomes were chromosomes 3, 5, 6, 8, 12, and 13. The mean total of fragments per chromosome was 39.8 (range 12-116). In 1 UM, chromothripsis was present in 2 different chromosomes. GNAQ, GNA11 or CYSLTR2 mutations were present in 6 of these tumors and 5 tumors harbored a BAP1 mutation and/or lacked BAP1 protein expression by immunohistochemistry. Four of these tumors metastasized and for the fifth only short follow-up data are available. One of these metastatic tumors harbored an SF3B1 mutation. No EIF1AX mutations were detected in any of the tumors. To conclude, chromothripsis is a rare event in UM, occurring in 2.8% of samples and without significant association with mutations in any of the common UM driver genes.

Published

2018

36. Knockin mouse with mutant Gα11 mimics human inherited hypocalcemia and is rescued by pharmacologic inhibitors

Author

Roszko, Kelly L, Bi, Ruiye, Gorvin, Caroline M, Bräuner-Osborne, Hans, Xiong, Xiao-Feng, Inoue, Asuka, Thakker, Rajesh V, Strømgaard, Kristian, Gardella, Thomas, Mannstadt, Michael, Roszko, Kelly L, Bi, Ruiye, Gorvin, Caroline M, Bräuner-Osborne, Hans, Xiong, Xiao-Feng, Inoue, Asuka, Thakker, Rajesh V, Strømgaard, Kristian, Gardella, Thomas, and Mannstadt, Michael

Abstract

Heterotrimeric G proteins play critical roles in transducing extracellular signals generated by 7-transmembrane domain receptors. Somatic gain-of-function mutations in G protein α subunits are associated with a variety of diseases. Recently, we identified gain-of-function mutations in Gα11 in patients with autosomal-dominant hypocalcemia type 2 (ADH2), an inherited disorder of hypocalcemia, low parathyroid hormone (PTH), and hyperphosphatemia. We have generated knockin mice harboring the point mutation GNA11 c.C178T (p.Arg60Cys) identified in ADH2 patients. The mutant mice faithfully replicated human ADH2. They also exhibited low bone mineral density and increased skin pigmentation. Treatment with NPS 2143, a negative allosteric modulator of the calcium-sensing receptor (CASR), increased PTH and calcium concentrations in WT and mutant mice, suggesting that the gain-of-function effect of GNA11(R6OC) is partly dependent on coupling to the CASR. Treatment with the Gα11/q-specific inhibitor YM-254890 increased blood calcium in heterozygous but not in homozygous GNA11(R60C) mice, consistent with published crystal structure data showing that Arg60 forms a critical contact with YM-254890. This animal model of ADH2 provides insights into molecular mechanism of this G protein-related disease and potential paths toward new lines of therapy.

Published

2017

37. Uveal melanoma: epidemiology, etiology, and treatment of primary disease

Author

Krantz,Benjamin A, Dave,Nikita, Komatsubara,Kimberly M, Marr,Brian P, Carvajal,Richard D, Krantz,Benjamin A, Dave,Nikita, Komatsubara,Kimberly M, Marr,Brian P, and Carvajal,Richard D

Abstract

Benjamin A Krantz,1 Nikita Dave,2 Kimberly M Komatsubara,2 Brian P Marr,3,4 Richard D Carvajal5 1Division of Hospital Medicine, 2Division of Hematology/Oncology, Columbia University Medical Center, 3Ophthalmic Oncology Service, Memorial Sloan Kettering Cancer Center, 4Department of Ophthalmology, Weill Cornell Medical College, 5Division of Hematology/Oncology, Columbia University Medical Center, New York, NY, USA Abstract: Uveal melanoma (UM) is the most common intraocular malignancy and arises from melanocytes in the iris, ciliary body, or choroid. Early diagnosis and local treatment is crucial, as survival correlates with primary tumor size. However, approximately 50% of patients will develop metastatic disease with 6–12 months’ survival from metastatic diagnosis. Genomic analyses have led to the development of gene-expression profiles that effectively predict metastatic progression; unfortunately, no adjuvant therapy has been shown to prolong survival to date. New insights into the molecular biology of UM have found frequent activating mutations in genes encoding for the G-protein α-subunit, GNAQ and GNA11, and improved understanding of the downstream signaling pathways MAPK, PI3K/Akt, and Hippo have afforded an array of new targets for treatment of this disease. Studies are under way with rationally developed regimens targeting these pathways, and novel agents are under development. We review the diagnosis, management, and surveillance of primary UM and the adjuvant therapy trials under way. Keywords: uveal melanoma, ocular melanoma, GNAQ, GNA11, MAP kinase, MEK

Published

2017

38. Conjunctival melanoma:New insights in tumour genetics and immunology, leading to new therapeutic options

Author

Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, Jager, Martine J., Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, and Jager, Martine J.

