Familial melanoma-astrocytoma syndrome is a tumor predisposition syndrome caused by inactivating germline alteration of the <italic>CDKN2A</italic> tumor suppressor gene on chromosome 9p21. While some families with germline <italic>CDKN2A</italic> mutations are prone to development of just melanomas, other families develop both melanomas, astrocytomas, and occasionally other nervous-system neoplasms including peripheral nerve sheath tumors and meningiomas. The histologic spectrum of the astrocytomas that arise as part of this syndrome is not well described, nor are the additional genetic alterations that drive these astrocytomas apart from the germline <italic>CDKN2A</italic> inactivation. Herein, we report the case of a young man with synchronous development of a pleomorphic xanthoastrocytoma, diffuse astrocytoma, and paraspinal mass radiographically consistent with a peripheral nerve sheath tumor. His paternal family history is significant for melanoma, glioblastoma, and oral squamous cell carcinoma. Genomic profiling revealed that he harbors a heterozygous deletion in the germline of chromosome 9p21.3 encompassing the <italic>CDKN2A</italic> and <italic>CDKN2B</italic> tumor suppressor genes. Both the pleomorphic xanthoastrocytoma and diffuse astrocytoma were found to have homozygous deletion of <italic>CDKN2A/B</italic> due to somatic loss of the other copy of chromosome 9p containing the remaining intact alleles. Additional somatic alterations included <italic>BRAF</italic> p.V600E mutation in the pleomorphic xanthoastrocytoma and <italic>PTPN11</italic>, <italic>ATRX</italic>, and <italic>NF1</italic> mutations in the diffuse astrocytoma. The presence of germline <italic>CDKN2A/B</italic> inactivation together with the presence of multiple anatomically, histologically, and genetically distinct astrocytic neoplasms, both with accompanying somatic loss of heterozygosity for the <italic>CDKN2A/B</italic> deletion, led to a diagnosis of familial melanoma-astrocytoma syndrome. This remarkable case illustrates the histologic and genetic diversity that astrocytomas arising as part of this rare glioma predisposition syndrome can demonstrate. .
Familial melanoma-astrocytoma syndrome is a tumor predisposition syndrome caused by inactivating germline alteration of the <italic>CDKN2A</italic> tumor suppressor gene on chromosome 9p21. While some families with germline <italic>CDKN2A</italic> mutations are prone to development of just melanomas, other families develop both melanomas, astrocytomas, and occasionally other nervous-system neoplasms including peripheral nerve sheath tumors and meningiomas. The histologic spectrum of the astrocytomas that arise as part of this syndrome is not well described, nor are the additional genetic alterations that drive these astrocytomas apart from the germline <italic>CDKN2A</italic> inactivation. Herein, we report the case of a young man with synchronous development of a pleomorphic xanthoastrocytoma, diffuse astrocytoma, and paraspinal mass radiographically consistent with a peripheral nerve sheath tumor. His paternal family history is significant for melanoma, glioblastoma, and oral squamous cell carcinoma. Genomic profiling revealed that he harbors a heterozygous deletion in the germline of chromosome 9p21.3 encompassing the <italic>CDKN2A</italic> and <italic>CDKN2B</italic> tumor suppressor genes. Both the pleomorphic xanthoastrocytoma and diffuse astrocytoma were found to have homozygous deletion of <italic>CDKN2A/B</italic> due to somatic loss of the other copy of chromosome 9p containing the remaining intact alleles. Additional somatic alterations included <italic>BRAF</italic> p.V600E mutation in the pleomorphic xanthoastrocytoma and <italic>PTPN11</italic>, <italic>ATRX</italic>, and <italic>NF1</italic> mutations in the diffuse astrocytoma. The presence of germline <italic>CDKN2A/B</italic> inactivation together with the presence of multiple anatomically, histologically, and genetically distinct astrocytic neoplasms, both with accompanying somatic loss of heterozygosity for the <italic>CDKN2A/B</italic> deletion, led to a diagnosis of familial melanoma-astrocytoma syndrome. This remarkable case illustrates the histologic and genetic diversity that astrocytomas arising as part of this rare glioma predisposition syndrome can demonstrate. .
