Cytogenetic prognostication within medulloblastoma subgroups

David J. H. Shih; Paul A. Northcott; Marc Remke; Andrey Korshunov; Vijay Ramaswamy; Marcel Kool; Betty Luu; Yuan Yao; Xin Wang; Adrian M. Dubuc; Livia Garzia; John Peacock; Stephen C. Mack; Xiaochong Wu; Adi Rolider; A. Sorana Morrissy; Florence M. G. Cavalli; David T. W. Jones; Karel Zitterbart; Claudia C. Faria; Ulrich Schüller; Leos Kren; Toshihiro Kumabe; Teiji Tominaga; Young Shin Ra; Miklós Garami; Peter Hauser; Jennifer A. Chan; Shenandoah Robinson; László Bognár; Almos Klekner; Ali G. Saad; Linda M. Liau; Steffen Albrecht; Adam Fontebasso; Giuseppe Cinalli; Pasqualino De Antonellis; Massimo Zollo; Michael K. Cooper; Reid C. Thompson; Simon Bailey; Janet C. Lindsey; Concezio Di Rocco; Luca Massimi; Erna M. C. Michiels; Stephen W. Scherer; Joanna J. Phillips; Nalin Gupta; Xing Fan; Karin M. Muraszko; Rajeev Vibhakar; Charles G. Eberhart; Maryam Fouladi; Boleslaw Lach; Shin Jung; Robert J. Wechsler-Reya; Michelle Fèvre-Montange; Anne Jouvet; Nada Jabado; Ian F. Pollack; William A. Weiss; Ji-Yeoun Lee; Byung-Kyu Cho; Seung-Ki Kim; Kyu-Chang Wang; Jeffrey R. Leonard; Joshua B. Rubin; Carmen De Torres; Cinzia Lavarino; Jaume Mora; Yoon-Jae Cho; Uri Tabori; James M. Olson; Amar Gajjar; Roger J. Packer; Stefan Rutkowski; Scott L. Pomeroy; Pim J. French; Nanne K. Kloosterhof; Johan M. Kros; Erwin G. Van Meir; Steven C. Clifford; Franck Bourdeaut; Olivier Delattre; François F. Doz; Cynthia E. Hawkins; David Malkin; Wieslawa A. Grajkowska; Marta Perek-Polnik; Eric Bouffet; James T. Rutka; Stefan M. Pfister; Michael D. Taylor

doi:10.1200/JCO.2013.50.9539

Cytogenetic prognostication within medulloblastoma subgroups

David J. H. Shih, Paul A. Northcott, Marc Remke, Andrey Korshunov, Vijay Ramaswamy, Marcel Kool, Betty Luu, Yuan Yao, Xin Wang, Adrian M. Dubuc, Livia Garzia, John Peacock, Stephen C. Mack, Xiaochong Wu, Adi Rolider, A. Sorana Morrissy, Florence M. G. Cavalli, David T. W. Jones, Karel Zitterbart, Claudia C. FariaUlrich Schüller, Leos Kren, Toshihiro Kumabe, Teiji Tominaga, Young Shin Ra, Miklós Garami, Peter Hauser, Jennifer A. Chan, Shenandoah Robinson, László Bognár, Almos Klekner, Ali G. Saad, Linda M. Liau, Steffen Albrecht, Adam Fontebasso, Giuseppe Cinalli, Pasqualino De Antonellis, Massimo Zollo, Michael K. Cooper, Reid C. Thompson, Simon Bailey, Janet C. Lindsey, Concezio Di Rocco, Luca Massimi, Erna M. C. Michiels, Stephen W. Scherer, Joanna J. Phillips, Nalin Gupta, Xing Fan, Karin M. Muraszko, Rajeev Vibhakar, Charles G. Eberhart, Maryam Fouladi, Boleslaw Lach, Shin Jung, Robert J. Wechsler-Reya, Michelle Fèvre-Montange, Anne Jouvet, Nada Jabado, Ian F. Pollack, William A. Weiss, Ji-Yeoun Lee, Byung-Kyu Cho, Seung-Ki Kim, Kyu-Chang Wang, Jeffrey R. Leonard, Joshua B. Rubin, Carmen De Torres, Cinzia Lavarino, Jaume Mora, Yoon-Jae Cho, Uri Tabori, James M. Olson, Amar Gajjar, Roger J. Packer, Stefan Rutkowski, Scott L. Pomeroy, Pim J. French, Nanne K. Kloosterhof, Johan M. Kros, Erwin G. Van Meir, Steven C. Clifford, Franck Bourdeaut, Olivier Delattre, François F. Doz, Cynthia E. Hawkins, David Malkin, Wieslawa A. Grajkowska, Marta Perek-Polnik, Eric Bouffet, James T. Rutka, Stefan M. Pfister, Michael D. Taylor