Abstract

Recent developments in oncology have led to a better molecular and cellular understanding of cancer, and the introduction of novel therapies. Conjunctival melanoma (CoM) is a rare but potentially devastating disease. A better understanding of CoM, leading to the development of novel therapies, is urgently needed. CoM is characterized by mutations that have also been identified in cutaneous melanoma, e.g. in BRAF, NRAS and TERT. These mutations are distinct from the mutations found in uveal melanoma (UM), affecting genes such as GNAQ, GNA11, and BAP1. Targeted therapies that are successful in cutaneous melanoma may therefore be useful in CoM. A recent breakthrough in the treatment of patients with metastatic cutaneous melanoma was the development of immunotherapy. While immunotherapy is currently sparsely effective in intraocular tumours such as UM, the similarities between CoM and cutaneous melanoma (including in their immunological tumour micro environment) provide hope for the application of immunotherapy in CoM, and preliminary clinical data are indeed emerging to support this use. This review aims to provide a comprehensive overview of the current knowledge regarding CoM, with a focus on the genetic and immunologic understanding. We elaborate on the distinct position of CoM in contrast to other types of melanoma, and explain how new insights in the pathophysiology of this disease guide the development of new, personalized, treatments.

Published

2022

39. Conjunctival melanoma:New insights in tumour genetics and immunology, leading to new therapeutic options

Author

Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, Jager, Martine J., Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, and Jager, Martine J.

Abstract

Recent developments in oncology have led to a better molecular and cellular understanding of cancer, and the introduction of novel therapies. Conjunctival melanoma (CoM) is a rare but potentially devastating disease. A better understanding of CoM, leading to the development of novel therapies, is urgently needed. CoM is characterized by mutations that have also been identified in cutaneous melanoma, e.g. in BRAF, NRAS and TERT. These mutations are distinct from the mutations found in uveal melanoma (UM), affecting genes such as GNAQ, GNA11, and BAP1. Targeted therapies that are successful in cutaneous melanoma may therefore be useful in CoM. A recent breakthrough in the treatment of patients with metastatic cutaneous melanoma was the development of immunotherapy. While immunotherapy is currently sparsely effective in intraocular tumours such as UM, the similarities between CoM and cutaneous melanoma (including in their immunological tumour micro environment) provide hope for the application of immunotherapy in CoM, and preliminary clinical data are indeed emerging to support this use. This review aims to provide a comprehensive overview of the current knowledge regarding CoM, with a focus on the genetic and immunologic understanding. We elaborate on the distinct position of CoM in contrast to other types of melanoma, and explain how new insights in the pathophysiology of this disease guide the development of new, personalized, treatments.

Published

2022

40. Conjunctival melanoma:New insights in tumour genetics and immunology, leading to new therapeutic options

Author

Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, Jager, Martine J., Brouwer, Niels J., Verdijk, Robert M., Heegaard, Steffen, Marinkovic, Marina, Esmaeli, Bita, and Jager, Martine J.

Abstract

Recent developments in oncology have led to a better molecular and cellular understanding of cancer, and the introduction of novel therapies. Conjunctival melanoma (CoM) is a rare but potentially devastating disease. A better understanding of CoM, leading to the development of novel therapies, is urgently needed. CoM is characterized by mutations that have also been identified in cutaneous melanoma, e.g. in BRAF, NRAS and TERT. These mutations are distinct from the mutations found in uveal melanoma (UM), affecting genes such as GNAQ, GNA11, and BAP1. Targeted therapies that are successful in cutaneous melanoma may therefore be useful in CoM. A recent breakthrough in the treatment of patients with metastatic cutaneous melanoma was the development of immunotherapy. While immunotherapy is currently sparsely effective in intraocular tumours such as UM, the similarities between CoM and cutaneous melanoma (including in their immunological tumour micro environment) provide hope for the application of immunotherapy in CoM, and preliminary clinical data are indeed emerging to support this use. This review aims to provide a comprehensive overview of the current knowledge regarding CoM, with a focus on the genetic and immunologic understanding. We elaborate on the distinct position of CoM in contrast to other types of melanoma, and explain how new insights in the pathophysiology of this disease guide the development of new, personalized, treatments.