Family history of brain tumors is an important risk factor in a small fraction of patients with primary glial neoplasms of the central nervous system [1, 2]. Among these patients, a subset harbor pathogenic germline alterations as part of well-characterized tumor predisposition syndromes [3]. These include germline mutations or deletions affecting the NF1tumor suppressor gene as part of neurofibromatosis type 1 syndrome, TP53tumor suppressor gene as part of Li-Fraumeni syndrome, and mismatch repair genes (e.g. MLH1, MSH2, MSH6, PMS2) as part of Lynch/Turcot syndrome. Multiple additional glioma susceptibility genes have been more recently identified. These include POT1, which encodes a protein involved in telomere maintenance, in which inactivating germline mutations have been identified in families with multiple members affected by oligodendroglioma [4]. Consortiums, such as GLIOGENE, are currently performing genome-wide association studies on large numbers of patients with primary glial neoplasms in order to determine the complete spectrum of genetic variants that increase risk of glioma development [5].In addition to the aforementioned genetic syndromes, familial melanoma-astrocytoma syndrome has emerged as a rare cause of inherited glioma predisposition. Kaufman et al. [6] first described in 1993 a family in which cutaneous malignant melanoma or cerebral astrocytoma were seen in eight members over three generations and therefore suggested the presence of a possible new genetic syndrome. A study in 1995 examined the incidence of tumors of the nervous system as second cancers or in family members of 904 patients with cutaneous melanoma, which identified 15 families with cutaneous melanoma in which one or more family members had nervous system tumors including astrocytoma, glioblastoma, meningioma, and “acoustic neurilemmoma” (now referred to as vestibular schwannoma) [7]. Then a third study in 1997 described a family with a cancer syndrome including cutaneous melanoma, dysplastic nevi, astrocytoma, neurofibroma, schwannoma, and meningioma [8]. Together, these epidemiologic studies identified the presence of a distinct tumor predisposition syndrome that includes increased risk for both melanoma and nervous system tumors, predominantly astrocytomas.The genetic basis of this tumor predisposition syndrome was elucidated in 1998 by Bahuau et al. [9] who reported identification of deletions of the INK4 locus at chromosome 9p21.3 in both of the families described in the original 1993 and 1997 reports. The INK4 locus contains, in close proximity, both the CDKN2A and CDKN2Btumor suppressor genes. CDKN2A encodes the p16INK4acyclin-dependent kinase inhibitor and in an alternative reading frame also encodes p14ARF, an inhibitor of p53 signaling, while CDKN2B encodes p15INK4b, a cyclin-dependent kinase inhibitor with a high degree of homology to p16INK4a. CDKN2A had already been recognized as one of the major susceptibility genes for familial cutaneous melanoma, most commonly due to inactivating point mutations but also occasionally gene deletions [10, 11]. Familial melanoma-astrocytoma syndrome is now appreciated to represent an autosomal-dominant variant of the familial melanoma syndrome caused by heterozygous germline CDKN2A inactivation that also includes development of astrocytomas and occasionally other neural tumors including peripheral nerve sheath tumors and meningioma (Online Mendelian Inheritance in Man, entry # 155755).Since the initial reports, a few additional families with genetically-confirmed familial melanoma-astrocytoma syndrome have been described [12, 13, 14, 15, 16, 17]. However, the histologic features of the astrocytomas that arise as part of this syndrome are not well described, nor are the somatic genetic alterations that drive these astrocytomas in addition to the germline CDKN2A inactivation. Herein, we report the case of a young man with a family history of melanoma, glioblastoma, and oral squamous cell carcinoma who was found to have synchronous development of a pleomorphic xanthoastrocytoma, diffuse astrocytoma, and a paraspinal mass radiographically consistent with a peripheral nerve sheath tumor. Pathologic and genomic assessment demonstrated the presence of germline CDKN2A/B deletion diagnostic of familial melanoma-astrocytoma syndrome, and also revealed the diversity of histologic features and genetic alterations that can be seen in astrocytomas arising as part of this rare glioma predisposition syndrome.
