Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients

J. Castillo; V. Bernard; F. A. San Lucas; K. Allenson; M. Capello; D. U. Kim; P. Gascoyne; F. C. Mulu; B. M. Stephens; J. Huang; H. Wang; A. A. Momin; R. O. Jacamo; M. Katz; R. Wolff; M. Javle; G. Varadhachary; I. I. Wistuba; S. Hanash; A. Maitra; H. Alvarez

doi:10.1093/annonc/mdx542

Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients

J. Castillo, V. Bernard, F. A. San Lucas, K. Allenson, M. Capello, D. U. Kim, P. Gascoyne, F. C. Mulu, B. M. Stephens, J. Huang, H. Wang, A. A. Momin, R. O. Jacamo, M. Katz, R. Wolff, M. Javle, G. Varadhachary, I. I. Wistuba, S. Hanash, A. MaitraH. Alvarez

Research output: Contribution to journal › Article › peer-review

165 Scopus citations

Abstract

Background: Detection of circulating tumor DNA can be limited due to their relative scarcity in circulation, particularly while patients are actively undergoing therapy. Exosomes provide a vehicle through which cancer-specific material can be enriched from the compendium of circulating non-neoplastic tissue-derived nucleic acids. We carried out a comprehensive profiling of the pancreatic ductal adenocarcinoma (PDAC) exosomal 'surfaceome' in order to identify surface proteins that will render liquid biopsies amenable to cancer-derived exosome enrichment for downstream molecular profiling. Patients and methods: Surface exosomal proteins were profiled in 13 human PDAC and 2 non-neoplastic cell lines by liquid chromatography-mass spectrometry. A total of 173 prospectively collected blood samples from 103 PDAC patients underwent exosome isolation. Droplet digital PCR was used on 74 patients (136 total exosome samples) to determine baseline KRAS mutation call rates while patients were on therapy. PDAC-specific exosome capture was then carried out on additional 29 patients (37 samples) using an antibody cocktail directed against selected proteins, followed by droplet digital PCR analysis. Exosomal DNA in a PDAC patient resistant to therapy were profiled using a molecular barcoded, targeted sequencing panel to determine the utility of enriched nucleic acid material for comprehensive molecular analysis. Results: Proteomic analysis of the exosome 'surfaceome' revealed multiple PDAC-specific biomarker candidates: CLDN4, EPCAM, CD151, LGALS3BP, HIST2H2BE, and HIST2H2BF. KRAS mutations in total exosomes were detected in 44.1% of patients undergoing active therapy compared with 73.0% following exosome capture using the selected biomarkers. Enrichment of exosomal cargo was amenable to molecular profiling, elucidating a putative mechanism of resistance to PARP inhibitor therapy in a patient harboring a BRCA2 mutation. Conclusion: Exosomes provide unique opportunities in the context of liquid biopsies for enrichment of tumor-specific material in circulation. We present a comprehensive surfaceome characterization of PDAC exosomes which allows for capture and molecular profiling of tumor-derived DNA.

Original language	English (US)
Pages (from-to)	223-229
Number of pages	7
Journal	Annals of Oncology
Volume	29
Issue number	1
DOIs	https://doi.org/10.1093/annonc/mdx542
State	Published - Jan 1 2018

Keywords

Exosomes
Liquid biopsies
Next-generation sequencing
Pancreatic cancer
Proteomics

ASJC Scopus subject areas

Hematology
Oncology

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10.1093/annonc/mdx542

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Castillo, J., Bernard, V., San Lucas, F. A., Allenson, K., Capello, M., Kim, D. U., Gascoyne, P., Mulu, F. C., Stephens, B. M., Huang, J., Wang, H., Momin, A. A., Jacamo, R. O., Katz, M., Wolff, R., Javle, M., Varadhachary, G., Wistuba, I. I., Hanash, S., ... Alvarez, H. (2018). Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients. Annals of Oncology, 29(1), 223-229. https://doi.org/10.1093/annonc/mdx542

Castillo, J, Bernard, V, San Lucas, FA, Allenson, K, Capello, M, Kim, DU, Gascoyne, P, Mulu, FC, Stephens, BM, Huang, J, Wang, H, Momin, AA, Jacamo, RO, Katz, M , Wolff, R , Javle, M, Varadhachary, G, Wistuba, II , Hanash, S , Maitra, A & Alvarez, H 2018, 'Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients', Annals of Oncology, vol. 29, no. 1, pp. 223-229. https://doi.org/10.1093/annonc/mdx542

