Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma

Norman G. Nicolson; Joseph A. Tandurella; Lawrence W. Wu; Jignasha Patel; Eli Morris; Toni T. Seppälä; Samantha Guinn; Haley Zlomke; Christopher R. Shubert; Kelly J. Lafaro; William R. Burns; John L. Cameron; Jin He; Elana Fertig; Elizabeth M. Jaffee; Jacquelyn W. Zimmerman; Richard A. Burkhart

doi:10.1097/SLA.0000000000006517

Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma

Norman G. Nicolson, Joseph A. Tandurella, Lawrence W. Wu, Jignasha Patel, Eli Morris, Toni T. Seppälä, Samantha Guinn, Haley Zlomke, Christopher R. Shubert, Kelly J. Lafaro, William R. Burns, John L. Cameron, Jin He, Elana Fertig, Elizabeth M. Jaffee, Jacquelyn W. Zimmerman, Richard A. Burkhart

School of Medicine

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

Abstract

Objective: We integrate a new approach to chemosensitivity data for clinically-relevant regimen matching, and demonstrate the relationship with clinical outcomes in a large PDO biobank. Summary Background Data: Pancreatic ductal adenocarcinoma (PDAC) usually recurs following potentially curative resection. Prior studies related patient-derived organoid (PDO) chemosensitivity with clinical responses. Methods: PDOs were established from pre-treatment biopsies in a multi-institution clinical trial (n=21) and clinical specimens at a high-volume pancreatectomy center (n=74, of which 48 were pre-treated). PDO in vitro chemosensitivities to standard-of-care chemotherapeutics (pharmacotypes) were matched to potential clinically-relevant regimens by a weighted nearest-neighbors analysis. Clinical outcomes were then compared for patients who had well-matched versus poorly-matched treatment according to this metric. Results: Our function matched 91% of PDOs to a standard-of-care regimen (9% pan-resistant). PDOs poorly-matched to the neoadjuvant regimen received would have matched to an alternative in 34% of cases. Patients receiving neoadjuvant chemotherapy well-matched to their pharmacotype experienced improved CA 19-9 response (60% decreased to normal when well-matched, 29% when poorly-matched, p<0.05) and lymph node down-staging (33% N0 after poorly-matched, 69% after well-matched, p<0.05). Patients receiving both well-matched neoadjuvant and adjuvant chemotherapy experienced improved recurrence-free- and overall survival (median RFS 8.5 months poorly-matched, 15.9 months well-matched, p<0.05; median OS 19.5 versus 30.3 months, p<0.05). Conclusion: In vitro PDO pharmacotyping can inform PDAC therapy selection. We demonstrate improved outcomes including survival for patients treated with regimens well-matched to their PDO chemosensitivities. A subsequent prospective study using PDO pharmacotype matching could improve oncologic outcomes and improve quality of life by avoiding therapies not expected to be effective.

Original language	English (US)
Article number	10.1097/SLA.0000000000006517
Journal	Annals of surgery
DOIs	https://doi.org/10.1097/SLA.0000000000006517
State	Accepted/In press - 2024

ASJC Scopus subject areas

Surgery

Access to Document

10.1097/SLA.0000000000006517

Cite this

Nicolson, N. G., Tandurella, J. A., Wu, L. W., Patel, J., Morris, E., Seppälä, T. T., Guinn, S., Zlomke, H., Shubert, C. R., Lafaro, K. J., Burns, W. R., Cameron, J. L., He, J., Fertig, E., Jaffee, E. M., Zimmerman, J. W., & Burkhart, R. A. (Accepted/In press). Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma. Annals of surgery, Article 10.1097/SLA.0000000000006517. https://doi.org/10.1097/SLA.0000000000006517

Nicolson, NG, Tandurella, JA, Wu, LW, Patel, J, Morris, E, Seppälä, TT, Guinn, S, Zlomke, H, Shubert, CR , Lafaro, KJ , Burns, WR , Cameron, JL , He, J, Fertig, E, Jaffee, EM , Zimmerman, JW & Burkhart, RA 2024, 'Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma', Annals of surgery. https://doi.org/10.1097/SLA.0000000000006517