Case report
A 23-year-old Caucasian man initially presented with new-onset generalized tonic-clonic seizures. He was found to have a non-enhancing lesion in the left frontal lobe and underwent resection which demonstrated a low-grade astrocytoma. Evaluation of IDH1/2, ATRX, TP53, and BRAF status was not performed, and this specimen is not currently available for our pathologic review and genetic analysis. Dermatologic evaluation did not demonstrate any café-au-lait macules or axillary or inguinal freckling but did reveal scattered melanocytic nevi. Additionally, no Lisch nodules or cutaneous neurofibromas were present. His mother is alive without a personal or significant family history of neoplasia. His father has a history of multifocal high-grade epithelial dysplasia of the oropharynx as well as resection of squamous cell carcinoma from the oral cavity. His sister died of glioblastoma at age 14, and his paternal grandfather had a history of cutaneous melanoma and died of brain cancer. Two paternal uncles are currently alive, one with a history of cutaneous melanoma and the other with a history of oral cancer. A pedigree of the paternal lineage is shown in Figure 1.
Figure 1.
Pedigree of the patient’s family and paternal lineage. The proband is marked with an arrow. SCC = squamous cell carcinoma of the oropharynx; LGG = low-grade glioma (diffuse astrocytoma); PXA = pleomorphic xanthoastrocytoma.
After resection, no additional adjuvant therapy was administered, and he was monitored by regular MR imaging of the brain over the next several years. Aside from suffering from occasional seizures associated with poor compliance to anticonvulsant medications, the patient remained otherwise neurologically intact. A surveillance scan 8 years after his initial surgery, now at 31 years of age, revealed a new area of nodular enhancement with associated hemorrhage adjacent to the prior resection cavity in the left frontal lobe (Figure 2A, B, C). Additionally, a new T2- and fluid-attenuated inversion recovery (FLAIR) hyperintense mass lesion in the right cerebellar hemisphere was seen that did not enhance after contrast administration (Figure 3A, B). The patient underwent a gross total resection of the enhancing nodule in the left frontal lobe. Pathology demonstrated a solid, non-infiltrative astrocytic neoplasm with marked nuclear pleomorphism, occasional xanthomatous tumor cells with foamy cytoplasm, and numerous eosinophilic granular bodies (Figure 2D, E). The mitotic index was low, and high-grade histologic features including necrosis and microvascular proliferation were not identified. An immunostain for type IV collagen revealed abundant intercellular collagen deposition (Figure 2F). Additional immunostains revealed that the tumor cells had intact/retained expression of ATRX protein and were negative for IDH1-R132H mutant protein. Ki67 labeling was seen in ~ 2% of tumor cells. A diagnosis of pleomorphic xanthoastrocytoma (PXA), WHO grade II, was rendered. Given this diagnosis and the potential for PXA to disseminate in the cerebrospinal fluid throughout the neuraxis, the right cerebellar lesion was considered worrisome for disseminated disease versus possibly representing a second primary tumor. To further evaluate the patient, MR imaging of the spinal cord was also performed, which demonstrated an expansile, contrast-enhancing mass within the right C6-7 neural foramen tracking along the C7 nerve root, consistent with a peripheral nerve sheath tumor (Figure 4). A resection of the right cerebellar lesion was performed 1 month following the left frontal craniotomy. Pathology demonstrated a diffuse astrocytoma composed of neoplastic fibrillary astrocytes with elongate and irregular, hyperchromatic nuclei infiltrating through the subcortical white matter and internal granular layer of the cerebellum (Figure 3C). The tumor cells demonstrated absence of ATRX immunostaining with intact staining in entrapped non-neoplastic neurons and endothelial cells, consistent with ATRX loss (Figure 3D). The tumor cells were negative for IDH1-R132H and histone H3-K27M mutant proteins by immunohistochemistry. Ki67 labeling was present in ~ 5% of tumor cells. A diagnosis of diffuse astrocytoma, WHO grade II, was rendered. Given the significant family history and the presence of multiple histologically-distinct brain tumors and a peripheral nerve sheath tumor, genomic testing was recommended.
Figure 2.
