Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer

Koji Tamura; Jun Yu; Tatsuo Hata; Masaya Suenaga; Koji Shindo; Toshiya Abe; Anne MacGregor-Das; Michael Borges; Christopher L. Wolfgang; Matthew J. Weiss; Jin He; Marcia Irene Canto; Gloria M. Petersen; Steven Gallinger; Sapna Syngal; Randall E. Brand; Anil Rustgi; Sara H. Olson; Elena Stoffel; Michele L. Cote; George Zogopoulos; James B. Potash; Fernando S. Goes; Richard W. McCombie; Peter P. Zandi; Mehdi Pirooznia; Melissa Kramer; Jennifer Parla; James R. Eshleman; Nicholas J. Roberts; Ralph H. Hruban; Alison Patricia Klein; Michael Goggins

doi:10.1073/pnas.1720588115

Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer

Koji Tamura, Jun Yu, Tatsuo Hata, Masaya Suenaga, Koji Shindo, Toshiya Abe, Anne MacGregor-Das, Michael Borges, Christopher L. Wolfgang, Matthew J. Weiss, Jin He, Marcia Irene Canto, Gloria M. Petersen, Steven Gallinger, Sapna Syngal, Randall E. Brand, Anil Rustgi, Sara H. Olson, Elena Stoffel, Michele L. CoteGeorge Zogopoulos, James B. Potash, Fernando S. Goes, Richard W. McCombie, Peter P. Zandi, Mehdi Pirooznia, Melissa Kramer, Jennifer Parla, James R. Eshleman, Nicholas J. Roberts, Ralph H. Hruban, Alison Patricia Klein, Michael Goggins

School of Medicine

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

21 Scopus citations

Abstract

To evaluate whether germline variants in genes encoding pancreatic secretory enzymes contribute to pancreatic cancer susceptibility, we sequenced the coding regions of CPB1 and other genes encoding pancreatic secretory enzymes and known pancreatitis susceptibility genes (PRSS1, CPA1, CTRC, and SPINK1) in a hospital series of pancreatic cancer cases and controls. Variants in CPB1, CPA1 (encoding carboxypeptidase B1 and A1), and CTRC were evaluated in a second set of cases with familial pancreatic cancer and controls. More deleterious CPB1 variants, defined as having impaired protein secretion and induction of endoplasmic reticulum (ER) stress in transfected HEK 293T cells, were found in the hospital series of pancreatic cancer cases (5/986, 0.5%) than in controls (0/1,045, P = 0.027). Among familial pancreatic cancer cases, ER stress-inducing CPB1 variants were found in 4 of 593 (0.67%) vs. 0 of 967 additional controls (P = 0.020), with a combined prevalence in pancreatic cancer cases of 9/1,579 vs. 0/2,012 controls (P < 0.01). More ER stress-inducing CPA1 variants were also found in the combined set of hospital and familial cases with pancreatic cancer than in controls [7/1,546 vs. 1/2,012; P = 0.025; odds ratio, 9.36 (95% CI, 1.15–76.02)]. Overall, 16 (1%) of 1,579 pancreatic cancer cases had an ER stress-inducing CPA1 or CPB1 variant, compared with 1 of 2,068 controls (P < 0.00001). No other candidate genes had statistically significant differences in variant prevalence between cases and controls. Our study indicates ER stress-inducing variants in CPB1 and CPA1 are associated with pancreatic cancer susceptibility and implicate ER stress in pancreatic acinar cells in pancreatic cancer development.

Original language	English (US)
Pages (from-to)	4767-4772
Number of pages	6
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	115
Issue number	18
DOIs	https://doi.org/10.1073/pnas.1720588115
State	Published - May 1 2018

Keywords

CPA1
CPB1
ER stress
Pancreatic cancer
Pancreatitis

ASJC Scopus subject areas

General

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10.1073/pnas.1720588115

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Tamura, K., Yu, J., Hata, T., Suenaga, M., Shindo, K., Abe, T., MacGregor-Das, A., Borges, M., Wolfgang, C. L., Weiss, M. J., He, J., Canto, M. I., Petersen, G. M., Gallinger, S., Syngal, S., Brand, R. E., Rustgi, A., Olson, S. H., Stoffel, E., ... Goggins, M. (2018). Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer. Proceedings of the National Academy of Sciences of the United States of America, 115(18), 4767-4772. https://doi.org/10.1073/pnas.1720588115

Tamura, K, Yu, J, Hata, T, Suenaga, M, Shindo, K, Abe, T, MacGregor-Das, A, Borges, M, Wolfgang, CL, Weiss, MJ, He, J , Canto, MI, Petersen, GM, Gallinger, S, Syngal, S, Brand, RE, Rustgi, A, Olson, SH, Stoffel, E, Cote, ML, Zogopoulos, G, Potash, JB , Goes, FS, McCombie, RW, Zandi, PP, Pirooznia, M, Kramer, M, Parla, J, Eshleman, JR , Roberts, NJ , Hruban, RH , Klein, AP & Goggins, M 2018, 'Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer', Proceedings of the National Academy of Sciences of the United States of America, vol. 115, no. 18, pp. 4767-4772. https://doi.org/10.1073/pnas.1720588115