@article{0052ed7062e9431e9a3b5d82b46b1eb4,

title = "Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma",

abstract = "Objective: We integrate a new approach to chemosensitivity data for clinically-relevant regimen matching, and demonstrate the relationship with clinical outcomes in a large PDO biobank. Summary Background Data: Pancreatic ductal adenocarcinoma (PDAC) usually recurs following potentially curative resection. Prior studies related patient-derived organoid (PDO) chemosensitivity with clinical responses. Methods: PDOs were established from pre-treatment biopsies in a multi-institution clinical trial (n=21) and clinical specimens at a high-volume pancreatectomy center (n=74, of which 48 were pre-treated). PDO in vitro chemosensitivities to standard-of-care chemotherapeutics (pharmacotypes) were matched to potential clinically-relevant regimens by a weighted nearest-neighbors analysis. Clinical outcomes were then compared for patients who had well-matched versus poorly-matched treatment according to this metric. Results: Our function matched 91% of PDOs to a standard-of-care regimen (9% pan-resistant). PDOs poorly-matched to the neoadjuvant regimen received would have matched to an alternative in 34% of cases. Patients receiving neoadjuvant chemotherapy well-matched to their pharmacotype experienced improved CA 19-9 response (60% decreased to normal when well-matched, 29% when poorly-matched, p<0.05) and lymph node down-staging (33% N0 after poorly-matched, 69% after well-matched, p<0.05). Patients receiving both well-matched neoadjuvant and adjuvant chemotherapy experienced improved recurrence-free- and overall survival (median RFS 8.5 months poorly-matched, 15.9 months well-matched, p<0.05; median OS 19.5 versus 30.3 months, p<0.05). Conclusion: In vitro PDO pharmacotyping can inform PDAC therapy selection. We demonstrate improved outcomes including survival for patients treated with regimens well-matched to their PDO chemosensitivities. A subsequent prospective study using PDO pharmacotype matching could improve oncologic outcomes and improve quality of life by avoiding therapies not expected to be effective.",

author = "Nicolson, {Norman G.} and Tandurella, {Joseph A.} and Wu, {Lawrence W.} and Jignasha Patel and Eli Morris and Sepp{\"a}l{\"a}, {Toni T.} and Samantha Guinn and Haley Zlomke and Shubert, {Christopher R.} and Lafaro, {Kelly J.} and Burns, {William R.} and Cameron, {John L.} and Jin He and Elana Fertig and Jaffee, {Elizabeth M.} and Zimmerman, {Jacquelyn W.} and Burkhart, {Richard A.}",

note = "Publisher Copyright: Copyright {\textcopyright} 2024 Wolters Kluwer Health, Inc.",

year = "2024",

doi = "10.1097/SLA.0000000000006517",

language = "English (US)",

journal = "Annals of surgery",

issn = "0003-4932",

publisher = "Wolters Kluwer Health",

}

TY - JOUR

T1 - Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma

AU - Nicolson, Norman G.

AU - Tandurella, Joseph A.

AU - Wu, Lawrence W.

AU - Patel, Jignasha

AU - Morris, Eli

AU - Seppälä, Toni T.

AU - Guinn, Samantha

AU - Zlomke, Haley

AU - Shubert, Christopher R.

AU - Lafaro, Kelly J.

AU - Burns, William R.

AU - Cameron, John L.

AU - He, Jin

AU - Fertig, Elana

AU - Jaffee, Elizabeth M.

AU - Zimmerman, Jacquelyn W.

AU - Burkhart, Richard A.