Imaging and histologic features of the pleomorphic xanthoastrocytoma resected from the left frontal lobe. A, B, C: Surveillance MR imaging 8 years after initial resection of a low-grade astrocytoma from the left frontal lobe demonstrated interval development of a new 7-mm focus of nodular enhancement adjacent to the prior resection cavity within the left medial orbital gyrus. Coronal T2/FLAIR-weighted image (A), coronal T1-weighted post-gadolinium image (B), and axial T1-weighted post-gadolinium image (C). D, E: Hematoxylin and eosin stained sections showing an astrocytic neoplasm with marked nuclear pleomorphism, numerous eosinophilic granular bodies (arrowheads), and occasional xanthomatous tumor cells with foamy cytoplasm. F: Immunostain for type IV collagen demonstrating abundant intercellular collagen deposition amongst the neoplastic astrocytes. Scale bar, 40 μm.
Figure 3.
Imaging and histologic features of the diffuse astrocytoma resected from the right cerebellum. A, B: T2/FLAIR-weighted MR images demonstrating a hyperintense mass lesion in the right cerebellar hemisphere (coronal, A; sagittal, B). C: Hematoxylin and eosin stained section showing a diffuse glial neoplasm composed of neoplastic fibrillary astrocytes with elongate and irregular, hyperchromatic nuclei infiltrating through the cerebellar subcortical white matter. D: Immunohistochemistry for ATRX protein demonstrating absence of staining in the tumor cells with intact staining in entrapped non-neoplastic neurons and endothelial cells, consistent with somatic ATRX loss. Scale bar, 40 µm.
Figure 4.
MR imaging of the cervical spine demonstrating an intradural, extramedullary mass centered in the right C6-C7 neural foramen and extending along the C7 nerve root (coronal T2-weighted, left; axial T1-weighted post-gadolinium, right).
After informed consent was obtained, targeted next-generation sequencing was performed on genomic DNA isolated from a peripheral blood sample and tumor tissue from the left frontal PXA and right cerebellar diffuse astrocytoma. This sequencing was performed on the UCSF500 Cancer Gene Panel as previously described, which utilizes capture-based next-generation sequencing targeting the coding regions of 479 cancer-associated genes along with select introns from 47 of these genes as well as the promoter region of the TERT gene [18].This analysis identified a focal heterozygous deletion on chromosome 9p21.3 spanning approximate coordinates chr9: g.21,700,000 – 22,800,000 (human genome assembly GRCh38) within the peripheral blood sample (Figure 5). This deletion contains both the CDKN2A and CDKN2Btumor suppressor genes. The left frontal PXA demonstrated homozygous deletion of CDKN2A/B due to loss of the other copy of chromosome 9 containing the remaining intact CDKN2A/B alleles. This was accompanied by the p.V600E somatic hotspot mutation in BRAF (Table 1). Alterations involving IDH1, IDH2, TP53, and ATRX were not identified. The right cerebellar diffuse astrocytoma demonstrated homozygous deletion of CDKN2A/B due to copy-neutral loss of heterozygosity of chromosome 9p. This was accompanied by a hotspot activating missense mutation in PTPN11, two inactivating frameshift mutations in the NF1tumor suppressor gene, and an inactivating frameshift mutation in the ATRXtumor suppressor gene. No alterations involving IDH1, IDH2, or TP53 were identified, nor was the BRAFp.V600E mutation found in the PXA. Apart from the copy number changes involving chromosome 9, no other chromosomal copy number aberrations were seen in either tumor.
Figure 5.
Genomic copy number analysis derived from targeted-capture next-generation sequencing data demonstrating heterozygous deletion on chromosome 9p21.3 containing the CDKN2A and CDKN2B tumor suppressor genes in the patient’s germline with somatic loss of chromosome 9p containing the remaining CDKN2A/B alleles in both astrocytic neoplasms. A: Genome-wide copy number plots of DNA extracted from peripheral blood (top), the left frontal pleomorphic xanthoastrocytoma (middle), and right cerebellar diffuse astrocytoma (bottom) demonstrating the focal deletion on chromosome 9p21, loss of chromosome 9 in the pleomorphic xanthoastrocytoma, and copy-neutral loss of heterozygosity of chromosome 9p in the diffuse astrocytoma, but no additional copy number alterations. B: Copy number plots for chromosome 9p highlighting identical boundaries of the focal 9p21.3 deletion within the peripheral blood and both tumors. The deletion is heterozygous within the peripheral blood and homozygous in both tumors due to somatic loss of the other copy of chromosome 9p.
