Characterisation of circulating tumor‐associated and immune cells in patients with advanced‐stage non‐small cell lung cancer

Vahid Yaghoubi Naei; Ekaterina Ivanova; William Mullally; Connor G O'Leary; Rahul Ladwa; Ken O'Byrne; Majid E Warkiani; Arutha Kulasinghe

doi:10.1002/cti2.1516

Clinical & Translational Immunology (Jan 2024)

Characterisation of circulating tumor‐associated and immune cells in patients with advanced‐stage non‐small cell lung cancer

Vahid Yaghoubi Naei,
Ekaterina Ivanova,
William Mullally,
Connor G O'Leary,
Rahul Ladwa,
Ken O'Byrne,
Majid E Warkiani,
Arutha Kulasinghe

Affiliations

Vahid Yaghoubi Naei: School of Biomedical Engineering University of Technology Sydney Sydney NSW Australia
Ekaterina Ivanova: Cancer and Ageing Research Program, Centre for Genomics and Personalised Health Queensland University of Technology Woolloongabba QLD Australia
William Mullally: The Princess Alexandra Hospital Brisbane QLD Australia
Connor G O'Leary: The Princess Alexandra Hospital Brisbane QLD Australia
Rahul Ladwa: Frazer Institute, Faculty of Medicine The University of Queensland Brisbane QLD Australia
Ken O'Byrne: The Princess Alexandra Hospital Brisbane QLD Australia
Majid E Warkiani: School of Biomedical Engineering University of Technology Sydney Sydney NSW Australia
Arutha Kulasinghe: Frazer Institute, Faculty of Medicine The University of Queensland Brisbane QLD Australia

DOI: https://doi.org/10.1002/cti2.1516
Journal volume & issue: Vol. 13, no. 6
pp. n/a – n/a

Abstract

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Abstract Objectives Globally, non‐small cell lung cancer (NSCLC) is the most prevalent form of lung cancer and the leading cause of cancer‐related deaths. Tumor‐associated circulating cells in NSCLC can have a wide variety of morphological and phenotypic characteristics, including epithelial, immunological or hybrid subtypes. The distinctive characteristics and potential clinical significance of these cells in patients with NSCLC are explored in this study. Methods We utilised a spiral microfluidic device to enrich large cells and cell aggregates from the peripheral blood samples of NSCLC patients. These cells were characterised through high‐resolution immunofluorescent imaging and statistical analysis, correlating findings with clinical information from our patient cohort. Results We have identified varied populations of heterotypic circulating tumor cell clusters with differing immune cell composition that included a distinct class of atypical tumor‐associated macrophages that exhibits unique morphology and cell size. This subtype's prevalence is positively correlated with the tumor stage, progression and metastasis. Conclusions Our study reveals a heterogeneous landscape of circulating tumor cells and their clusters, underscoring the complexity of NSCLC pathobiology. The identification of a unique subtype of atypical tumor‐associatedmacrophages that simultaneously express both tumor and immune markers and whose presence correlates with late disease stages, poor clinical outcomes and metastatic risk infers the potential of these cells as biomarkers for NSCLC staging and prognosis. Future studies should focus on the role of these cells in the tumor microenvironment and their potential as therapeutic targets. Additionally, longitudinal studies tracking these cell types through disease progression could provide further insights into their roles in NSCLC evolution and response to treatment.

Published in Clinical & Translational Immunology

ISSN: 2050-0068 (Online)
Publisher: Wiley
Country of publisher: Australia
LCC subjects: Medicine: Internal medicine: Specialties of internal medicine: Immunologic diseases. Allergy
Website: https://onlinelibrary.wiley.com/journal/20500068

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Abstract

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