@article{50953bc500fe40e49c9ea41061d7869b,

title = "Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients",

abstract = "Background: Detection of circulating tumor DNA can be limited due to their relative scarcity in circulation, particularly while patients are actively undergoing therapy. Exosomes provide a vehicle through which cancer-specific material can be enriched from the compendium of circulating non-neoplastic tissue-derived nucleic acids. We carried out a comprehensive profiling of the pancreatic ductal adenocarcinoma (PDAC) exosomal 'surfaceome' in order to identify surface proteins that will render liquid biopsies amenable to cancer-derived exosome enrichment for downstream molecular profiling. Patients and methods: Surface exosomal proteins were profiled in 13 human PDAC and 2 non-neoplastic cell lines by liquid chromatography-mass spectrometry. A total of 173 prospectively collected blood samples from 103 PDAC patients underwent exosome isolation. Droplet digital PCR was used on 74 patients (136 total exosome samples) to determine baseline KRAS mutation call rates while patients were on therapy. PDAC-specific exosome capture was then carried out on additional 29 patients (37 samples) using an antibody cocktail directed against selected proteins, followed by droplet digital PCR analysis. Exosomal DNA in a PDAC patient resistant to therapy were profiled using a molecular barcoded, targeted sequencing panel to determine the utility of enriched nucleic acid material for comprehensive molecular analysis. Results: Proteomic analysis of the exosome 'surfaceome' revealed multiple PDAC-specific biomarker candidates: CLDN4, EPCAM, CD151, LGALS3BP, HIST2H2BE, and HIST2H2BF. KRAS mutations in total exosomes were detected in 44.1% of patients undergoing active therapy compared with 73.0% following exosome capture using the selected biomarkers. Enrichment of exosomal cargo was amenable to molecular profiling, elucidating a putative mechanism of resistance to PARP inhibitor therapy in a patient harboring a BRCA2 mutation. Conclusion: Exosomes provide unique opportunities in the context of liquid biopsies for enrichment of tumor-specific material in circulation. We present a comprehensive surfaceome characterization of PDAC exosomes which allows for capture and molecular profiling of tumor-derived DNA.",

keywords = "Exosomes, Liquid biopsies, Next-generation sequencing, Pancreatic cancer, Proteomics",

author = "J. Castillo and V. Bernard and {San Lucas}, {F. A.} and K. Allenson and M. Capello and Kim, {D. U.} and P. Gascoyne and Mulu, {F. C.} and Stephens, {B. M.} and J. Huang and H. Wang and Momin, {A. A.} and Jacamo, {R. O.} and M. Katz and R. Wolff and M. Javle and G. Varadhachary and Wistuba, {I. I.} and S. Hanash and A. Maitra and H. Alvarez",

note = "Funding Information: MD Anderson Moonshot Program and the Khalifa Bin Zayed Al-Nahyan Foundation (no grant numbers apply); the National Institute of Health (U01CA196403 and U01CA200468 to AM); the Cancer Prevention Research Institute of Texas (RP160517 to AM and RP140106 to VB); a faculty fellowship from The University of Texas MD Anderson Cancer Center Duncan Family Institute for Cancer Prevention and Risk Assessment (MC) (no grant number applies); a foreign postdoctoral fellowship grant, Chile – CONICYT (JC) (no grant number applies). Publisher Copyright: {\textcopyright} The Author 2017.",

year = "2018",

month = jan,

day = "1",

doi = "10.1093/annonc/mdx542",

language = "English (US)",

volume = "29",

pages = "223--229",

journal = "Annals of Oncology",

issn = "0923-7534",

publisher = "Oxford University Press",

number = "1",

}

TY - JOUR

T1 - Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients

AU - Castillo, J.

AU - Bernard, V.

AU - San Lucas, F. A.

AU - Allenson, K.

AU - Capello, M.

AU - Kim, D. U.

AU - Gascoyne, P.

AU - Mulu, F. C.

AU - Stephens, B. M.

AU - Huang, J.

AU - Wang, H.

AU - Momin, A. A.

AU - Jacamo, R. O.

AU - Katz, M.

AU - Wolff, R.

AU - Javle, M.

AU - Varadhachary, G.

AU - Wistuba, I. I.

AU - Hanash, S.

AU - Maitra, A.

AU - Alvarez, H.

N1 - Funding Information: MD Anderson Moonshot Program and the Khalifa Bin Zayed Al-Nahyan Foundation (no grant numbers apply); the National Institute of Health (U01CA196403 and U01CA200468 to AM); the Cancer Prevention Research Institute of Texas (RP160517 to AM and RP140106 to VB); a faculty fellowship from The University of Texas MD Anderson Cancer Center Duncan Family Institute for Cancer Prevention and Risk Assessment (MC) (no grant number applies); a foreign postdoctoral fellowship grant, Chile – CONICYT (JC) (no grant number applies). Publisher Copyright: © The Author 2017.

