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Investigator

Massimo Cristofanilli

Professor of Medicine · Weill Cornell Medicine, Medicine-Hematology-Oncology

Papers

Genomic Landscape of Advanced Solid Tumors in Circulating Tumor DNA and Correlation With Tissue Sequencing: A Single Institution's Experience

PURPOSECirculating tumor DNA (ctDNA) has emerged as a promising noninvasive biomarker for baseline characterization and longitudinal monitoring of a tumor throughout disease management. The aim of this study was to evaluate the utility of ctDNA across a wide spectrum of tumor types.METHODSWe retrospectively identified 1,763 patients with advanced cancers who had next-generation sequencing of ctDNA or tumor tissue completed by a designated commercial assay at Northwestern University.RESULTSctDNA identified at least one gene alteration in 90% of patients. The number of detected alterations (NDA) and mutant allele frequency (MAF) of the most frequently mutated genes varied significantly across tumor types, with the highest MAF observed in gastric, colorectal, and breast cancers and the highest NDA observed in colorectal, lung squamous, and ovarian/endometrial cancers. TP53 was the most mutated gene in all tumor types. PIK3CA, ERBB2, BRCA1, and FGFR1 alterations were associated with breast cancer, and ESR1 mutations were exclusively detected in this tumor type. Colorectal cancer was characterized by alterations in KRAS and APC mutations, whereas KRAS, EGFR, PIK3CA, and BRAF mutations were common in lung adenocarcinoma. Concordance between blood and tissue sequencing was notably observed for truncal gene alterations (eg, APC and KRAS), whereas low concordance was often observed in genes associated with treatment resistance mechanisms (eg, RB1 and NF1). Tumor mutational burden (TMB) varied significantly across tumor types, and patients with high MAF or NDA had a significantly higher TMB score with one of the investigated platforms.CONCLUSIONThe study provided new insights into the ctDNA mutational landscape across solid tumors, suggesting new hypotheses-generating data and caveats for future histotype-agnostic workflows integrated with tissue-based biomarkers such as TMB.

531Works

1Papers

Breast NeoplasmsBiomarkers, TumorNeoplasm MetastasisCirculating Tumor DNAPrognosisCell Line, TumorTriple Negative Breast NeoplasmsCarcinoma, Lobular

Positions

2022–

Professor of Medicine

Weill Cornell Medicine · Medicine-Hematology-Oncology

2015–

Professor of Medicine

Northwestern University Feinberg School of Medicine · Medicine-Hematology & Oncology

2013–

Professor of Medical Oncology

Thomas Jefferson University · Medical Oncology

2010–

Professor and Chairman

Fox Chase Cancer Center · Medical Oncology

1998–

Associate Professor of Medicine

University of Texas MD Anderson Cancer Center · Breast Medical Oncology

Education

1998

Fellowship- Medical Oncology

University of Texas MD Anderson Cancer Center · Cancer Medicine

1996

Residency

Cabrini Medical Center · Medicine

1986

Università degli Studi di Roma La Sapienza · Medicine and Surgery

Links & IDs

0000-0002-4194-7175