Analysis of independent microarray datasets of renal biopsies identifies a robust transcript signature of acute allograft rejection

Saint-Mézard, Pierre; Berthier, Céline C.; Zhang, Hai; Hertig, Alexandre; Kaiser, Sérgio; Schumacher, M.; Wieczorek, Grazyna; Bigaud, Marc; Kehren, Jeanne; Rondeau, Éric; Raulf, Friedrich; Marti, Hans-Peter

doi:10.1111/j.1432-2277.2008.00790.x

Cited by 79 publications

(86 citation statements)

References 18 publications

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“…Second, we found that IFϩi was associated with upregulation of immune/ inflammatory pathways linked with acute cellular rejection. [17][18][19][20][21][22][23] The results lend credence to the view that early surveillance histology with or without targeted molecular analysis provides important prognostic information. 10,24 They also suggest that analysis of intragraft innate and adaptive immune pathways during early posttransplantation years 25 may provide the basis for interventions to subvert chronic deterioration in a subset of recipients with clinical expectations of excellent long-term outcome.…”

mentioning

confidence: 53%

“…22,23 Most striking, gene expression signatures associated with cytotoxic T lymphocytes, IFN-␥ response, B cells, and acute rejection were heavily enriched in IFϩi compared with normal and IF-alone groups (Supplemental Tables S2 and S3). Microarrays were also carried out on T4 biopsies from the three groups and were compared in a paired manner with the results of T12 microarrays to determine expression changes over time of acute rejection-associated genes.…”

Section: Ihc Targeted Molecular Profiling and Microarray Analysesmentioning

confidence: 99%

“…Microarrays were also carried out on T4 biopsies from the three groups and were compared in a paired manner with the results of T12 microarrays to determine expression changes over time of acute rejection-associated genes. 23 Between T4 and T12, only the IFϩi group demonstrated altered expression of a substantial proportion (38%) of the acute rejection-associated genes (Supplemental Table S3). Finally, we sought to determine whether the biological responses of renal parenchymal cells could be distinguished from those of infiltrating leukocytes.…”

Section: Ihc Targeted Molecular Profiling and Microarray Analysesmentioning

confidence: 99%

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Fibrosis with Inflammation at One Year Predicts Transplant Functional Decline

Park

Griffin

Cornell³

et al. 2010

Journal of the American Society of Nephrology

196

168

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Lack of knowledge regarding specific causes for late loss of kidney transplants hampers improvements in long-term allograft survival. Kidney transplants with both interstitial fibrosis and subclinical inflammation but not fibrosis alone after 1 year have reduced survival. This study tested whether fibrosis with inflammation at 1 year associates with decline of renal function in a low-risk cohort and characterized the nature of the inflammation. We studied 151 living-donor, tacrolimus/mycophenolate-treated recipients without overt risk factors for reduced graft survival. Transplants with normal histology (n ϭ 86) or fibrosis alone (n ϭ 45) on 1-year protocol biopsy had stable renal function between 1 and 5 years, whereas those with both fibrosis and inflammation (n ϭ 20) exhibited a decline in GFR and reduced graft survival. Immunohistochemistry confirmed increased interstitial T cells and macrophages/dendritic cells in the group with both fibrosis and inflammation, and there was increased expression of transcripts related to innate and cognate immunity. Pathway-and pathologic process-specific analyses of microarray profiles revealed that potentially damaging immunologic activities were enriched among the overexpressed transcripts (e.g., Toll-like receptor signaling, antigen presentation/dendritic cell maturation, IFN-␥-inducible response, cytotoxic T lymphocyte-associated and acute rejection-associated genes). Therefore, the combination of fibrosis and inflammation in 1-year protocol biopsies associates with reduced graft function and survival as well as a rejection-like gene expression signature, even among recipients with no clinical risk factors for poor outcomes. Early interventions aimed at altering rejection-like inflammation may improve long-term survival of kidney allografts.