Table 1.
Somatic alterations identified in the left frontal pleomorphic xanthoastrocytoma and right cerebellar diffuse astrocytoma.
Pleomorphic xanthoastrocytoma, left frontal lobe
Variant
Reference transcript
Classification
CDKN2A/B homozygous deletion
N/A
Pathogenic
BRAF p.V600E
NM_004333
Pathogenic
CDH1 p.V55G
NM_004360
VUS
SPTA1 p.T1953I
NM_003126
VUS
Diffuse astrocytoma, right cerebellum
Variant
Reference transcript
Classification
CDKN2A/B homozygous deletion
N/A
Pathogenic
ATRX p.G1152fs
NM_000489
Pathogenic
NF1 p.L1246fs
NM_001042492
Pathogenic
NF1 p.W1685fs
NM_001042492
Pathogenic
PTPN11 p.T73I
NM_002834
Pathogenic
fs = frameshift; N/A = not applicable; VUS = variant of unknown significance.
The presence of germline CDKN2A/B inactivation together with the presence of multiple anatomically, histologically, and genetically distinct astrocytic neoplasms, both with accompanying somatic loss of the remaining CDKN2A/B alleles, is diagnostic of familial melanoma-astrocytoma syndrome. This genetic diagnosis is further supported by the significant family history of both glioblastoma and melanoma in the paternal lineage, suggesting that this is likely an inherited rather than de novo germline alteration in this patient. The patient and his family have been referred to a medical geneticist with expertise in cancer risk evaluation; however, no genetic evaluation of any family members has yet been performed. Given his newly-identified tumor predisposition syndrome, the patient has initiated the recommended cancer screening, including annual dermatologic, ophthalmologic, and dental examinations to monitor for the development of cutaneous, ocular, and mucosal melanoma. He will continue to undergo regular surveillance imaging of the brain. Additionally, imaging of the chest, abdomen, and pelvis was performed to rule out the presence of visceral malignancy, which was unrevealing except for the presence of the paraspinal peripheral nerve sheath tumor that remains asymptomatic and is being radiographically monitored at present.
Discussion
This is the first report, to our knowledge, to demonstrate multiple distinct histologic subtypes of astrocytoma in a patient with familial melanoma-astrocytoma syndrome. The histologic features of the astrocytomas that arise as part of this syndrome are not well described, and pleomorphic xanthoastrocytoma has not been previously described in association with familial melanoma-astrocytoma syndrome. We document the presence of two anatomically-distinct neoplasms, one with histologic features diagnostic of pleomorphic xanthoastrocytoma and one with histologic features diagnostic of diffuse astrocytoma. The pathologic findings in this patient thus expand the histologic diversity of astrocytic neoplasms that can be seen as part of this syndrome, which can range from pleomorphic xanthoastrocytoma to diffuse or anaplastic astrocytoma to glioblastoma. We are not aware of any reports describing tumors histologically resembling other glial neoplasms, including pilocytic astrocytoma, subependymal giant cell astrocytoma, ganglioglioma, or oligodendroglioma in patients with this syndrome.Additionally, we describe for the first time the cooperating somatic alterations that drive gliomagenesis in those astrocytomas arising as part of familial melanoma-astrocytoma syndrome in addition to germline