Extracellular vesicle heterogeneity through the lens of multiomics

Silva, Taylon F.; Hutchins, Elizabeth; Zhao, Wenyan; Ciani, Yari; Kim, Minhyung; Emily, Ko; Mariscal, Javier; Qiu, Zhuyu; Bedier, Fatima; Kittel, Agnes; Zhou, Bo; Wang, Yang; Hall, Megan; Galasso, Francesca; Reiman, Rebecca; Freeman, Michael R.; Parker, Sarah; Van Eyk, Jennifer; Yang, Wei; Posadas, Edwin; Guarnerio, Jlenia; Nolan, John; Thery, Clotilde; Zijlstra, Andries; Stott, Shannon; You, Sungyong; Demichelis, Francesca; Boutros, Paul C; Van Keuren-Jensen, Kendall; Di Vizio, Dolores

doi:10.1016/j.xcrm.2025.102161

Extracellular vesicles (EVs) are heterogeneous in size, biogenesis, content, and function. Aggressive cancer cells release a distinct, poorly characterized, and particularly large EV subtype, namely large oncosomes (LOs). This study employs an optimized method to improve LO yields and integrates mass spectrometry and RNA sequencing (RNA-seq) to profile their molecular cargo. A consistent set of proteins enriched in LOs is identified across glioma, prostate, and breast cancer cell lines. These proteins are also present as mRNA in LOs from the prostate cancer model and are abundant in plasma LOs from 20 patients with metastasis. Single-LO RNA-seq confirms bulk LO cargo, demonstrating the utility of single-cell technologies for large vesicle analysis. Our patient study provides proof-of-principle evidence that we can use multiomics to delve into EV heterogeneity, biogenesis, and composition. It also suggests that plasma LOs help stratify patients, supporting their potential prognostic value for developing a multi-analyte approach for liquid biopsy.

Extracellular vesicle heterogeneity through the lens of multiomics / Silva, Taylon F.; Hutchins, Elizabeth; Zhao, Wenyan; Ciani, Yari; Kim, Minhyung; Ko, Emily; Mariscal, Javier; Qiu, Zhuyu; Bedier, Fatima; Kittel, Agnes; Zhou, Bo; Wang, Yang; Hall, Megan; Galasso, Francesca; Reiman, Rebecca; Freeman, Michael R.; Parker, Sarah; Van Eyk, Jennifer; Yang, Wei; Posadas, Edwin; Guarnerio, Jlenia; Nolan, John; Thery, Clotilde; Zijlstra, Andries; Stott, Shannon; You, Sungyong; Demichelis, Francesca; Boutros, Paul C; Van Keuren-Jensen, Kendall; Di Vizio, Dolores. - In: CELL REPORTS MEDICINE. - ISSN 2666-3791. - 6:7(2025), pp. 102161.01-102161.e10. [10.1016/j.xcrm.2025.102161]

Extracellular vesicle heterogeneity through the lens of multiomics

Silva, Taylon F.;Hutchins, Elizabeth;Zhao, Wenyan;Ciani, Yari;Kim, Minhyung;Ko, Emily;Mariscal, Javier;Qiu, Zhuyu;Bedier, Fatima;Kittel, Agnes;Zhou, Bo;Wang, Yang;Hall, Megan;Galasso, Francesca;Reiman, Rebecca;Freeman, Michael R.;Parker, Sarah;Van Eyk, Jennifer;Yang, Wei;Posadas, Edwin;Guarnerio, Jlenia;Nolan, John;Thery, Clotilde;Zijlstra, Andries;Stott, Shannon;You, Sungyong;Demichelis, Francesca;Boutros, Paul C;Van Keuren-Jensen, Kendall;Di Vizio, Dolores

2025-01-01

Abstract

Extracellular vesicles (EVs) are heterogeneous in size, biogenesis, content, and function. Aggressive cancer cells release a distinct, poorly characterized, and particularly large EV subtype, namely large oncosomes (LOs). This study employs an optimized method to improve LO yields and integrates mass spectrometry and RNA sequencing (RNA-seq) to profile their molecular cargo. A consistent set of proteins enriched in LOs is identified across glioma, prostate, and breast cancer cell lines. These proteins are also present as mRNA in LOs from the prostate cancer model and are abundant in plasma LOs from 20 patients with metastasis. Single-LO RNA-seq confirms bulk LO cargo, demonstrating the utility of single-cell technologies for large vesicle analysis. Our patient study provides proof-of-principle evidence that we can use multiomics to delve into EV heterogeneity, biogenesis, and composition. It also suggests that plasma LOs help stratify patients, supporting their potential prognostic value for developing a multi-analyte approach for liquid biopsy.

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	Anno di pubblicazione (Date of publication)
	
				2025
			
	Titolo del periodico (Journal title)
	
				CELL REPORTS MEDICINE
			
	Numero e parte del fascicolo (Issue number and part)
	
				7
			
	DOI
	
				https://dx.doi.org/10.1016/j.xcrm.2025.102161
			
	Codice PubMed (PubMed Identifier)
	
				40482644
			
	Codice Scopus (Scopus identifier)
	
				2-s2.0-105007448844
			
	Codice WOS (WOS identifier)
	
				WOS:001539725900001
			
	Tutti gli autori
	
						Silva, Taylon F.; Hutchins, Elizabeth; Zhao, Wenyan; Ciani, Yari; Kim, Minhyung; Ko, Emily; Mariscal, Javier; Qiu, Zhuyu; Bedier, Fatima; Kittel, Agne...espandi
						
	Citazione
	
				Extracellular vesicle heterogeneity through the lens of multiomics / Silva, Taylon F.; Hutchins, Elizabeth; Zhao, Wenyan; Ciani, Yari; Kim, Minhyung; Ko, Emily; Mariscal, Javier; Qiu, Zhuyu; Bedier, Fatima; Kittel, Agnes; Zhou, Bo; Wang, Yang; Hall, Megan; Galasso, Francesca; Reiman, Rebecca; Freeman, Michael R.; Parker, Sarah; Van Eyk, Jennifer; Yang, Wei; Posadas, Edwin; Guarnerio, Jlenia; Nolan, John; Thery, Clotilde; Zijlstra, Andries; Stott, Shannon; You, Sungyong; Demichelis, Francesca; Boutros, Paul C; Van Keuren-Jensen, Kendall; Di Vizio, Dolores. - In: CELL REPORTS MEDICINE. - ISSN 2666-3791. - 6:7(2025), pp. 102161.01-102161.e10. [10.1016/j.xcrm.2025.102161]
			
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				03.1 Articolo su rivista (Journal article)

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