Risultato della ricerca: Contributo in rivista › Articolo in rivista

171 Citazioni (Scopus)

Abstract

Purpose: Medulloblastoma comprises four distinct molecular subgroups: WNT, SHH, Group 3, and Group 4. Current medulloblastoma protocols stratify patients based on clinical features: patient age, metastatic stage, extent of resection, and histologic variant. Stark prognostic and genetic differences among the four subgroups suggest that subgroup-specific molecular biomarkers could improve patient prognostication. Patients and Methods: Molecular biomarkers were identified from a discovery set of 673 medulloblastomas from 43 cities around the world. Combined risk stratification models were designed based on clinical and cytogenetic biomarkers identified by multivariable Cox proportional hazards analyses. Identified biomarkers were tested using fluorescent in situ hybridization (FISH) on a nonoverlapping medulloblastoma tissue microarray (n = 453), with subsequent validation of the risk stratification models. Results: Subgroup information improves the predictive accuracy of a multivariable survival model compared with clinical biomarkers alone. Most previously published cytogenetic biomarkers are only prognostic within a single medulloblastoma subgroup. Profiling six FISH biomarkers (GLI2, MYC, chromosome 11 [chr11], chr14, 17p, and 17q) on formalin-fixed paraffin-embedded tissues, we can reliably and reproducibly identify very low-risk and very high-risk patients within SHH, Group 3, and Group 4 medulloblastomas. Conclusion: Combining subgroup and cytogenetic biomarkers with established clinical biomarkers substantially improves patient prognostication, even in the context of heterogeneous clinical therapies. The prognostic significance of most molecular biomarkers is restricted to a specific subgroup. We have identified a small panel of cytogenetic biomarkers that reliably identifies very high-risk and very low-risk groups of patients, making it an excellent tool for selecting patients for therapy intensification and therapy de-escalation in future clinical trials. © 2014 by American Society of Clinical Oncology.

Lingua originale	English
pagine (da-a)	886-896
Numero di pagine	11
Rivista	Journal of Clinical Oncology
Volume	32
DOI	https://doi.org/10.1200/JCO.2013.50.9539
Stato di pubblicazione	Pubblicato - 2014

Keywords

Adolescent
Biomarkers, Tumor
Cancer Research
Child
Child, Preschool
Chromosomes, Human, Pair 11
Chromosomes, Human, Pair 14
Cytogenetics
Female
Gene Expression Profiling
Gene Expression Regulation, Neoplastic
Hedgehog Proteins
Humans
In Situ Hybridization, Fluorescence
Infant
Kruppel-Like Transcription Factors
Male
Medulloblastoma
Nuclear Proteins
Oncology
Predictive Value of Tests
Prognosis
Proportional Hazards Models
Proto-Oncogene Proteins c-myc
Reproducibility of Results
Risk Assessment
Risk Factors
Tissue Array Analysis
Wnt Proteins
Young Adult
Zinc Finger Protein Gli2

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10.1200/JCO.2013.50.9539

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Shih, D. J. H., Northcott, P. A., Remke, M., Korshunov, A., Ramaswamy, V., Kool, M., Luu, B., Yao, Y., Wang, X., Dubuc, A. M., Garzia, L., Peacock, J., Mack, S. C., Wu, X., Rolider, A., Morrissy, A. S., Cavalli, F. M. G., Jones, D. T. W., Zitterbart, K., ... Taylor, M. D. (2014). Cytogenetic prognostication within medulloblastoma subgroups. Journal of Clinical Oncology, 32, 886-896. https://doi.org/10.1200/JCO.2013.50.9539

