Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans

Pervinder Sagoo; Esperanza Perucha; Birgit Sawitzki; Stefan Tomiuk; David A. Stephens; Patrick Miqueu; Stephanie Chapman; Ligia Craciun; Ruhena Sergeant; Sophie Brouard; Flavia Rovis; Elvira Jimenez; Amany Ballow; Magali Giral; Irene Rebollo-mesa; Alain Le Moine; Cecile Braudeau; Rachel Hilton; Bernhard Gerstmayer; Katarzyna Bourcier; Adnan Sharif; Magdalena Krajewska; Graham M. Lord; Ian Roberts; Michel Goldman; Kathryn J. Wood; Kenneth Newell; Vicki Seyfert-margolis; Anthony N. Warrens; Uwe Janssen; Hans-dieter Volk; Jean-paul Soulillou; Maria P. Hernandez-fuentes; Robert I. Lechler

doi:10.1172/JCI39922

Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans

Pervinder Sagoo, Esperanza Perucha, Birgit Sawitzki, Stefan Tomiuk, David A. Stephens, Patrick Miqueu, Stephanie Chapman, Ligia Craciun, Ruhena Sergeant, Sophie Brouard, Flavia Rovis, Elvira Jimenez, Amany Ballow, Magali Giral, Irene Rebollo-mesa, Alain Le Moine, Cecile Braudeau, Rachel Hilton, Bernhard Gerstmayer, Katarzyna BourcierAdnan Sharif, Magdalena Krajewska, Graham M. Lord, Ian Roberts, Michel Goldman, Kathryn J. Wood, Kenneth Newell, Vicki Seyfert-margolis, Anthony N. Warrens, Uwe Janssen, Hans-dieter Volk, Jean-paul Soulillou, Maria P. Hernandez-fuentes, Robert I. Lechler

FBMH Faculty Office Administration (L5)

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

Abstract

Identifying transplant recipients in whom immunological tolerance is established or is developing would allow an individually tailored approach to their posttransplantation management. In this study, we aimed to develop reliable and reproducible in vitro assays capable of detecting tolerance in renal transplant recipients. Several biomarkers and bioassays were screened on a training set that included 11 operationally tolerant renal transplant recipients, recipient groups following different immunosuppressive regimes, recipients undergoing chronic rejection, and healthy controls. Highly predictive assays were repeated on an independent test set that included 24 tolerant renal transplant recipients. Tolerant patients displayed an expansion of peripheral blood B and NK lymphocytes, fewer activated CD4+ T cells, a lack of donor-specific antibodies, donor-specific hyporesponsiveness of CD4+ T cells, and a high ratio of forkhead box P3 to α-1,2-mannosidase gene expression. Microarray analysis further revealed in tolerant recipients a bias toward differential expression of B cell–related genes and their associated molecular pathways. By combining these indices of tolerance as a cross-platform biomarker signature, we were able to identify tolerant recipients in both the training set and the test set. This study provides an immunological profile of the tolerant state that, with further validation, should inform and shape drug-weaning protocols in renal transplant recipients.

Original language	English
Pages (from-to)	1848-1861
Journal	Journal of Clinical Investigation
Volume	120
Issue number	6
DOIs	https://doi.org/10.1172/JCI39922
Publication status	Published - 1 Jun 2010

Access to Document

10.1172/JCI39922

http://www.jci.org/articles/view/39922

Cite this

Sagoo, P., Perucha, E., Sawitzki, B., Tomiuk, S., Stephens, D. A., Miqueu, P., Chapman, S., Craciun, L., Sergeant, R., Brouard, S., Rovis, F., Jimenez, E., Ballow, A., Giral, M., Rebollo-mesa, I., Le Moine, A., Braudeau, C., Hilton, R., Gerstmayer, B., ... Lechler, R. I. (2010). Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans. Journal of Clinical Investigation, 120(6), 1848-1861. https://doi.org/10.1172/JCI39922

@article{97a79f8c16a448de823f0a9f04a675b2,

title = "Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans",

abstract = "Identifying transplant recipients in whom immunological tolerance is established or is developing would allow an individually tailored approach to their posttransplantation management. In this study, we aimed to develop reliable and reproducible in vitro assays capable of detecting tolerance in renal transplant recipients. Several biomarkers and bioassays were screened on a training set that included 11 operationally tolerant renal transplant recipients, recipient groups following different immunosuppressive regimes, recipients undergoing chronic rejection, and healthy controls. Highly predictive assays were repeated on an independent test set that included 24 tolerant renal transplant recipients. Tolerant patients displayed an expansion of peripheral blood B and NK lymphocytes, fewer activated CD4+ T cells, a lack of donor-specific antibodies, donor-specific hyporesponsiveness of CD4+ T cells, and a high ratio of forkhead box P3 to α-1,2-mannosidase gene expression. Microarray analysis further revealed in tolerant recipients a bias toward differential expression of B cell–related genes and their associated molecular pathways. By combining these indices of tolerance as a cross-platform biomarker signature, we were able to identify tolerant recipients in both the training set and the test set. This study provides an immunological profile of the tolerant state that, with further validation, should inform and shape drug-weaning protocols in renal transplant recipients.",

author = "Pervinder Sagoo and Esperanza Perucha and Birgit Sawitzki and Stefan Tomiuk and Stephens, {David A.} and Patrick Miqueu and Stephanie Chapman and Ligia Craciun and Ruhena Sergeant and Sophie Brouard and Flavia Rovis and Elvira Jimenez and Amany Ballow and Magali Giral and Irene Rebollo-mesa and {Le Moine}, Alain and Cecile Braudeau and Rachel Hilton and Bernhard Gerstmayer and Katarzyna Bourcier and Adnan Sharif and Magdalena Krajewska and Lord, {Graham M.} and Ian Roberts and Michel Goldman and Wood, {Kathryn J.} and Kenneth Newell and Vicki Seyfert-margolis and Warrens, {Anthony N.} and Uwe Janssen and Hans-dieter Volk and Jean-paul Soulillou and Hernandez-fuentes, {Maria P.} and Lechler, {Robert I.}",