Published

2022

41. GNA11-mutated Sturge-Weber syndrome has distinct neurological and dermatological features.

Author

Dompmartin, A. and Dompmartin, A.

Subjects

Radboudumc 16: Vascular damage RIHS: Radboud Institute for Health Sciences., Radboudumc 9: Rare cancers RIMLS: Radboud Institute for Molecular Life Sciences.

Published

2022

42. Metastatic disease in polyploid uveal melanoma patients is associated with BAP1 mutations

Author

Yavuzyigitoglu, S. (Serdar), Mensink, H.W. (Hanneke), Smit, K.N. (Kyra), Vaarwater, J. (Jolanda), Verdijk, R.M. (Robert), Beverloo, H.B. (Berna), Brüggenwirth, H.T. (Hennie), Marion, R. (Ronald) van, Dubbink, H.J. (Erik Jan), Paridaens, A.D.A. (Dion), Naus, N.C. (Nicole), Klein, A. (Annelies) de, Kiliç, E. (Emine), Yavuzyigitoglu, S. (Serdar), Mensink, H.W. (Hanneke), Smit, K.N. (Kyra), Vaarwater, J. (Jolanda), Verdijk, R.M. (Robert), Beverloo, H.B. (Berna), Brüggenwirth, H.T. (Hennie), Marion, R. (Ronald) van, Dubbink, H.J. (Erik Jan), Paridaens, A.D.A. (Dion), Naus, N.C. (Nicole), Klein, A. (Annelies) de, and Kiliç, E. (Emine)

Abstract

PURPOSE. Most of the uvea melanoma (UM) display a near-diploid (normal, ~2N) karyotype with only a few chromosomal changes. In contrast to these simple aberrations 18% of the UM samples show a polyploid character (>2N) and this was associated with an unfavorable prognosis. This study attempts to gain insight in the prognostic value of polyploidy in UM. METHODS. In 202 patients the ploidy status of the UM was determined using cytogenetic analysis, fluorescence-in-situ-hybridization (FISH), multiplex ligation dependent probe amplification (MLPA), and/or single nucleotide polymorphism (SNP) array analysis. Immunohistochemistry was used to determine the BAP1 expression and mutation analyses of BAP1 (coding regions) and the mutation hotspots for the SF3B1, EIF1AX, GNAQ, and GNA11 genes was carried out using Sanger sequencing or whole-exome sequencing. RESULTS. Twenty-three patients had a polyploid UM karyotype (11.4%). Patients with a polyploid tumor had larger tumors (15.61 vs. 13.13 mm, P = 0.004), and more often loss of heterozygosity of chromosome 3 (P ¼ 0.003). No difference in occurrence of mutations between polyploid and diploid tumors was observed for BAP1, SF3B1, EIF1AX, GNAQ, and GNA11. Polyploidy did not affect survival (P = 0.143). BAP1 deficiency was the only significant independent prognostic predictor for patients with polyploid tumors, with a 16- fold increased hazard ratio (HR 15.90, P = 0.009). CONCLUSIONS. The prevalence of mutations in the UM related genes is not different in polyploid UM compared with diploid UM. Moreover, similar to patients with diploid UM, BAP1 mutation is the most significant prognostic predictor of metastasis in patients with polyploid UM.

Published

2016

43. Deep sequencing of uveal melanoma identifies a recurrent mutation in PLCB4

Author

Johansson, Peter, Aoude, Lauren G, Wadt, Karin, Glasson, William J, Warrier, Sunil K, Hewitt, Alex W, Kiilgaard, Jens Folke, Heegaard, Steffen, Isaacs, Tim, Franchina, Maria, Ingvar, Christian, Vermeulen, Tersia, Whitehead, Kevin J, Schmidt, Christopher W, Palmer, Jane M, Symmons, Judith, Gerdes, Anne-Marie, Jönsson, Göran, Hayward, Nicholas K, Johansson, Peter, Aoude, Lauren G, Wadt, Karin, Glasson, William J, Warrier, Sunil K, Hewitt, Alex W, Kiilgaard, Jens Folke, Heegaard, Steffen, Isaacs, Tim, Franchina, Maria, Ingvar, Christian, Vermeulen, Tersia, Whitehead, Kevin J, Schmidt, Christopher W, Palmer, Jane M, Symmons, Judith, Gerdes, Anne-Marie, Jönsson, Göran, and Hayward, Nicholas K