@article{0392e7c4b4774df1b1f87da95cf99a40,

title = "Cytogenetic prognostication within medulloblastoma subgroups",

abstract = "Purpose: Medulloblastoma comprises four distinct molecular subgroups: WNT, SHH, Group 3, and Group 4. Current medulloblastoma protocols stratify patients based on clinical features: patient age, metastatic stage, extent of resection, and histologic variant. Stark prognostic and genetic differences among the four subgroups suggest that subgroup-specific molecular biomarkers could improve patient prognostication. Patients and Methods: Molecular biomarkers were identified from a discovery set of 673 medulloblastomas from 43 cities around the world. Combined risk stratification models were designed based on clinical and cytogenetic biomarkers identified by multivariable Cox proportional hazards analyses. Identified biomarkers were tested using fluorescent in situ hybridization (FISH) on a nonoverlapping medulloblastoma tissue microarray (n = 453), with subsequent validation of the risk stratification models. Results: Subgroup information improves the predictive accuracy of a multivariable survival model compared with clinical biomarkers alone. Most previously published cytogenetic biomarkers are only prognostic within a single medulloblastoma subgroup. Profiling six FISH biomarkers (GLI2, MYC, chromosome 11 [chr11], chr14, 17p, and 17q) on formalin-fixed paraffin-embedded tissues, we can reliably and reproducibly identify very low-risk and very high-risk patients within SHH, Group 3, and Group 4 medulloblastomas. Conclusion: Combining subgroup and cytogenetic biomarkers with established clinical biomarkers substantially improves patient prognostication, even in the context of heterogeneous clinical therapies. The prognostic significance of most molecular biomarkers is restricted to a specific subgroup. We have identified a small panel of cytogenetic biomarkers that reliably identifies very high-risk and very low-risk groups of patients, making it an excellent tool for selecting patients for therapy intensification and therapy de-escalation in future clinical trials. {\textcopyright} 2014 by American Society of Clinical Oncology.",

keywords = "Adolescent, Biomarkers, Tumor, Cancer Research, Child, Child, Preschool, Chromosomes, Human, Pair 11, Chromosomes, Human, Pair 14, Cytogenetics, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Hedgehog Proteins, Humans, In Situ Hybridization, Fluorescence, Infant, Kruppel-Like Transcription Factors, Male, Medulloblastoma, Nuclear Proteins, Oncology, Predictive Value of Tests, Prognosis, Proportional Hazards Models, Proto-Oncogene Proteins c-myc, Reproducibility of Results, Risk Assessment, Risk Factors, Tissue Array Analysis, Wnt Proteins, Young Adult, Zinc Finger Protein Gli2, Adolescent, Biomarkers, Tumor, Cancer Research, Child, Child, Preschool, Chromosomes, Human, Pair 11, Chromosomes, Human, Pair 14, Cytogenetics, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic, Hedgehog Proteins, Humans, In Situ Hybridization, Fluorescence, Infant, Kruppel-Like Transcription Factors, Male, Medulloblastoma, Nuclear Proteins, Oncology, Predictive Value of Tests, Prognosis, Proportional Hazards Models, Proto-Oncogene Proteins c-myc, Reproducibility of Results, Risk Assessment, Risk Factors, Tissue Array Analysis, Wnt Proteins, Young Adult, Zinc Finger Protein Gli2",

author = "Shih, {David J. H.} and Northcott, {Paul A.} and Marc Remke and Andrey Korshunov and Vijay Ramaswamy and Marcel Kool and Betty Luu and Yuan Yao and Xin Wang and Dubuc, {Adrian M.} and Livia Garzia and John Peacock and Mack, {Stephen C.} and Xiaochong Wu and Adi Rolider and Morrissy, {A. Sorana} and Cavalli, {Florence M. G.} and Jones, {David T. W.} and Karel Zitterbart and Faria, {Claudia C.} and Ulrich Sch{\"u}ller and Leos Kren and Toshihiro Kumabe and Teiji Tominaga and Ra, {Young Shin} and Mikl{\'o}s Garami and Peter Hauser and Chan, {Jennifer A.} and Shenandoah Robinson and L{\'a}szl{\'o} Bogn{\'a}r and Almos Klekner and Saad, {Ali G.} and Liau, {Linda M.} and Steffen Albrecht and Adam Fontebasso and Giuseppe Cinalli and {De Antonellis}, Pasqualino and Massimo Zollo and Cooper, {Michael K.} and Thompson, {Reid C.} and Simon Bailey and Lindsey, {Janet C.} and {Di Rocco}, Concezio and Luca Massimi and Michiels, {Erna M. C.} and Scherer, {Stephen W.} and Phillips, {Joanna J.} and Nalin Gupta and Xing Fan and Muraszko, {Karin M.} and Rajeev Vibhakar and Eberhart, {Charles G.} and Maryam Fouladi and Boleslaw Lach and Shin Jung and Wechsler-Reya, {Robert J.} and Michelle F{\`e}vre-Montange and Anne Jouvet and Nada Jabado and Pollack, {Ian F.} and Weiss, {William A.} and Ji-Yeoun Lee and Byung-Kyu Cho and Seung-Ki Kim and Kyu-Chang Wang and Leonard, {Jeffrey R.} and Rubin, {Joshua B.} and {De Torres}, Carmen and Cinzia Lavarino and Jaume Mora and Yoon-Jae Cho and Uri Tabori and Olson, {James M.} and Amar Gajjar and Packer, {Roger J.} and Stefan Rutkowski and Pomeroy, {Scott L.} and French, {Pim J.} and Kloosterhof, {Nanne K.} and Kros, {Johan M.} and {Van Meir}, {Erwin G.} and Clifford, {Steven C.} and Franck Bourdeaut and Olivier Delattre and Doz, {Fran{\c c}ois F.} and Hawkins, {Cynthia E.} and David Malkin and Grajkowska, {Wieslawa A.} and Marta Perek-Polnik and Eric Bouffet and Rutka, {James T.} and Pfister, {Stefan M.} and Taylor, {Michael D.}",