@article{0cac903f5ff44a5984ee07b78392101b,

title = "Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer",

abstract = "To evaluate whether germline variants in genes encoding pancreatic secretory enzymes contribute to pancreatic cancer susceptibility, we sequenced the coding regions of CPB1 and other genes encoding pancreatic secretory enzymes and known pancreatitis susceptibility genes (PRSS1, CPA1, CTRC, and SPINK1) in a hospital series of pancreatic cancer cases and controls. Variants in CPB1, CPA1 (encoding carboxypeptidase B1 and A1), and CTRC were evaluated in a second set of cases with familial pancreatic cancer and controls. More deleterious CPB1 variants, defined as having impaired protein secretion and induction of endoplasmic reticulum (ER) stress in transfected HEK 293T cells, were found in the hospital series of pancreatic cancer cases (5/986, 0.5%) than in controls (0/1,045, P = 0.027). Among familial pancreatic cancer cases, ER stress-inducing CPB1 variants were found in 4 of 593 (0.67%) vs. 0 of 967 additional controls (P = 0.020), with a combined prevalence in pancreatic cancer cases of 9/1,579 vs. 0/2,012 controls (P < 0.01). More ER stress-inducing CPA1 variants were also found in the combined set of hospital and familial cases with pancreatic cancer than in controls [7/1,546 vs. 1/2,012; P = 0.025; odds ratio, 9.36 (95% CI, 1.15–76.02)]. Overall, 16 (1%) of 1,579 pancreatic cancer cases had an ER stress-inducing CPA1 or CPB1 variant, compared with 1 of 2,068 controls (P < 0.00001). No other candidate genes had statistically significant differences in variant prevalence between cases and controls. Our study indicates ER stress-inducing variants in CPB1 and CPA1 are associated with pancreatic cancer susceptibility and implicate ER stress in pancreatic acinar cells in pancreatic cancer development.",

keywords = "CPA1, CPB1, ER stress, Pancreatic cancer, Pancreatitis",

author = "Koji Tamura and Jun Yu and Tatsuo Hata and Masaya Suenaga and Koji Shindo and Toshiya Abe and Anne MacGregor-Das and Michael Borges and Wolfgang, {Christopher L.} and Weiss, {Matthew J.} and Jin He and Canto, {Marcia Irene} and Petersen, {Gloria M.} and Steven Gallinger and Sapna Syngal and Brand, {Randall E.} and Anil Rustgi and Olson, {Sara H.} and Elena Stoffel and Cote, {Michele L.} and George Zogopoulos and Potash, {James B.} and Goes, {Fernando S.} and McCombie, {Richard W.} and Zandi, {Peter P.} and Mehdi Pirooznia and Melissa Kramer and Jennifer Parla and Eshleman, {James R.} and Roberts, {Nicholas J.} and Hruban, {Ralph H.} and Klein, {Alison Patricia} and Michael Goggins",

note = "Funding Information: ACKNOWLEDGMENTS. We thank all study participants and the members of NFPTR for providing clinical data and samples. This work was supported by NIH Grants CA62924, CA176828, CA210170, CA154823, CA132829, CA190889, and P30CA008748; Susan Wojcicki and Dennis Troper; the Rolfe Pancreatic Cancer Foundation; and the Karp Family HH&M Metals Fund. M.G. is the Sol Goldman Professor of Pancreatic Cancer Research. Publisher Copyright: {\textcopyright} 2018 National Academy of Sciences. All rights reserved.",

year = "2018",

month = may,

day = "1",

doi = "10.1073/pnas.1720588115",

language = "English (US)",

volume = "115",

pages = "4767--4772",

journal = "Proceedings of the National Academy of Sciences of the United States of America",

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T1 - Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer

AU - Tamura, Koji

AU - Yu, Jun

AU - Hata, Tatsuo

AU - Suenaga, Masaya

AU - Shindo, Koji

AU - Abe, Toshiya

AU - MacGregor-Das, Anne

AU - Borges, Michael

AU - Wolfgang, Christopher L.

AU - Weiss, Matthew J.

AU - He, Jin

AU - Canto, Marcia Irene

AU - Petersen, Gloria M.

AU - Gallinger, Steven

AU - Syngal, Sapna

AU - Brand, Randall E.

AU - Rustgi, Anil

AU - Olson, Sara H.

AU - Stoffel, Elena

AU - Cote, Michele L.

AU - Zogopoulos, George

AU - Potash, James B.