Abstract

Next generation sequencing of uveal melanoma (UM) samples has identified a number of recurrent oncogenic or loss-of-function mutations in key driver genes including: GNAQ, GNA11, EIF1AX, SF3B1 and BAP1. To search for additional driver mutations in this tumor type we carried out whole-genome or whole-exome sequencing of 28 tumors or primary cell lines. These samples have a low mutation burden, with a mean of 10.6 protein changing mutations per sample (range 0 to 53). As expected for these sun-shielded melanomas the mutation spectrum was not consistent with an ultraviolet radiation signature, instead, a BRCA mutation signature predominated. In addition to mutations in the known UM driver genes, we found a recurrent mutation in PLCB4 (c.G1888T, p.D630Y, NM_000933), which was validated using Sanger sequencing. The identical mutation was also found in published UM sequence data (1 of 56 tumors), supporting its role as a novel driver mutation in UM. PLCB4 p.D630Y mutations are mutually exclusive with mutations in GNA11 and GNAQ, consistent with PLCB4 being the canonical downstream target of the former gene products. Taken together these data suggest that the PLCB4 hotspot mutation is similarly a gain-of-function mutation leading to activation of the same signaling pathway, promoting UM tumorigenesis.

Published

2016

44. Metastatic Disease in Polyploid Uveal Melanoma Patients Is Associated With BAP1 Mutations

Author

Yavuzyigitoglu, Serdar, Mensink, HW, Smit, Kyra, Vaarwater, Jolanda, Verdijk, Rob, Beverloo, Berna, Brüggenwirth, Hennie, van Marion, Ronald, Dubbink, Erik jan, Paridaens, D, Naus, Nicole, de Klein, Annelies, Kiliç, Emine, Yavuzyigitoglu, Serdar, Mensink, HW, Smit, Kyra, Vaarwater, Jolanda, Verdijk, Rob, Beverloo, Berna, Brüggenwirth, Hennie, van Marion, Ronald, Dubbink, Erik jan, Paridaens, D, Naus, Nicole, de Klein, Annelies, and Kiliç, Emine

Abstract

PURPOSE. Most of the uvea melanoma (UM) display a near-diploid (normal, similar to 2N) karyotype with only a few chromosomal changes. In contrast to these simple aberrations 18% of the UM samples show a polyploid character (>2N) and this was associated with an unfavorable prognosis. This study attempts to gain insight in the prognostic value of polyploidy in UM. METHODS. In 202 patients the ploidy status of the UM was determined using cytogenetic analysis, fluorescence-in-situ-hybridization (FISH), multiplex ligation dependent probe amplification (MLPA), and/or single nucleotide polymorphism (SNP) array analysis. Immunohistochemistry was used to determine the BAP1 expression and mutation analyses of BAP1 (coding regions) and the mutation hotspots for the SF3B1, EIF1AX, GNAQ, and GNA11 genes was carried out using Sanger sequencing or whole-exome sequencing. RESULTS. Twenty-three patients had a polyploid UM karyotype (11.4%). Patients with a polyploid tumor had larger tumors (15.61 vs. 13.13 mm, P = 0.004), and more often loss of heterozygosity of chromosome 3 (P = 0.003). No difference in occurrence of mutations between polyploid and diploid tumors was observed for BAP1, SF3B1, EIF1AX, GNAQ, and GNA11. Polyploidy did not affect survival (P = 0.143). BAP1 deficiency was the only significant independent prognostic predictor for patients with polyploid tumors, with a 16-fold increased hazard ratio (HR 15.90, P = 0.009). CONCLUSIONS. The prevalence of mutations in the UM related genes is not different in polyploid UM compared with diploid UM. Moreover, similar to patients with diploid UM, BAP1 mutation is the most significant prognostic predictor of metastasis in patients with polyploid UM.

Published

2016

45. Mutations in g protein encoding genes and chromosomal alterations in primary leptomeningeal melanocytic neoplasms

Author

Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., Groenen, P.J.T.A., Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., and Groenen, P.J.T.A.