year = "2014",

doi = "10.1200/JCO.2013.50.9539",

language = "English",

volume = "32",

pages = "886--896",

journal = "Journal of Clinical Oncology",

issn = "0732-183X",

publisher = "Lippincott Williams and Wilkins",

}

Shih, DJH, Northcott, PA, Remke, M, Korshunov, A, Ramaswamy, V, Kool, M, Luu, B, Yao, Y, Wang, X, Dubuc, AM, Garzia, L, Peacock, J, Mack, SC, Wu, X, Rolider, A, Morrissy, AS, Cavalli, FMG, Jones, DTW, Zitterbart, K, Faria, CC, Schüller, U, Kren, L, Kumabe, T, Tominaga, T, Ra, YS, Garami, M, Hauser, P, Chan, JA, Robinson, S, Bognár, L, Klekner, A, Saad, AG, Liau, LM, Albrecht, S, Fontebasso, A, Cinalli, G, De Antonellis, P, Zollo, M, Cooper, MK, Thompson, RC, Bailey, S, Lindsey, JC, Di Rocco, C, Massimi, L, Michiels, EMC, Scherer, SW, Phillips, JJ, Gupta, N, Fan, X, Muraszko, KM, Vibhakar, R, Eberhart, CG, Fouladi, M, Lach, B, Jung, S, Wechsler-Reya, RJ, Fèvre-Montange, M, Jouvet, A, Jabado, N, Pollack, IF, Weiss, WA, Lee, J-Y, Cho, B-K, Kim, S-K, Wang, K-C, Leonard, JR, Rubin, JB, De Torres, C, Lavarino, C, Mora, J, Cho, Y-J, Tabori, U, Olson, JM, Gajjar, A, Packer, RJ, Rutkowski, S, Pomeroy, SL, French, PJ, Kloosterhof, NK, Kros, JM, Van Meir, EG, Clifford, SC, Bourdeaut, F, Delattre, O, Doz, FF, Hawkins, CE, Malkin, D, Grajkowska, WA, Perek-Polnik, M, Bouffet, E, Rutka, JT, Pfister, SM & Taylor, MD 2014, 'Cytogenetic prognostication within medulloblastoma subgroups', Journal of Clinical Oncology, vol. 32, pagg. 886-896. https://doi.org/10.1200/JCO.2013.50.9539

TY - JOUR

T1 - Cytogenetic prognostication within medulloblastoma subgroups

AU - Shih, David J. H.

AU - Northcott, Paul A.

AU - Remke, Marc

AU - Korshunov, Andrey

AU - Ramaswamy, Vijay

AU - Kool, Marcel

AU - Luu, Betty

AU - Yao, Yuan

AU - Wang, Xin

AU - Dubuc, Adrian M.

AU - Garzia, Livia

AU - Peacock, John

AU - Mack, Stephen C.

AU - Wu, Xiaochong

AU - Rolider, Adi

AU - Morrissy, A. Sorana

AU - Cavalli, Florence M. G.

AU - Jones, David T. W.

