Your search keyword '"Higa, Nikki"' showing total 2 results

1. Liquid Biopsy Profiling with Multiple Tests in Patients with Metastatic Breast Cancer.

Author

Higa, Nikki, Welter, Lisa, Xu, Liya, Kolatkar, Anand, Bramlett, Kelli S., Gjoerup, Ole V., Graf, Ryon, Huang, Richard S.P., Leary, Rebecca J., Lee, Young, Perkins, Jeremy G., Riker, Adam I., Singh, Angad P., Tafra, Lorraine, Tweed, Carol K., Shriver, Craig D., Hicks, James, and Kuhn, Peter

Subjects

*BIOPSY, *METASTATIC breast cancer, *MEDICAL care, *BREAST cancer, *CANCER cells

Abstract

The chief goal of the Blood Profiling Atlas in Cancer (BloodPAC) consortium is to promote collaborative efforts that support the development and implementation of liquid biopsy tests. Here, we report the results of a pilot study conducted by three BloodPAC members that aimed to demonstrate a multisite liquid biopsy testing framework using longitudinal blood specimens from 38 patients with metastatic breast cancer. Three laboratories receiving identical samples from two clinical sites each applied a different targeted sequencing platform to analyze mutations in cell-free DNA (cfDNA). The resulting mutational profiles reflected common breast cancer alterations, including clinically actionable mutations for 40% of hormone- receptor-positive patients. In 12 genes with shared target regions across sequencing panels, perfect inter-assay concordance was also observed for mutations detected above the lowest common assay limit of detection. Whole-genome copy number profiling of cfDNA and circulating tumor cells (CTCs) further revealed marked heterogeneity in copy number alterations and cfDNA tumor fractions across patients. Additionally, comparison of tumor fraction and CTC abundance demonstrated the complementary nature of cfDNA and CTC analyses. Overall, the framework described in this study may serve as a resource for future trials aiming to identify multimodal liquid biopsy biomarkers to guide clinical care. [ABSTRACT FROM AUTHOR]

Published

2024

2. Cell State and Cell Type: Deconvoluting Circulating Tumor Cell Populations in Liquid Biopsies by Multi-Omics.

Author

Welter, Lisa, Zheng, Serena, Setayesh, Sonia Maryam, Morikado, Michael, Agrawal, Arushi, Nevarez, Rafael, Naghdloo, Amin, Pore, Milind, Higa, Nikki, Kolatkar, Anand, Thiele, Jana-Aletta, Sharma, Priyanka, Moore, Halle C. F., Richer, Jennifer K., Elias, Anthony, Pienta, Kenneth J., Zurita, Amado J., Gross, Mitchell E., Shishido, Stephanie N., and Hicks, James

Subjects

ENDOTHELIAL cells, DISEASE progression, CELL culture, FLUOROIMMUNOASSAY, BLOOD collection, EPITHELIAL-mesenchymal transition, MULTIOMICS, GENOMICS, RESEARCH funding, BODY fluid examination, BREAST tumors, PROSTATE tumors, LONGITUDINAL method

Abstract

Simple Summary: In addition to millions of normal red and white blood cells, the blood of cancer patients contains a variety of very rare cell types associated with the tumor. A simple blood draw or 'liquid biopsy' can, thus, provide important information about the state of the disease no matter where it exists in the body. In this paper, we describe a method for imaging all rare cells in a blood draw and the means to define each cell type using a combination of genomic, proteomic, and morphological measurements to distinguish tumor cells from mesenchymal and endothelial cells that are present in the tumor microenvironment. We compare the results of this assay among multiple prostate and breast cancer patients and show that this cellular profiling method is valid across patients and cancer types and may provide important biomarkers for assessing disease in real time. Bi-directional crosstalk between the tumor and the tumor microenvironment (TME) has been shown to increase the rate of tumor evolution and to play a key role in neoplastic progression, therapeutic resistance, and a patient's overall survival. Here, we set out to use a comprehensive liquid-biopsy analysis to study cancer and specific TME cells in circulation and their association with disease status. Cytokeratin+, CD45- circulating rare cells (CRCs) from nine breast and four prostate cancer patients were characterized through morphometrics, single-cell copy number analysis, and targeted multiplexed proteomics to delineate cancer cell lineage from other rare cells originating in the TME. We show that we can detect epithelial circulating tumor cells (EPI.CTC), CTCs undergoing epithelial-to-mesenchymal transition (EMT.CTC) and circulating endothelial cells (CECs) using a universal rare event detection platform (HDSCA). Longitudinal analysis of an index patient finds that CTCs are present at the time of disease progression, while CECs are predominately present at the time of stable disease. In a small cohort of prostate and breast cancer patients, we find high inter-patient and temporal intra-patient variability in the expression of tissue specific markers such as ER, HER2, AR, PSA and PSMA and EpCAM. Our study stresses the importance of the multi-omic characterization of circulating rare cells in patients with breast and prostate carcinomas, specifically highlighting overlapping and cell type defining proteo-genomic characteristics of CTCs and CECs. [ABSTRACT FROM AUTHOR]

Published

2023