Your search keyword '"Van Allen E"' showing total 8 results

1. Successful whole-exome sequencing from a prostate cancer bone metastasis biopsy.

Author

Van Allen, E M, Foye, A, Wagle, N, Kim, W, Carter, S L, McKenna, A, Simko, J P, Garraway, L A, and Febbo, P G

Subjects

*BONE metastasis, *BONE cancer, *CANCER invasiveness, *METASTASIS, *BIOPSY

Abstract

Background:Comprehensive molecular characterization of cancer that has metastasized to bone has proved challenging, which may limit the diagnostic and potential therapeutic opportunities for patients with bone-only metastatic disease.Methods:We describe successful tissue acquisition, DNA extraction, and whole-exome sequencing from a bone metastasis of a patient with metastatic, castration-resistant prostate cancer (PCa).Results:The resulting high-quality tumor sequencing identified plausibly actionable somatic genomic alterations that dysregulate the phosphoinostide 3-kinase pathway, as well as a theoretically actionable germline variant in the BRCA2 gene.Conclusions:We demonstrate the feasibility of diagnostic bone metastases profiling and analysis that will be required for the widespread application of prospective 'precision medicine' to men with advanced PCa. [ABSTRACT FROM AUTHOR]

Published

2014

2. Somatic ERCC2 Mutations Confer Cisplatin Sensitivity in Muscle-Invasive Urothelial Cancer.

Author

Mouw, K., Van Allen, E., O’Connor, K., Wagle, N., Kim, P., Al-Ahmadie, H., Zhu, C., Ostravnaya, I., Iyer, G., Signoretti, S., Reuter, V., Getz, G., Kantoff, P.W., Bochner, B., Choueiri, T.K., Bajorin, D.F., Gabriel, S., D’Andrea, A., Garraway, L., and Rosenberg, J.E.

Subjects

*URINARY organ cancer treatment, *CANCER chemotherapy, *SOMATIC mutation, *CYSTECTOMY, *URINARY organ cancer, *CISPLATIN, *PATIENTS

Published

2014

3. Characterizing diversity in the tumor-immune microenvironment of distinct subclasses of gastroesophageal adenocarcinomas.

Author

Derks, S., de Klerk, L. K., Xu, X., Fleitas, T., Liu, K. X., Liu, Y., Dietlein, F., Margolis, C., Chiaravalli, A. M., Da Silva, A. C., Ogino, S., Akarca, F. G., Freeman, G. J., Rodig, S. J., Hornick, J. L., van Allen, E., Li, B., Liu, S. X., Thorsson, V., and Bass, A. J.

Subjects

*IMMUNE checkpoint inhibitors, *T cells, *BARRETT'S esophagus, *TERTIARY structure, *CELL cycle, *TUMOR microenvironment

Abstract

Background: Gastroesophageal adenocarcinomas (GEAs) are heterogeneous cancers where immune checkpoint inhibitors have robust efficacy in heavily inflamed microsatellite instability (MSI) or Epstein-Barr virus (EBV)-positive subtypes. Immune checkpoint inhibitor responses are markedly lower in diffuse/genome stable (GS) and chromosomal instable (CIN) GEAs. In contrast to EBV and MSI subtypes, the tumor microenvironment of CIN and GS GEAs have not been fully characterized to date, which limits our ability to improve immunotherapeutic strategies. Patients and methods: Here we aimed to identify tumor-immune cell association across GEA subclasses using data from The Cancer Genome Atlas (N = 453 GEAs) and archival GEA resection specimen (N ? 71). The Cancer Genome Atlas RNAseq data were used for computational inferences of immune cell subsets, which were correlated to tumor characteristics within and between subtypes. Archival tissues were used for more spatial immune characterization spanning immunohistochemistry and mRNA expression analyses. Results: Our results confirmed substantial heterogeneity in the tumor microenvironment between distinct subtypes. While MSI-high and EBVþ GEAs harbored most intense T cell infiltrates, the GS group showed enrichment of CD4þ T cells, macrophages and B cells and, in w50% of cases, evidence for tertiary lymphoid structures. In contrast, CIN cancers possessed CD8þ T cells predominantly at the invasive margin while tumor-associated macrophages showed tumor infiltrating capacity. Relatively T cell-rich 'hot' CIN GEAs were often from Western patients, while immunological 'cold' CIN GEAs showed enrichment of MYC and cell cycle pathways, including amplification of CCNE1. Conclusions: These results reveal the diversity of immune phenotypes of GEA. Half of GS gastric cancers have tertiary lymphoid structures and are therefore promising candidates for immunotherapy. The majority of CIN GEAs, however, exhibit T cell exclusion and infiltrating macrophages. Associations of immune-poor CIN GEAs with MYC activity and CCNE1 amplification may enable new studies to determine precise mechanisms of immune evasion, ultimately inspiring new therapeutic modalities. [ABSTRACT FROM AUTHOR]