AU - Goes, Fernando S.

AU - McCombie, Richard W.

AU - Zandi, Peter P.

AU - Pirooznia, Mehdi

AU - Kramer, Melissa

AU - Parla, Jennifer

AU - Eshleman, James R.

AU - Roberts, Nicholas J.

AU - Hruban, Ralph H.

AU - Klein, Alison Patricia

AU - Goggins, Michael

N1 - Funding Information: ACKNOWLEDGMENTS. We thank all study participants and the members of NFPTR for providing clinical data and samples. This work was supported by NIH Grants CA62924, CA176828, CA210170, CA154823, CA132829, CA190889, and P30CA008748; Susan Wojcicki and Dennis Troper; the Rolfe Pancreatic Cancer Foundation; and the Karp Family HH&M Metals Fund. M.G. is the Sol Goldman Professor of Pancreatic Cancer Research. Publisher Copyright: © 2018 National Academy of Sciences. All rights reserved.

PY - 2018/5/1

Y1 - 2018/5/1

N2 - To evaluate whether germline variants in genes encoding pancreatic secretory enzymes contribute to pancreatic cancer susceptibility, we sequenced the coding regions of CPB1 and other genes encoding pancreatic secretory enzymes and known pancreatitis susceptibility genes (PRSS1, CPA1, CTRC, and SPINK1) in a hospital series of pancreatic cancer cases and controls. Variants in CPB1, CPA1 (encoding carboxypeptidase B1 and A1), and CTRC were evaluated in a second set of cases with familial pancreatic cancer and controls. More deleterious CPB1 variants, defined as having impaired protein secretion and induction of endoplasmic reticulum (ER) stress in transfected HEK 293T cells, were found in the hospital series of pancreatic cancer cases (5/986, 0.5%) than in controls (0/1,045, P = 0.027). Among familial pancreatic cancer cases, ER stress-inducing CPB1 variants were found in 4 of 593 (0.67%) vs. 0 of 967 additional controls (P = 0.020), with a combined prevalence in pancreatic cancer cases of 9/1,579 vs. 0/2,012 controls (P < 0.01). More ER stress-inducing CPA1 variants were also found in the combined set of hospital and familial cases with pancreatic cancer than in controls [7/1,546 vs. 1/2,012; P = 0.025; odds ratio, 9.36 (95% CI, 1.15–76.02)]. Overall, 16 (1%) of 1,579 pancreatic cancer cases had an ER stress-inducing CPA1 or CPB1 variant, compared with 1 of 2,068 controls (P < 0.00001). No other candidate genes had statistically significant differences in variant prevalence between cases and controls. Our study indicates ER stress-inducing variants in CPB1 and CPA1 are associated with pancreatic cancer susceptibility and implicate ER stress in pancreatic acinar cells in pancreatic cancer development.

AB - To evaluate whether germline variants in genes encoding pancreatic secretory enzymes contribute to pancreatic cancer susceptibility, we sequenced the coding regions of CPB1 and other genes encoding pancreatic secretory enzymes and known pancreatitis susceptibility genes (PRSS1, CPA1, CTRC, and SPINK1) in a hospital series of pancreatic cancer cases and controls. Variants in CPB1, CPA1 (encoding carboxypeptidase B1 and A1), and CTRC were evaluated in a second set of cases with familial pancreatic cancer and controls. More deleterious CPB1 variants, defined as having impaired protein secretion and induction of endoplasmic reticulum (ER) stress in transfected HEK 293T cells, were found in the hospital series of pancreatic cancer cases (5/986, 0.5%) than in controls (0/1,045, P = 0.027). Among familial pancreatic cancer cases, ER stress-inducing CPB1 variants were found in 4 of 593 (0.67%) vs. 0 of 967 additional controls (P = 0.020), with a combined prevalence in pancreatic cancer cases of 9/1,579 vs. 0/2,012 controls (P < 0.01). More ER stress-inducing CPA1 variants were also found in the combined set of hospital and familial cases with pancreatic cancer than in controls [7/1,546 vs. 1/2,012; P = 0.025; odds ratio, 9.36 (95% CI, 1.15–76.02)]. Overall, 16 (1%) of 1,579 pancreatic cancer cases had an ER stress-inducing CPA1 or CPB1 variant, compared with 1 of 2,068 controls (P < 0.00001). No other candidate genes had statistically significant differences in variant prevalence between cases and controls. Our study indicates ER stress-inducing variants in CPB1 and CPA1 are associated with pancreatic cancer susceptibility and implicate ER stress in pancreatic acinar cells in pancreatic cancer development.

KW - CPA1

KW - CPB1

KW - ER stress

KW - Pancreatic cancer

KW - Pancreatitis

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Mutations in the pancreatic secretory enzymes CPA1 and CPB1 are associated with pancreatic cancer

Abstract

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