inactivation of CDKN2A. In the pleomorphic xanthoastrocytoma, we show that the germline CDKN2A/B deletion was accompanied by somatic loss of the remaining CDKN2A/B alleles as well as the activating p.V600E hotspot mutation in BRAF. Together, CDKN2A deletion and BRAFp.V600E are the two characteristic somatic alterations seen in the majority of sporadic pleomorphic xanthoastrocytomas [19]. In the diffuse astrocytoma, we show that the germline CDKN2A/B deletion was accompanied by somatic loss of the remaining CDKN2A/B alleles as well as an activating hotspot mutation in PTPN11 and inactivating frameshift mutations in the ATRX and NF1tumor suppressor genes. ATRX mutations are present in greater than 90% of diffuse lower-grade astrocytomas and are frequently accompanied by TP53 and IDH1 or IDH2 mutations [20]. The diffuse astrocytoma in this patient lacked alterations in TP53, IDH1, and IDH2. Instead, the additional cooperating mutations involved PTPN11 and NF1. Amongst sporadic gliomas, PTPN11 mutations are rare and most commonly found in pilocytic astrocytomas, whereas NF1 mutations are very common in primary glioblastomas but not typically seen in diffuse lower-grade astrocytomas [19, 20, 21]. Somatic CDKN2A deletions are common in both diffuse lower-grade astrocytomas and primary glioblastomas [20, 21]. Thus, while the genetic alterations seen in this patient’s pleomorphic xanthoastrocytoma are typical for this tumor type, the genetic alterations seen in the diffuse astrocytoma are somewhat unusual and make prognostic classification based on the molecular profile challenging [22].Regarding management, optimal treatment strategies for patients with familial melanoma-astrocytoma syndrome are unknown. While specific recommendations regarding disease surveillance have not been established given the rarity of this syndrome, these patients require regular brain imaging to monitor for astrocytoma development; dermatologic and ophthalmologic evaluation to monitor for cutaneous and ocular melanoma development; dental exam to monitor for oropharyngeal dysplasia and mucosal melanoma; and body imaging to monitor for development of visceral malignancies, in particular pancreatic carcinoma. Additionally, genetic counseling for the patient and their families is essential.In summary, we present a rare case of a patient with familial melanoma-astrocytoma syndrome who was found to have synchronous development of two anatomically, histologically, and genetically distinct astrocytomas as well as a presumed peripheral nerve sheath tumor. Our report highlights the histologic spectrum of astrocytic neoplasms that can be seen as part of this syndrome, as well as defining the cooperating genetic alterations that drive these astrocytomas.
Acknowledgment
D.A.S. is supported by the NIH Director’s Early Independence Award (DP5 OD021403).
Conflict of interest
The authors have no conflicts of interest related to this case report to disclose.fs = frameshift; N/A = not applicable; VUS = variant of unknown significance.
Authors: M Bahuau; D Vidaud; M Kujas; A Palangié; B Assouline; M Chaignaud-Lebreton; M Prieur; M Vidaud; J P Harpey; J Lafourcade; B Caille Journal: Ann Genet Date: 1997
Authors: F Petronzelli; D Sollima; G Coppola; M E Martini-Neri; G Neri; M Genuardi Journal: Genes Chromosomes Cancer Date: 2001-08 Impact factor: 5.006