Published

2020

4. Phase 2 trial of sunitinib and gemcitabine in patients with sarcomatoid and/or poor-risk metastatic renal cell carcinoma. Michaelson MD, McKay RR, Werner L, Atkins MB, Van Allen EM, Olivier KM, Song J, Signoretti S, McDermott DF, Choueiri TK.Cancer. 2015 Oct 1;121(19):3435-43. [Epub 2015 Jun 8]. doi: 10.1002/cncr.29503.

Author

Jay, Raman, McKay, R R, Werner, L, Atkins, M B, Van Allen, E M, Olivier, K M, Song, J, Signoretti, S, McDermott, D F, and Choueiri, T K

Abstract

Background: Sarcomatoid renal cell carcinoma (RCC) is associated with an aggressive biology and a poor prognosis. Poor-risk RCC is defined by clinical prognostic factors and demonstrates similarly aggressive behavior. No standard treatment exists for patients with sarcomatoid RCC, and treatment options for patients with poor-risk disease are of limited benefit. The objective of this study was to investigate the efficacy of antiangiogenic therapy in combination with cytotoxic chemotherapy in clinically aggressive RCC.Methods: This was a phase 2, single-arm trial of sunitinib and gemcitabine in patients with sarcomatoid or poor-risk RCC. The primary end point was the objective response rate (ORR). Secondary end points included the time to progression (TTP), overall survival (OS), safety, and biomarker correlatives.Results: Overall, 39 patients had sarcomatoid RCC, and 33 had poor-risk RCC. The ORR was 26% for patients with sarcomatoid RCC and 24% for patients with poor-risk RCC. The median TTP and OS for patients with sarcomatoid RCC were 5 and 10 months, respectively. For patients with poor-risk disease, the median TTP and OS were 5.5 and 15 months, respectively. Patients whose tumors had>10% sarcomatoid histology had a higher clinical benefit rate (ORR plus stable disease) than those with≤10% sarcomatoid histology (P = 0.04). The most common grade 3 or higher treatment-related adverse events included neutropenia (n = 20), anemia (n = 10), and fatigue (n = 7).Conclusions: These results suggest that antiangiogenic therapy and cytotoxic chemotherapy are an active and well-tolerated combination for patients with aggressive RCC. The combination may be more efficacious than either therapy alone and is currently under further investigation. [ABSTRACT FROM AUTHOR]

Published

2017

5. Preclinical Models of DNA Repair Deficiency in Prostate Cancer.

Author

Fitzpatrick, K., Hwang, J., Cai, M.Y., Liu, D., Kochupurakkal, B., Van Allen, E., DAndrea, A.D., and Mouw, K.

Published

2018

6. Mapping the Functional Landscape of ERCC2 Mutations in Muscle-Invasive Bladder Cancer.

Author

Frazier, Z., Damish, A., Reznichenko, E., Liu, D., Rosenberg, J., Van Allen, E., Lazaro, J.B., D'Andrea, A.D., and Mouw, K.

Subjects

*BLADDER cancer, *GENETIC mutation

Published

2017

7. Genomic Evolution and Acquired Resistance to Pre-Operative Chemoradiation Therapy in Locally Advanced Rectal Cancer.

Author

Kamran, S.C., Lennerz, J.K., Reardon, B., Mullane, S.A., Wo, J.Y., Willers, H., Corcoran, R., Van Allen, E., and Hong, T.S.

Subjects

*RECTAL cancer treatment, *CANCER chemotherapy, *PREOPERATIVE care

Published

2017

8. Genomic Analysis of Chemoradiation Therapy Response in Anal Carcinoma.

Author

Mouw, K., Amin-Mansour, A., Braunstein, L.Z., Pike, J., Damish, A., Hornick, J., D'Andrea, A.D., Van Allen, E., and Mamon, H.J.

Subjects

*ANAL cancer treatment, *CANCER radiotherapy, *CANCER chemotherapy, *BIOMARKERS, *CANCER relapse, *NUCLEOTIDE sequencing

Published

2015