AU - Zitterbart, Karel

AU - Faria, Claudia C.

AU - Schüller, Ulrich

AU - Kren, Leos

AU - Kumabe, Toshihiro

AU - Tominaga, Teiji

AU - Ra, Young Shin

AU - Garami, Miklós

AU - Hauser, Peter

AU - Chan, Jennifer A.

AU - Robinson, Shenandoah

AU - Bognár, László

AU - Klekner, Almos

AU - Saad, Ali G.

AU - Liau, Linda M.

AU - Albrecht, Steffen

AU - Fontebasso, Adam

AU - Cinalli, Giuseppe

AU - De Antonellis, Pasqualino

AU - Zollo, Massimo

AU - Cooper, Michael K.

AU - Thompson, Reid C.

AU - Bailey, Simon

AU - Lindsey, Janet C.

AU - Di Rocco, Concezio

AU - Massimi, Luca

AU - Michiels, Erna M. C.

AU - Scherer, Stephen W.

AU - Phillips, Joanna J.

AU - Gupta, Nalin

AU - Fan, Xing

AU - Muraszko, Karin M.

AU - Vibhakar, Rajeev

AU - Eberhart, Charles G.

AU - Fouladi, Maryam

AU - Lach, Boleslaw

AU - Jung, Shin

AU - Wechsler-Reya, Robert J.

AU - Fèvre-Montange, Michelle

AU - Jouvet, Anne

AU - Jabado, Nada

AU - Pollack, Ian F.

AU - Weiss, William A.

AU - Lee, Ji-Yeoun

AU - Cho, Byung-Kyu

AU - Kim, Seung-Ki

AU - Wang, Kyu-Chang

AU - Leonard, Jeffrey R.

AU - Rubin, Joshua B.

AU - De Torres, Carmen

AU - Lavarino, Cinzia

AU - Mora, Jaume

AU - Cho, Yoon-Jae

AU - Tabori, Uri

AU - Olson, James M.

AU - Gajjar, Amar

AU - Packer, Roger J.

AU - Rutkowski, Stefan

AU - Pomeroy, Scott L.

AU - French, Pim J.

AU - Kloosterhof, Nanne K.

AU - Kros, Johan M.

AU - Van Meir, Erwin G.

AU - Clifford, Steven C.

AU - Bourdeaut, Franck

AU - Delattre, Olivier

AU - Doz, François F.

AU - Hawkins, Cynthia E.

AU - Malkin, David

AU - Grajkowska, Wieslawa A.

AU - Perek-Polnik, Marta

AU - Bouffet, Eric

AU - Rutka, James T.

AU - Pfister, Stefan M.

AU - Taylor, Michael D.

PY - 2014

Y1 - 2014

N2 - Purpose: Medulloblastoma comprises four distinct molecular subgroups: WNT, SHH, Group 3, and Group 4. Current medulloblastoma protocols stratify patients based on clinical features: patient age, metastatic stage, extent of resection, and histologic variant. Stark prognostic and genetic differences among the four subgroups suggest that subgroup-specific molecular biomarkers could improve patient prognostication. Patients and Methods: Molecular biomarkers were identified from a discovery set of 673 medulloblastomas from 43 cities around the world. Combined risk stratification models were designed based on clinical and cytogenetic biomarkers identified by multivariable Cox proportional hazards analyses. Identified biomarkers were tested using fluorescent in situ hybridization (FISH) on a nonoverlapping medulloblastoma tissue microarray (n = 453), with subsequent validation of the risk stratification models. Results: Subgroup information improves the predictive accuracy of a multivariable survival model compared with clinical biomarkers alone. Most previously published cytogenetic biomarkers are only prognostic within a single medulloblastoma subgroup. Profiling six FISH biomarkers (GLI2, MYC, chromosome 11 [chr11], chr14, 17p, and 17q) on formalin-fixed paraffin-embedded tissues, we can reliably and reproducibly identify very low-risk and very high-risk patients within SHH, Group 3, and Group 4 medulloblastomas. Conclusion: Combining subgroup and cytogenetic biomarkers with established clinical biomarkers substantially improves patient prognostication, even in the context of heterogeneous clinical therapies. The prognostic significance of most molecular biomarkers is restricted to a specific subgroup. We have identified a small panel of cytogenetic biomarkers that reliably identifies very high-risk and very low-risk groups of patients, making it an excellent tool for selecting patients for therapy intensification and therapy de-escalation in future clinical trials. © 2014 by American Society of Clinical Oncology.