PY - 2018/1/1

Y1 - 2018/1/1

N2 - Background: Detection of circulating tumor DNA can be limited due to their relative scarcity in circulation, particularly while patients are actively undergoing therapy. Exosomes provide a vehicle through which cancer-specific material can be enriched from the compendium of circulating non-neoplastic tissue-derived nucleic acids. We carried out a comprehensive profiling of the pancreatic ductal adenocarcinoma (PDAC) exosomal 'surfaceome' in order to identify surface proteins that will render liquid biopsies amenable to cancer-derived exosome enrichment for downstream molecular profiling. Patients and methods: Surface exosomal proteins were profiled in 13 human PDAC and 2 non-neoplastic cell lines by liquid chromatography-mass spectrometry. A total of 173 prospectively collected blood samples from 103 PDAC patients underwent exosome isolation. Droplet digital PCR was used on 74 patients (136 total exosome samples) to determine baseline KRAS mutation call rates while patients were on therapy. PDAC-specific exosome capture was then carried out on additional 29 patients (37 samples) using an antibody cocktail directed against selected proteins, followed by droplet digital PCR analysis. Exosomal DNA in a PDAC patient resistant to therapy were profiled using a molecular barcoded, targeted sequencing panel to determine the utility of enriched nucleic acid material for comprehensive molecular analysis. Results: Proteomic analysis of the exosome 'surfaceome' revealed multiple PDAC-specific biomarker candidates: CLDN4, EPCAM, CD151, LGALS3BP, HIST2H2BE, and HIST2H2BF. KRAS mutations in total exosomes were detected in 44.1% of patients undergoing active therapy compared with 73.0% following exosome capture using the selected biomarkers. Enrichment of exosomal cargo was amenable to molecular profiling, elucidating a putative mechanism of resistance to PARP inhibitor therapy in a patient harboring a BRCA2 mutation. Conclusion: Exosomes provide unique opportunities in the context of liquid biopsies for enrichment of tumor-specific material in circulation. We present a comprehensive surfaceome characterization of PDAC exosomes which allows for capture and molecular profiling of tumor-derived DNA.

AB - Background: Detection of circulating tumor DNA can be limited due to their relative scarcity in circulation, particularly while patients are actively undergoing therapy. Exosomes provide a vehicle through which cancer-specific material can be enriched from the compendium of circulating non-neoplastic tissue-derived nucleic acids. We carried out a comprehensive profiling of the pancreatic ductal adenocarcinoma (PDAC) exosomal 'surfaceome' in order to identify surface proteins that will render liquid biopsies amenable to cancer-derived exosome enrichment for downstream molecular profiling. Patients and methods: Surface exosomal proteins were profiled in 13 human PDAC and 2 non-neoplastic cell lines by liquid chromatography-mass spectrometry. A total of 173 prospectively collected blood samples from 103 PDAC patients underwent exosome isolation. Droplet digital PCR was used on 74 patients (136 total exosome samples) to determine baseline KRAS mutation call rates while patients were on therapy. PDAC-specific exosome capture was then carried out on additional 29 patients (37 samples) using an antibody cocktail directed against selected proteins, followed by droplet digital PCR analysis. Exosomal DNA in a PDAC patient resistant to therapy were profiled using a molecular barcoded, targeted sequencing panel to determine the utility of enriched nucleic acid material for comprehensive molecular analysis. Results: Proteomic analysis of the exosome 'surfaceome' revealed multiple PDAC-specific biomarker candidates: CLDN4, EPCAM, CD151, LGALS3BP, HIST2H2BE, and HIST2H2BF. KRAS mutations in total exosomes were detected in 44.1% of patients undergoing active therapy compared with 73.0% following exosome capture using the selected biomarkers. Enrichment of exosomal cargo was amenable to molecular profiling, elucidating a putative mechanism of resistance to PARP inhibitor therapy in a patient harboring a BRCA2 mutation. Conclusion: Exosomes provide unique opportunities in the context of liquid biopsies for enrichment of tumor-specific material in circulation. We present a comprehensive surfaceome characterization of PDAC exosomes which allows for capture and molecular profiling of tumor-derived DNA.

KW - Exosomes

KW - Liquid biopsies

KW - Next-generation sequencing

KW - Pancreatic cancer

KW - Proteomics

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DO - 10.1093/annonc/mdx542

M3 - Article

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AN - SCOPUS:85041222874

SN - 0923-7534

VL - 29

SP - 223

EP - 229

JO - Annals of Oncology

JF - Annals of Oncology

IS - 1

ER -

Surfaceome profiling enables isolation of cancerspecific exosomal cargo in liquid biopsies from pancreatic cancer patients

Abstract

Keywords

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