| Literature DB >> 31957112 |
Merav E Shaul1, Ophir Eyal1, Silvia Guglietta2,3, Pazzit Aloni1, Asaf Zlotnik1, Ester Forkosh1, Liran Levy1, Lukas M Weber4,5, Yonathan Levin1, Alon Pomerantz1, Hovav Nechushtan6, Evgeniy Eruslanov7, Sunil Singhal7, Mark D Robinson4,5, Carsten Krieg2,3, Zvi G Fridlender1.
Abstract
The accumulation of circulating low-density neutrophils (LDN) has been described in cancer patients and associated with tumor-supportive properties, as opposed to the high-density neutrophils (HDN). Here we aimed to evaluate the clinical significance of circulating LDN in lung cancer patients, and further assessed its diagnostic vs prognostic value. Using mass cytometry (CyTOF), we identified major subpopulations within the circulating LDN/HDN subsets and determined phenotypic modulations of these subsets along tumor progression. LDN were highly enriched in the low-density (LD) fraction of advanced lung cancer patients (median 7.0%; range 0.2%-80%, n = 64), but not in early stage patients (0.7%; 0.05%-6%; n = 35), healthy individuals (0.8%; 0%-3.5%; n = 15), or stable chronic obstructive pulmonary disease (COPD) patients (1.2%; 0.3%-7.4%, n = 13). Elevated LDN (>10%) remarkably related with poorer prognosis in late stage patients. We identified three main neutrophil subsets which proportions are markedly modified in cancer patients, with CD66b+ /CD10low /CXCR4+ /PDL1inter subset almost exclusively found in advanced lung cancer patients. We found substantial variability in subsets between patients, and demonstrated that HDN and LDN retain a degree of inherent spontaneous plasticity. Deep phenotypic characterization of cancer-related circulating neutrophils and their modulation along tumor progression is an important advancement in understanding the role of myeloid cells in lung cancer.Entities:
Keywords: lung cancer; mass cytometry; neutrophils; phenotypic modulation
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Year: 2020 PMID: 31957112 DOI: 10.1096/fj.201902467R
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.191