Abstract

Contains fulltext : 153459.pdf (publisher's version ) (Closed access), Limited data is available on the genetic features of primary leptomeningeal melanocytic neoplasms (LMNs). Similarities with uveal melanoma were recently suggested as both entities harbor oncogenic mutations in GNAQ and GNA11. Whether primary LMNs share additional genetic alterations with uveal melanoma including copy number variations is unknown. Twenty primary LMNs ranging from benign and intermediate-grade melanocytomas to melanomas were tested by direct sequencing for hotspot mutations in the genes GNA11, GNAQ, BRAF, NRAS and HRAS. Furthermore, the lesions were tested for copy number variations of chromosomes frequently present in uveal melanoma (1p, 3, 6 and 8q) by multiplex ligation-dependent probe amplification (MLPA). Genome-wide analyses of copy number alterations of two leptomeningeal melanocytic neoplasms were performed using the OncoScan SNP-array. GNAQ(Q209) mutations were present in eleven LMNs, while two of 20 cases carried a GNA11(Q209) mutation. No BRAF, HRAS or NRAS hotspot mutations were detected. Monosomy 3 and gain of 8q were present in one leptomeningeal melanoma, and one intermediate-grade melanocytoma harbored a gain of chromosome 6. With MLPA, the melanocytomas did not show any further gross chromosomal variations. Our data shows that primary LMNs, like uveal melanoma, harbor oncogenic mutations in GNAQ and GNA11 but lack mutations in BRAF, NRAS and HRAS. This finding may help in the differential diagnosis between a primary LMN and a metastasis from a cutaneous melanoma to the central nervous system. Copy number variations in some aggressive LMNs resemble those present in uveal melanoma but their prognostic significance is unclear.

Published

2015

46. Whole-genome copy-number analysis identifies new leads for chromosomal aberrations involved in the oncogenesis and metastastic behavior of uveal melanomas

Author

Engen-van Grunsven, A.C.H. van, Baar, M.P., Pfundt, R.P., Rijntjes, J., Kusters-vandevelde, H.V., Delbecq, A.L., Keunen, J.E.E., Klevering, J., Wesseling, P., Blokx, W.A.M., Groenen, P.J.T.A., Engen-van Grunsven, A.C.H. van, Baar, M.P., Pfundt, R.P., Rijntjes, J., Kusters-vandevelde, H.V., Delbecq, A.L., Keunen, J.E.E., Klevering, J., Wesseling, P., Blokx, W.A.M., and Groenen, P.J.T.A.

Abstract

Item does not contain fulltext, To further elucidate the genetic underpinnings of uveal melanoma (UM) and identify new markers that correlate with disease outcome, archival formalin-fixed, paraffin-embedded enucleation specimens from 25 patients with UM and a mean follow-up of 14 years were analyzed for whole-genome copy-number alterations using OncoScan analysis. Copy-number alterations of chromosomes 1, 3, 6, and 8 were also analyzed in these tumors using multiplex ligation-dependent probe-amplification, and mutations in GNAQ, GNA11, and BAP1 were searched for by Sanger sequencing. Our study confirms the previously reported GNAQ and GNA11 mutation frequencies in UMs as well as the presence of monosomy 3 as a factor strongly indicating poor prognosis. Two cases with metastatic disease, but without monosomy of chromosome 3, showed loss of a small region in the distal part of chromosome 2p. Also, UMs leading to metastatic disease had more chromosomal aberrations than those without metastases. Three UMs lacking a GNAQ or a GNA11 mutation showed a gain of chromosome 8q; one of these cases showed extensive chromothripsis. Another case (with suspect lung metastasis) showed focal chromothripsis. Our whole-genome copy-number analysis shows that focal loss of chromosome 2p may be involved in the metastatic spread of UMs without monosomy 3; metastatic UMs carry more chromosomal aberrations than those without metastases; and chromothripsis may play a role in the oncogenesis of UMs, but does not necessarily indicate a poor prognosis. The clinical and particularly diagnostic utility of these findings needs to be corroborated in a larger set of patients with UM.

Published

2015

47. Mutations in g protein encoding genes and chromosomal alterations in primary leptomeningeal melanocytic neoplasms

Author

Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., Groenen, P.J.T.A., Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., and Groenen, P.J.T.A.