year = "2010",

month = jun,

day = "1",

doi = "10.1172/JCI39922",

language = "English",

volume = "120",

pages = "1848--1861",

journal = "Journal of Clinical Investigation",

issn = "0021-9738",

publisher = "American Society for Clinical Investigation",

number = "6",

}

Sagoo, P, Perucha, E, Sawitzki, B, Tomiuk, S, Stephens, DA, Miqueu, P, Chapman, S, Craciun, L, Sergeant, R, Brouard, S, Rovis, F, Jimenez, E, Ballow, A, Giral, M, Rebollo-mesa, I, Le Moine, A, Braudeau, C, Hilton, R, Gerstmayer, B, Bourcier, K, Sharif, A, Krajewska, M, Lord, GM, Roberts, I, Goldman, M, Wood, KJ, Newell, K, Seyfert-margolis, V, Warrens, AN, Janssen, U, Volk, H, Soulillou, J, Hernandez-fuentes, MP & Lechler, RI 2010, 'Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans', Journal of Clinical Investigation, vol. 120, no. 6, pp. 1848-1861. https://doi.org/10.1172/JCI39922

TY - JOUR

T1 - Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans

AU - Sagoo, Pervinder

AU - Perucha, Esperanza

AU - Sawitzki, Birgit

AU - Tomiuk, Stefan

AU - Stephens, David A.

AU - Miqueu, Patrick

AU - Chapman, Stephanie

AU - Craciun, Ligia

AU - Sergeant, Ruhena

AU - Brouard, Sophie

AU - Rovis, Flavia

AU - Jimenez, Elvira

AU - Ballow, Amany

AU - Giral, Magali

AU - Rebollo-mesa, Irene

AU - Le Moine, Alain

AU - Braudeau, Cecile

AU - Hilton, Rachel

AU - Gerstmayer, Bernhard

AU - Bourcier, Katarzyna

AU - Sharif, Adnan

AU - Krajewska, Magdalena

AU - Lord, Graham M.

AU - Roberts, Ian

AU - Goldman, Michel

AU - Wood, Kathryn J.

AU - Newell, Kenneth

AU - Seyfert-margolis, Vicki

AU - Warrens, Anthony N.

AU - Janssen, Uwe

AU - Volk, Hans-dieter

AU - Soulillou, Jean-paul

AU - Hernandez-fuentes, Maria P.

AU - Lechler, Robert I.

PY - 2010/6/1

Y1 - 2010/6/1

N2 - Identifying transplant recipients in whom immunological tolerance is established or is developing would allow an individually tailored approach to their posttransplantation management. In this study, we aimed to develop reliable and reproducible in vitro assays capable of detecting tolerance in renal transplant recipients. Several biomarkers and bioassays were screened on a training set that included 11 operationally tolerant renal transplant recipients, recipient groups following different immunosuppressive regimes, recipients undergoing chronic rejection, and healthy controls. Highly predictive assays were repeated on an independent test set that included 24 tolerant renal transplant recipients. Tolerant patients displayed an expansion of peripheral blood B and NK lymphocytes, fewer activated CD4+ T cells, a lack of donor-specific antibodies, donor-specific hyporesponsiveness of CD4+ T cells, and a high ratio of forkhead box P3 to α-1,2-mannosidase gene expression. Microarray analysis further revealed in tolerant recipients a bias toward differential expression of B cell–related genes and their associated molecular pathways. By combining these indices of tolerance as a cross-platform biomarker signature, we were able to identify tolerant recipients in both the training set and the test set. This study provides an immunological profile of the tolerant state that, with further validation, should inform and shape drug-weaning protocols in renal transplant recipients.

AB - Identifying transplant recipients in whom immunological tolerance is established or is developing would allow an individually tailored approach to their posttransplantation management. In this study, we aimed to develop reliable and reproducible in vitro assays capable of detecting tolerance in renal transplant recipients. Several biomarkers and bioassays were screened on a training set that included 11 operationally tolerant renal transplant recipients, recipient groups following different immunosuppressive regimes, recipients undergoing chronic rejection, and healthy controls. Highly predictive assays were repeated on an independent test set that included 24 tolerant renal transplant recipients. Tolerant patients displayed an expansion of peripheral blood B and NK lymphocytes, fewer activated CD4+ T cells, a lack of donor-specific antibodies, donor-specific hyporesponsiveness of CD4+ T cells, and a high ratio of forkhead box P3 to α-1,2-mannosidase gene expression. Microarray analysis further revealed in tolerant recipients a bias toward differential expression of B cell–related genes and their associated molecular pathways. By combining these indices of tolerance as a cross-platform biomarker signature, we were able to identify tolerant recipients in both the training set and the test set. This study provides an immunological profile of the tolerant state that, with further validation, should inform and shape drug-weaning protocols in renal transplant recipients.

U2 - 10.1172/JCI39922

DO - 10.1172/JCI39922

M3 - Article

SN - 0021-9738

VL - 120

SP - 1848

EP - 1861

JO - Journal of Clinical Investigation

JF - Journal of Clinical Investigation

IS - 6

ER -

Development of a cross-platform biomarker signature to detect renal transplant tolerance in humans

Abstract

Access to Document

Fingerprint

Cite this