Authors: Cameron W Brennan; Roel G W Verhaak; Aaron McKenna; Benito Campos; Houtan Noushmehr; Sofie R Salama; Siyuan Zheng; Debyani Chakravarty; J Zachary Sanborn; Samuel H Berman; Rameen Beroukhim; Brady Bernard; Chang-Jiun Wu; Giannicola Genovese; Ilya Shmulevich; Jill Barnholtz-Sloan; Lihua Zou; Rahulsimham Vegesna; Sachet A Shukla; Giovanni Ciriello; W K Yung; Wei Zhang; Carrie Sougnez; Tom Mikkelsen; Kenneth Aldape; Darell D Bigner; Erwin G Van Meir; Michael Prados; Andrew Sloan; Keith L Black; Jennifer Eschbacher; Gaetano Finocchiaro; William Friedman; David W Andrews; Abhijit Guha; Mary Iacocca; Brian P O'Neill; Greg Foltz; Jerome Myers; Daniel J Weisenberger; Robert Penny; Raju Kucherlapati; Charles M Perou; D Neil Hayes; Richard Gibbs; Marco Marra; Gordon B Mills; Eric Lander; Paul Spellman; Richard Wilson; Chris Sander; John Weinstein; Matthew Meyerson; Stacey Gabriel; Peter W Laird; David Haussler; Gad Getz; Lynda Chin Journal: Cell Date: 2013-10-10 Impact factor: 41.582
Authors: Daniel J Brat; Roel G W Verhaak; Kenneth D Aldape; W K Alfred Yung; Sofie R Salama; Lee A D Cooper; Esther Rheinbay; C Ryan Miller; Mark Vitucci; Olena Morozova; A Gordon Robertson; Houtan Noushmehr; Peter W Laird; Andrew D Cherniack; Rehan Akbani; Jason T Huse; Giovanni Ciriello; Laila M Poisson; Jill S Barnholtz-Sloan; Mitchel S Berger; Cameron Brennan; Rivka R Colen; Howard Colman; Adam E Flanders; Caterina Giannini; Mia Grifford; Antonio Iavarone; Rajan Jain; Isaac Joseph; Jaegil Kim; Katayoon Kasaian; Tom Mikkelsen; Bradley A Murray; Brian Patrick O'Neill; Lior Pachter; Donald W Parsons; Carrie Sougnez; Erik P Sulman; Scott R Vandenberg; Erwin G Van Meir; Andreas von Deimling; Hailei Zhang; Daniel Crain; Kevin Lau; David Mallery; Scott Morris; Joseph Paulauskis; Robert Penny; Troy Shelton; Mark Sherman; Peggy Yena; Aaron Black; Jay Bowen; Katie Dicostanzo; Julie Gastier-Foster; Kristen M Leraas; Tara M Lichtenberg; Christopher R Pierson; Nilsa C Ramirez; Cynthia Taylor; Stephanie Weaver; Lisa Wise; Erik Zmuda; Tanja Davidsen; John A Demchok; Greg Eley; Martin L Ferguson; Carolyn M Hutter; Kenna R Mills Shaw; Bradley A Ozenberger; Margi Sheth; Heidi J Sofia; Roy Tarnuzzer; Zhining Wang; Liming Yang; Jean Claude Zenklusen; Brenda Ayala; Julien Baboud; Sudha Chudamani; Mark A Jensen; Jia Liu; Todd Pihl; Rohini Raman; Yunhu Wan; Ye Wu; Adrian Ally; J Todd Auman; Miruna Balasundaram; Saianand Balu; Stephen B Baylin; Rameen Beroukhim; Moiz S Bootwalla; Reanne Bowlby; Christopher A Bristow; Denise Brooks; Yaron Butterfield; Rebecca Carlsen; Scott Carter; Lynda Chin; Andy Chu; Eric Chuah; Kristian Cibulskis; Amanda Clarke; Simon G Coetzee; Noreen Dhalla; Tim Fennell; Sheila Fisher; Stacey Gabriel; Gad Getz; Richard Gibbs; Ranabir Guin; Angela Hadjipanayis; D Neil Hayes; Toshinori Hinoue; Katherine Hoadley; Robert A Holt; Alan P Hoyle; Stuart R Jefferys; Steven Jones; Corbin D Jones; Raju Kucherlapati; Phillip H Lai; Eric Lander; Semin Lee; Lee Lichtenstein; Yussanne Ma; Dennis T Maglinte; Harshad S Mahadeshwar; Marco A Marra; Michael Mayo; Shaowu Meng; Matthew L Meyerson; Piotr A Mieczkowski; Richard A Moore; Lisle E Mose; Andrew J Mungall; Angeliki Pantazi; Michael Parfenov; Peter J Park; Joel S Parker; Charles M Perou; Alexei Protopopov; Xiaojia Ren; Jeffrey Roach; Thaís S Sabedot; Jacqueline Schein; Steven E Schumacher; Jonathan G