Abstract

Contains fulltext : 153459.pdf (publisher's version ) (Closed access), Limited data is available on the genetic features of primary leptomeningeal melanocytic neoplasms (LMNs). Similarities with uveal melanoma were recently suggested as both entities harbor oncogenic mutations in GNAQ and GNA11. Whether primary LMNs share additional genetic alterations with uveal melanoma including copy number variations is unknown. Twenty primary LMNs ranging from benign and intermediate-grade melanocytomas to melanomas were tested by direct sequencing for hotspot mutations in the genes GNA11, GNAQ, BRAF, NRAS and HRAS. Furthermore, the lesions were tested for copy number variations of chromosomes frequently present in uveal melanoma (1p, 3, 6 and 8q) by multiplex ligation-dependent probe amplification (MLPA). Genome-wide analyses of copy number alterations of two leptomeningeal melanocytic neoplasms were performed using the OncoScan SNP-array. GNAQ(Q209) mutations were present in eleven LMNs, while two of 20 cases carried a GNA11(Q209) mutation. No BRAF, HRAS or NRAS hotspot mutations were detected. Monosomy 3 and gain of 8q were present in one leptomeningeal melanoma, and one intermediate-grade melanocytoma harbored a gain of chromosome 6. With MLPA, the melanocytomas did not show any further gross chromosomal variations. Our data shows that primary LMNs, like uveal melanoma, harbor oncogenic mutations in GNAQ and GNA11 but lack mutations in BRAF, NRAS and HRAS. This finding may help in the differential diagnosis between a primary LMN and a metastasis from a cutaneous melanoma to the central nervous system. Copy number variations in some aggressive LMNs resemble those present in uveal melanoma but their prognostic significance is unclear.

Published

2015

48. Whole-genome copy-number analysis identifies new leads for chromosomal aberrations involved in the oncogenesis and metastastic behavior of uveal melanomas

Author

Engen-van Grunsven, A.C.H. van, Baar, M.P., Pfundt, R.P., Rijntjes, J., Kusters-vandevelde, H.V., Delbecq, A.L., Keunen, J.E.E., Klevering, J., Wesseling, P., Blokx, W.A.M., Groenen, P.J.T.A., Engen-van Grunsven, A.C.H. van, Baar, M.P., Pfundt, R.P., Rijntjes, J., Kusters-vandevelde, H.V., Delbecq, A.L., Keunen, J.E.E., Klevering, J., Wesseling, P., Blokx, W.A.M., and Groenen, P.J.T.A.

Abstract

Item does not contain fulltext, To further elucidate the genetic underpinnings of uveal melanoma (UM) and identify new markers that correlate with disease outcome, archival formalin-fixed, paraffin-embedded enucleation specimens from 25 patients with UM and a mean follow-up of 14 years were analyzed for whole-genome copy-number alterations using OncoScan analysis. Copy-number alterations of chromosomes 1, 3, 6, and 8 were also analyzed in these tumors using multiplex ligation-dependent probe-amplification, and mutations in GNAQ, GNA11, and BAP1 were searched for by Sanger sequencing. Our study confirms the previously reported GNAQ and GNA11 mutation frequencies in UMs as well as the presence of monosomy 3 as a factor strongly indicating poor prognosis. Two cases with metastatic disease, but without monosomy of chromosome 3, showed loss of a small region in the distal part of chromosome 2p. Also, UMs leading to metastatic disease had more chromosomal aberrations than those without metastases. Three UMs lacking a GNAQ or a GNA11 mutation showed a gain of chromosome 8q; one of these cases showed extensive chromothripsis. Another case (with suspect lung metastasis) showed focal chromothripsis. Our whole-genome copy-number analysis shows that focal loss of chromosome 2p may be involved in the metastatic spread of UMs without monosomy 3; metastatic UMs carry more chromosomal aberrations than those without metastases; and chromothripsis may play a role in the oncogenesis of UMs, but does not necessarily indicate a poor prognosis. The clinical and particularly diagnostic utility of these findings needs to be corroborated in a larger set of patients with UM.

Published

2015

49. Mutations in g protein encoding genes and chromosomal alterations in primary leptomeningeal melanocytic neoplasms

Author

Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., Groenen, P.J.T.A., Kusters-vandevelde, H.V., Engen-van Grunsven, A.C.H. van, Coupland, S.E., Lake, S.L., Rijntjes, J., Pfundt, R.P., Kusters, B., Wesseling, P., Blokx, W.A.M., and Groenen, P.J.T.A.