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mentioning

confidence: 53%

Section: Ihc Targeted Molecular Profiling and Microarray Analysesmentioning

confidence: 99%

Section: Ihc Targeted Molecular Profiling and Microarray Analysesmentioning

confidence: 99%

See 1 more Smart Citation

Fibrosis with Inflammation at One Year Predicts Transplant Functional Decline

Park

Griffin

Cornell³

et al. 2010

Journal of the American Society of Nephrology

196

168

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“…While many investigators have analyzed molecular changes in biopsies with histologic rejection, using either RT-PCR (17,18) or microarrays (19)(20)(21), these studies failed to distinguish TCMR from antibody-mediated rejection (ABMR), in part because the criteria for diagnosing ABMR, particularly C4d-negative ABMR, are evolving and remain controversial (22,23). Because of this, we established the Alberta Transplant Applied Genomics Centre (ATAGC) Reference Standard histology system (http://atagc.med.ualberta.ca/) in a prospective cohort of 403 indication biopsies (the BFC403 cohort).…”

Section: Introductionmentioning

confidence: 99%

Potential Impact of Microarray Diagnosis of T Cell–Mediated Rejection in Kidney Transplants: The INTERCOM Study

Halloran

Pereira

Chang

et al. 2013

American Journal of Transplantation

113

121

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We previously developed a microarray-based test for T cell-mediated rejection (TCMR) in a reference set of 403 biopsies. To determine the potential impact of this test in clinical practice, we undertook INTERCOM, a prospective international study of 300 indication biopsies from 264 patients (ClinicalTrials.gov NCT01299168). Biopsies from six centers-Baltimore, Barcelona, Edmonton, Hannover, Manchester and Minneapolis-were analyzed by microarrays, assigning TCMR scores by an algorithm developed in the reference set and comparing TCMR scores to local histology assessment. The TCMR score correlated with histologic TCMR lesions-tubulitis and interstitial infiltration. The accuracy for primary histologic diagnoses (0.87) was similar to the reference set (0.89). The TCMR scores reclassified 77/300 biopsies (26%): 16 histologic TCMR were molecularly non-TCMR; 15 histologic non-TCMR were molecularly TCMR, including 6 with polyoma virus nephropathy; and all 46 ''borderline'' biopsies were reclassified as TCMR (8) or non-TCMR (38). Like the reference set, discrepancies were primarily in situations where histology has known limitations, for example, in biopsies with scarring and inflammation/tubulitis potentially from other diseases. Neither the TCMR score nor histologic TCMR was associated with graft loss. Thus the molecular TCMR score has potential to add new insight, particularly in situations where histology is ambiguous or potentially misleading.

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“…Nephrology researchers have begun to employ these innovative high-throughput procedures to identify the whole basal expression profile of normal or pathological human kidney [100], to select biomarkers predicting acute and chronic allograft outcomes [101,102] and to assess more clearly the intricate molecular pathways associated to the pathogenesis and onset of several immunological renal diseases [103,104]. On the contrary, only few reports to date have been published describing the multi-genetic influence on drug response in nephrology.…”

Section: Pharmacogenomics and Immunosuppressive Drugs Used In Clinicamentioning

confidence: 99%

Pharmacogenomics: a new paradigm to personalize treatments in nephrology patients

Zaza

Granata

Sallustio

et al. 2009

Clinical and Experimental Immunology

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SummaryAlthough notable progress has been made in the therapeutic management of patients with chronic kidney disease in both conservative and renal replacement treatments (dialysis and transplantation), the occurrence of medication-related problems (lack of efficacy, adverse drug reactions) still represents a key clinical issue. Recent evidence suggests that adverse drug reactions are major causes of death and hospital admission in Europe and the United States. The reasons for these conditions are represented by environmental/non-genetic and genetic factors responsible for the great inter-patient variability in drugs metabolism, disposition and therapeutic targets. Over the years several genetic settings have been linked, using pharmacogenetic approaches, to the effects and toxicity of many agents used in clinical nephrology. However, these strategies, analysing single gene or candidate pathways, do not represent the gold standard, being the overall pharmacological effects of medications and not typically monogenic traits. Therefore, to identify multi-genetic influence on drug response, researchers and clinicians from different fields of medicine and pharmacology have started to perform pharmacogenomic studies employing innovative whole genomic high-throughput technologies. However, to date, only few pharmacogenomics reports have been published in nephrology underlying the need to enhance the number of projects and to increase the research budget for this important research field. In the future we would expect that, applying the knowledge about an individual's inherited response to drugs, nephrologists will be able to prescribe medications based on each person's genetic make-up, to monitor carefully the efficacy/toxicity of a given drug and to modify the dosage or number of medications to obtain predefined clinical outcomes.

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Analysis of independent microarray datasets of renal biopsies identifies a robust transcript signature of acute allograft rejection

Cited by 79 publications

References 18 publications

Fibrosis with Inflammation at One Year Predicts Transplant Functional Decline

Fibrosis with Inflammation at One Year Predicts Transplant Functional Decline

Potential Impact of Microarray Diagnosis of T Cell–Mediated Rejection in Kidney Transplants: The INTERCOM Study

Pharmacogenomics: a new paradigm to personalize treatments in nephrology patients

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