PY - 2024

Y1 - 2024

N2 - Objective: We integrate a new approach to chemosensitivity data for clinically-relevant regimen matching, and demonstrate the relationship with clinical outcomes in a large PDO biobank. Summary Background Data: Pancreatic ductal adenocarcinoma (PDAC) usually recurs following potentially curative resection. Prior studies related patient-derived organoid (PDO) chemosensitivity with clinical responses. Methods: PDOs were established from pre-treatment biopsies in a multi-institution clinical trial (n=21) and clinical specimens at a high-volume pancreatectomy center (n=74, of which 48 were pre-treated). PDO in vitro chemosensitivities to standard-of-care chemotherapeutics (pharmacotypes) were matched to potential clinically-relevant regimens by a weighted nearest-neighbors analysis. Clinical outcomes were then compared for patients who had well-matched versus poorly-matched treatment according to this metric. Results: Our function matched 91% of PDOs to a standard-of-care regimen (9% pan-resistant). PDOs poorly-matched to the neoadjuvant regimen received would have matched to an alternative in 34% of cases. Patients receiving neoadjuvant chemotherapy well-matched to their pharmacotype experienced improved CA 19-9 response (60% decreased to normal when well-matched, 29% when poorly-matched, p<0.05) and lymph node down-staging (33% N0 after poorly-matched, 69% after well-matched, p<0.05). Patients receiving both well-matched neoadjuvant and adjuvant chemotherapy experienced improved recurrence-free- and overall survival (median RFS 8.5 months poorly-matched, 15.9 months well-matched, p<0.05; median OS 19.5 versus 30.3 months, p<0.05). Conclusion: In vitro PDO pharmacotyping can inform PDAC therapy selection. We demonstrate improved outcomes including survival for patients treated with regimens well-matched to their PDO chemosensitivities. A subsequent prospective study using PDO pharmacotype matching could improve oncologic outcomes and improve quality of life by avoiding therapies not expected to be effective.

AB - Objective: We integrate a new approach to chemosensitivity data for clinically-relevant regimen matching, and demonstrate the relationship with clinical outcomes in a large PDO biobank. Summary Background Data: Pancreatic ductal adenocarcinoma (PDAC) usually recurs following potentially curative resection. Prior studies related patient-derived organoid (PDO) chemosensitivity with clinical responses. Methods: PDOs were established from pre-treatment biopsies in a multi-institution clinical trial (n=21) and clinical specimens at a high-volume pancreatectomy center (n=74, of which 48 were pre-treated). PDO in vitro chemosensitivities to standard-of-care chemotherapeutics (pharmacotypes) were matched to potential clinically-relevant regimens by a weighted nearest-neighbors analysis. Clinical outcomes were then compared for patients who had well-matched versus poorly-matched treatment according to this metric. Results: Our function matched 91% of PDOs to a standard-of-care regimen (9% pan-resistant). PDOs poorly-matched to the neoadjuvant regimen received would have matched to an alternative in 34% of cases. Patients receiving neoadjuvant chemotherapy well-matched to their pharmacotype experienced improved CA 19-9 response (60% decreased to normal when well-matched, 29% when poorly-matched, p<0.05) and lymph node down-staging (33% N0 after poorly-matched, 69% after well-matched, p<0.05). Patients receiving both well-matched neoadjuvant and adjuvant chemotherapy experienced improved recurrence-free- and overall survival (median RFS 8.5 months poorly-matched, 15.9 months well-matched, p<0.05; median OS 19.5 versus 30.3 months, p<0.05). Conclusion: In vitro PDO pharmacotyping can inform PDAC therapy selection. We demonstrate improved outcomes including survival for patients treated with regimens well-matched to their PDO chemosensitivities. A subsequent prospective study using PDO pharmacotype matching could improve oncologic outcomes and improve quality of life by avoiding therapies not expected to be effective.

UR - http://www.scopus.com/inward/record.url?scp=85203457688&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85203457688&partnerID=8YFLogxK

U2 - 10.1097/SLA.0000000000006517

DO - 10.1097/SLA.0000000000006517

M3 - Article

C2 - 39229726

AN - SCOPUS:85203457688

SN - 0003-4932

JO - Annals of surgery

JF - Annals of surgery

M1 - 10.1097/SLA.0000000000006517

ER -

Patient-derived organoid pharmacotyping as a predictive tool for therapeutic selection in pancreatic ductal adenocarcinoma

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this