AB - Purpose: Medulloblastoma comprises four distinct molecular subgroups: WNT, SHH, Group 3, and Group 4. Current medulloblastoma protocols stratify patients based on clinical features: patient age, metastatic stage, extent of resection, and histologic variant. Stark prognostic and genetic differences among the four subgroups suggest that subgroup-specific molecular biomarkers could improve patient prognostication. Patients and Methods: Molecular biomarkers were identified from a discovery set of 673 medulloblastomas from 43 cities around the world. Combined risk stratification models were designed based on clinical and cytogenetic biomarkers identified by multivariable Cox proportional hazards analyses. Identified biomarkers were tested using fluorescent in situ hybridization (FISH) on a nonoverlapping medulloblastoma tissue microarray (n = 453), with subsequent validation of the risk stratification models. Results: Subgroup information improves the predictive accuracy of a multivariable survival model compared with clinical biomarkers alone. Most previously published cytogenetic biomarkers are only prognostic within a single medulloblastoma subgroup. Profiling six FISH biomarkers (GLI2, MYC, chromosome 11 [chr11], chr14, 17p, and 17q) on formalin-fixed paraffin-embedded tissues, we can reliably and reproducibly identify very low-risk and very high-risk patients within SHH, Group 3, and Group 4 medulloblastomas. Conclusion: Combining subgroup and cytogenetic biomarkers with established clinical biomarkers substantially improves patient prognostication, even in the context of heterogeneous clinical therapies. The prognostic significance of most molecular biomarkers is restricted to a specific subgroup. We have identified a small panel of cytogenetic biomarkers that reliably identifies very high-risk and very low-risk groups of patients, making it an excellent tool for selecting patients for therapy intensification and therapy de-escalation in future clinical trials. © 2014 by American Society of Clinical Oncology.

KW - Adolescent

KW - Biomarkers, Tumor

KW - Cancer Research

KW - Child

KW - Child, Preschool

KW - Chromosomes, Human, Pair 11

KW - Chromosomes, Human, Pair 14

KW - Cytogenetics

KW - Female

KW - Gene Expression Profiling

KW - Gene Expression Regulation, Neoplastic

KW - Hedgehog Proteins

KW - Humans

KW - In Situ Hybridization, Fluorescence

KW - Infant

KW - Kruppel-Like Transcription Factors

KW - Male

KW - Medulloblastoma

KW - Nuclear Proteins

KW - Oncology

KW - Predictive Value of Tests

KW - Prognosis

KW - Proportional Hazards Models

KW - Proto-Oncogene Proteins c-myc

KW - Reproducibility of Results

KW - Risk Assessment

KW - Risk Factors

KW - Tissue Array Analysis

KW - Wnt Proteins

KW - Young Adult

KW - Zinc Finger Protein Gli2

KW - Adolescent

KW - Biomarkers, Tumor

KW - Cancer Research

KW - Child

KW - Child, Preschool

KW - Chromosomes, Human, Pair 11

KW - Chromosomes, Human, Pair 14

KW - Cytogenetics

KW - Female

KW - Gene Expression Profiling

KW - Gene Expression Regulation, Neoplastic

KW - Hedgehog Proteins

KW - Humans

KW - In Situ Hybridization, Fluorescence

KW - Infant

KW - Kruppel-Like Transcription Factors

KW - Male

KW - Medulloblastoma

KW - Nuclear Proteins

KW - Oncology

KW - Predictive Value of Tests

KW - Prognosis

KW - Proportional Hazards Models

KW - Proto-Oncogene Proteins c-myc

KW - Reproducibility of Results

KW - Risk Assessment

KW - Risk Factors

KW - Tissue Array Analysis

KW - Wnt Proteins

KW - Young Adult

KW - Zinc Finger Protein Gli2

UR - http://hdl.handle.net/10807/124702

UR - http://jco.ascopubs.org/content/32/9/886.full.pdf+html

U2 - 10.1200/JCO.2013.50.9539

DO - 10.1200/JCO.2013.50.9539

M3 - Article

SN - 0732-183X

VL - 32

SP - 886

EP - 896

JO - Journal of Clinical Oncology

JF - Journal of Clinical Oncology

ER -

Cytogenetic prognostication within medulloblastoma subgroups

Abstract

Keywords

OSS delle Nazioni Unite

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