MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.

It remains challenging to produce decisive vaccines against MUC1, a tumor-associated antigen widely expressed by pancreas, breast and other tumors. Employing clinically relevant mouse models, we ruled out such causes as irreversible T-cell tolerance, inadequate avidity, and failure of T-cells to rec...

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Main Authors: Vani Lakshminarayanan, Nitin T Supekar, Jie Wei, Dustin B McCurry, Amylou C Dueck, Heidi E Kosiorek, Priyanka P Trivedi, Judy M Bradley, Cathy S Madsen, Latha B Pathangey, Dominique B Hoelzinger, Margreet A Wolfert, Geert-Jan Boons, Peter A Cohen, Sandra J Gendler
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2016-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4720451?pdf=render
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spelling doaj-5edccc34d6f44f97817a482f300515032020-11-25T02:31:45ZengPublic Library of Science (PLoS)PLoS ONE1932-62032016-01-01111e014592010.1371/journal.pone.0145920MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.Vani LakshminarayananNitin T SupekarJie WeiDustin B McCurryAmylou C DueckHeidi E KosiorekPriyanka P TrivediJudy M BradleyCathy S MadsenLatha B PathangeyDominique B HoelzingerMargreet A WolfertGeert-Jan BoonsPeter A CohenSandra J GendlerIt remains challenging to produce decisive vaccines against MUC1, a tumor-associated antigen widely expressed by pancreas, breast and other tumors. Employing clinically relevant mouse models, we ruled out such causes as irreversible T-cell tolerance, inadequate avidity, and failure of T-cells to recognize aberrantly glycosylated tumor MUC1. Instead, every tested MUC1 preparation, even non-glycosylated synthetic 9mer peptides, induced interferon gamma-producing CD4(+) and CD8(+) T-cells that recognized glycosylated variants including tumor-associated MUC1. Vaccination with synthetic peptides conferred protection as long as vaccination was repeated post tumor challenge. Failure to revaccinate post challenge was associated with down-regulated tumor MUC1 and MHC molecules. Surprisingly, direct admixture of MUC1-expressing tumor with MUC1-hyperimmune T-cells could not prevent tumor outgrowth or MUC1 immunoediting, whereas ex vivo activation of the hyperimmune T-cells prior to tumor admixture rendered them curative. Therefore, surrogate T-cell preactivation outside the tumor bed, either in culture or by repetitive vaccination, can overcome tumor escape.http://europepmc.org/articles/PMC4720451?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Vani Lakshminarayanan
Nitin T Supekar
Jie Wei
Dustin B McCurry
Amylou C Dueck
Heidi E Kosiorek
Priyanka P Trivedi
Judy M Bradley
Cathy S Madsen
Latha B Pathangey
Dominique B Hoelzinger
Margreet A Wolfert
Geert-Jan Boons
Peter A Cohen
Sandra J Gendler
spellingShingle Vani Lakshminarayanan
Nitin T Supekar
Jie Wei
Dustin B McCurry
Amylou C Dueck
Heidi E Kosiorek
Priyanka P Trivedi
Judy M Bradley
Cathy S Madsen
Latha B Pathangey
Dominique B Hoelzinger
Margreet A Wolfert
Geert-Jan Boons
Peter A Cohen
Sandra J Gendler
MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
PLoS ONE
author_facet Vani Lakshminarayanan
Nitin T Supekar
Jie Wei
Dustin B McCurry
Amylou C Dueck
Heidi E Kosiorek
Priyanka P Trivedi
Judy M Bradley
Cathy S Madsen
Latha B Pathangey
Dominique B Hoelzinger
Margreet A Wolfert
Geert-Jan Boons
Peter A Cohen
Sandra J Gendler
author_sort Vani Lakshminarayanan
title MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
title_short MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
title_full MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
title_fullStr MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
title_full_unstemmed MUC1 Vaccines, Comprised of Glycosylated or Non-Glycosylated Peptides or Tumor-Derived MUC1, Can Circumvent Immunoediting to Control Tumor Growth in MUC1 Transgenic Mice.
title_sort muc1 vaccines, comprised of glycosylated or non-glycosylated peptides or tumor-derived muc1, can circumvent immunoediting to control tumor growth in muc1 transgenic mice.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2016-01-01
description It remains challenging to produce decisive vaccines against MUC1, a tumor-associated antigen widely expressed by pancreas, breast and other tumors. Employing clinically relevant mouse models, we ruled out such causes as irreversible T-cell tolerance, inadequate avidity, and failure of T-cells to recognize aberrantly glycosylated tumor MUC1. Instead, every tested MUC1 preparation, even non-glycosylated synthetic 9mer peptides, induced interferon gamma-producing CD4(+) and CD8(+) T-cells that recognized glycosylated variants including tumor-associated MUC1. Vaccination with synthetic peptides conferred protection as long as vaccination was repeated post tumor challenge. Failure to revaccinate post challenge was associated with down-regulated tumor MUC1 and MHC molecules. Surprisingly, direct admixture of MUC1-expressing tumor with MUC1-hyperimmune T-cells could not prevent tumor outgrowth or MUC1 immunoediting, whereas ex vivo activation of the hyperimmune T-cells prior to tumor admixture rendered them curative. Therefore, surrogate T-cell preactivation outside the tumor bed, either in culture or by repetitive vaccination, can overcome tumor escape.
url http://europepmc.org/articles/PMC4720451?pdf=render
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