Seidman; Sahil Seth; Hui Shen; Janae V Simons; Payal Sipahimalani; Matthew G Soloway; Xingzhi Song; Huandong Sun; Barbara Tabak; Angela Tam; Donghui Tan; Jiabin Tang; Nina Thiessen; Timothy Triche; David J Van Den Berg; Umadevi Veluvolu; Scot Waring; Daniel J Weisenberger; Matthew D Wilkerson; Tina Wong; Junyuan Wu; Liu Xi; Andrew W Xu; Lixing Yang; Travis I Zack; Jianhua Zhang; B Arman Aksoy; Harindra Arachchi; Chris Benz; Brady Bernard; Daniel Carlin; Juok Cho; Daniel DiCara; Scott Frazer; Gregory N Fuller; JianJiong Gao; Nils Gehlenborg; David Haussler; David I Heiman; Lisa Iype; Anders Jacobsen; Zhenlin Ju; Sol Katzman; Hoon Kim; Theo Knijnenburg; Richard Bailey Kreisberg; Michael S Lawrence; William Lee; Kalle Leinonen; Pei Lin; Shiyun Ling; Wenbin Liu; Yingchun Liu; Yuexin Liu; Yiling Lu; Gordon Mills; Sam Ng; Michael S Noble; Evan Paull; Arvind Rao; Sheila Reynolds; Gordon Saksena; Zack Sanborn; Chris Sander; Nikolaus Schultz; Yasin Senbabaoglu; Ronglai Shen; Ilya Shmulevich; Rileen Sinha; Josh Stuart; S Onur Sumer; Yichao Sun; Natalie Tasman; Barry S Taylor; Doug Voet; Nils Weinhold; John N Weinstein; Da Yang; Kosuke Yoshihara; Siyuan Zheng; Wei Zhang; Lihua Zou; Ty Abel; Sara Sadeghi; Mark L Cohen; Jenny Eschbacher; Eyas M Hattab; Aditya Raghunathan; Matthew J Schniederjan; Dina Aziz; Gene Barnett; Wendi Barrett; Darell D Bigner; Lori Boice; Cathy Brewer; Chiara Calatozzolo; Benito Campos; Carlos Gilberto Carlotti; Timothy A Chan; Lucia Cuppini; Erin Curley; Stefania Cuzzubbo; Karen Devine; Francesco DiMeco; Rebecca Duell; J Bradley Elder; Ashley Fehrenbach; Gaetano Finocchiaro; William Friedman; Jordonna Fulop; Johanna Gardner; Beth Hermes; Christel Herold-Mende; Christine Jungk; Ady Kendler; Norman L Lehman; Eric Lipp; Ouida Liu; Randy Mandt; Mary McGraw; Roger Mclendon; Christopher McPherson; Luciano Neder; Phuong Nguyen; Ardene Noss; Raffaele Nunziata; Quinn T Ostrom; Cheryl Palmer; Alessandro Perin; Bianca Pollo; Alexander Potapov; Olga Potapova; W Kimryn Rathmell; Daniil Rotin; Lisa Scarpace; Cathy Schilero; Kelly Senecal; Kristen Shimmel; Vsevolod Shurkhay; Suzanne Sifri; Rosy Singh; Andrew E Sloan; Kathy Smolenski; Susan M Staugaitis; Ruth Steele; Leigh Thorne; Daniela P C Tirapelli; Andreas Unterberg; Mahitha Vallurupalli; Yun Wang; Ronald Warnick; Felicia Williams; Yingli Wolinsky; Sue Bell; Mara Rosenberg; Chip Stewart; Franklin Huang; Jonna L Grimsby; Amie J Radenbaugh; Jianan Zhang Journal: N Engl J Med Date: 2015-06-10 Impact factor: 91.245
Authors: Maria J Baker; Alisa M Goldstein; Patricia L Gordon; Kimberly S Harbaugh; Heath B Mackley; Michael J Glantz; Joseph J Drabick Journal: J Med Genet Date: 2016-01-21 Impact factor: 6.318
Authors: E Azizi; J Friedman; F Pavlotsky; J Iscovich; A Bornstein; R Shafir; H Trau; H Brenner; D Nass Journal: Cancer Date: 1995-11-01 Impact factor: 6.860
Authors: Wendy Yi-Ying Wu; Gunnar Johansson; Carl Wibom; Thomas Brännström; Annika Malmström; Roger Henriksson; Irina Golovleva; Melissa L Bondy; Ulrika Andersson; Anna M Dahlin; Beatrice Melin Journal: Cancers (Basel) Date: 2019-12-12 Impact factor: 6.639
Authors: Timothy F Tramontana; Mark S Marshall; Amy E Helvie; Morgan R Schmitt; Jennifer Ivanovich; Jacquelyn L Carter; Jamie L Renbarger; Michael J Ferguson Journal: JCO Precis Oncol Date: 2020-04-30
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