| Literature DB >> 34072942 |
Harrys Kishore Charles Jacob1,2, John Lalith Charles Richard3, Rossana Signorelli4, Tyler Kashuv5, Shweta Lavania1,2, Utpreksha Vaish6, Ranjitha Boopathy7, Ashley Middleton1,2, Melinda Minucci Boone8, Ramakrishnan Sundaram1,2, Vikas Dudeja1,2,7, Ashok Kumar Saluja1,2.
Abstract
Tumor cells dissociate from the primary site and enter into systemic circulation (circulating tumor cells, CTCs) either alone or as tumor microemboli (clusters); the latter having an increased predisposition towards forming distal metastases than single CTCs. The formation of clusters is, in part, created by contacts between cell-cell junction proteins and/or cytokine receptor pairs with other cells such as neutrophils, platelets, fibroblasts, etc. In the present study, we provide evidence for an extravesicular (EV) mode of communication between pancreatic cancer CTCs and neutrophils. Our results suggest that the EV proteome of CTCs contain signaling proteins that can modulate degranulation and granule mobilization in neutrophils and, also, contain tissue plasminogen activator and other proteins that can regulate cluster formation. By exposing naïve neutrophils to EVs isolated from CTCs, we further show how these changes are modulated in a dynamic fashion indicating evidence for a deeper EV based remodulatory effect on companion cells in clusters.Entities:
Keywords: circulating tumor cells; clusters; extracellular vesicles; granule mobilization; neutrophil degranulation; pancreatic cancer; reteplase activity
Year: 2021 PMID: 34072942 DOI: 10.3390/cancers13112727
Source DB: PubMed Journal: Cancers (Basel) ISSN: 2072-6694 Impact factor: 6.639