Abstract

Contains fulltext : 153459.pdf (publisher's version ) (Closed access), Limited data is available on the genetic features of primary leptomeningeal melanocytic neoplasms (LMNs). Similarities with uveal melanoma were recently suggested as both entities harbor oncogenic mutations in GNAQ and GNA11. Whether primary LMNs share additional genetic alterations with uveal melanoma including copy number variations is unknown. Twenty primary LMNs ranging from benign and intermediate-grade melanocytomas to melanomas were tested by direct sequencing for hotspot mutations in the genes GNA11, GNAQ, BRAF, NRAS and HRAS. Furthermore, the lesions were tested for copy number variations of chromosomes frequently present in uveal melanoma (1p, 3, 6 and 8q) by multiplex ligation-dependent probe amplification (MLPA). Genome-wide analyses of copy number alterations of two leptomeningeal melanocytic neoplasms were performed using the OncoScan SNP-array. GNAQ(Q209) mutations were present in eleven LMNs, while two of 20 cases carried a GNA11(Q209) mutation. No BRAF, HRAS or NRAS hotspot mutations were detected. Monosomy 3 and gain of 8q were present in one leptomeningeal melanoma, and one intermediate-grade melanocytoma harbored a gain of chromosome 6. With MLPA, the melanocytomas did not show any further gross chromosomal variations. Our data shows that primary LMNs, like uveal melanoma, harbor oncogenic mutations in GNAQ and GNA11 but lack mutations in BRAF, NRAS and HRAS. This finding may help in the differential diagnosis between a primary LMN and a metastasis from a cutaneous melanoma to the central nervous system. Copy number variations in some aggressive LMNs resemble those present in uveal melanoma but their prognostic significance is unclear.

Published

2015

50. Constitutive activation of the ERK pathway in melanoma and skin melanocytes in Grey horses

Author

Jiang, Lin, Campagne, Cécile, Sundström, Elisabeth, Sousa, Pedro, Imran, Saima, Seltenhammer, Monika, Pielberg, Gerli, Olsson, Mats J, Egidy, Giorgia, Andersson, Leif, Golovko, Anna, Jiang, Lin, Campagne, Cécile, Sundström, Elisabeth, Sousa, Pedro, Imran, Saima, Seltenhammer, Monika, Pielberg, Gerli, Olsson, Mats J, Egidy, Giorgia, Andersson, Leif, and Golovko, Anna

Abstract

BACKGROUND: Constitutive activation of the ERK pathway, occurring in the vast majority of melanocytic neoplasms, has a pivotal role in melanoma development. Different mechanisms underlie this activation in different tumour settings. The Grey phenotype in horses, caused by a 4.6 kb duplication in intron 6 of Syntaxin 17 (STX17), is associated with a very high incidence of cutaneous melanoma, but the molecular mechanism behind the melanomagenesis remains unknown. Here, we investigated the involvement of the ERK pathway in melanoma development in Grey horses. METHODS: Grey horse melanoma tumours, cell lines and normal skin melanocytes were analyzed with help of indirect immunofluorescence and immunoblotting for the expression of phospho-ERK1/2 in comparison to that in non-grey horse and human counterparts. The mutational status of BRAF, RAS, GNAQ, GNA11 and KIT genes in Grey horse melanomas was determined by direct sequencing. The effect of RAS, RAF and PI3K/AKT pathways on the activation of the ERK signaling in Grey horse melanoma cells was investigated with help of specific inhibitors and immunoblotting. Individual roles of RAF and RAS kinases on the ERK activation were examined using si-RNA based approach and immunoblotting. RESULTS: We found that the ERK pathway is constitutively activated in Grey horse melanoma tumours and cell lines in the absence of somatic activating mutations in BRAF, RAS, GNAQ, GNA11 and KIT genes or alterations in the expression of the main components of the pathway. The pathway is mitogenic and is mediated by BRAF, CRAF and KRAS kinases. Importantly, we found high activation of the ERK pathway also in epidermal melanocytes, suggesting a general predisposition to melanomagenesis in these horses. CONCLUSIONS: These findings demonstrate that the presence of the intronic 4.6 kb duplication in STX17 is strongly associated with constitutive activation of the ERK pathway in melanocytic cells in Grey horses in the absence of somatic mutations commo, De två första författarna delar förstaförfattarskapet.

Published

2014