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Multicenter Study
. 2021 Mar;99(3):737-749.
doi: 10.1016/j.kint.2020.06.043. Epub 2020 Aug 1.

Amniotic fluid peptides predict postnatal kidney survival in developmental kidney disease

Julie Klein  1 Bénédicte Buffin-Meyer  1 Franck Boizard  1 Nabila Moussaoui  1 Ophélie Lescat  1 Benjamin Breuil  1 Camille Fedou  1 Guylène Feuillet  1 Audrey Casemayou  1 Eric Neau  1 An Hindryckx  2 Luc Decatte  2 Elena Levtchenko  3 Anke Raaijmakers  3 Christophe Vayssière  4 Valérie Goua  5 Charlotte Lucas  6 Franck Perrotin  7 Sylvie Cloarec  8 Alexandra Benachi  9 Marie-Christine Manca-Pellissier  10 Hélène Laurichesse Delmas  11 Lucie Bessenay  12 Claudine Le Vaillant  13 Emma Allain-Launay  14 Jean Gondry  15 Bernard Boudailliez  16 Elisabeth Simon  17 Fabienne Prieur  18 Marie-Pierre Lavocat  19 Anne-Hélène Saliou  20 Loic De Parscau  21 Laurent Bidat  22 Catherine Noel  22 Corinne Floch  23 Guylène Bourdat-Michel  24 Romain Favre  25 Anne-Sophie Weingertner  25 Jean-François Oury  26 Véronique Baudouin  27 Jean-Paul Bory  28 Christine Pietrement  29 Maryse Fiorenza  30 Jérôme Massardier  31 Sylvie Kessler  32 Nadia Lounis  33 Françoise Conte Auriol  33 Pascale Marcorelles  34 Sophie Collardeau-Frachon  35 Petra Zürbig  36 Harald Mischak  37 Pedro Magalhães  38 Julie Batut  39 Patrick Blader  39 Jean-Sebastien Saulnier Blache  1 Jean-Loup Bascands  40 Franz Schaefer  41 Stéphane Decramer  42 Joost P Schanstra  43 BIOMAN consortium
Collaborators, Affiliations
Free article
Multicenter Study

Amniotic fluid peptides predict postnatal kidney survival in developmental kidney disease

Julie Klein et al. Kidney Int. 2021 Mar.
Free article

Abstract

Although a rare disease, bilateral congenital anomalies of the kidney and urinary tract (CAKUT) are the leading cause of end stage kidney disease in children. Ultrasound-based prenatal prediction of postnatal kidney survival in CAKUT pregnancies is far from accurate. To improve prediction, we conducted a prospective multicenter peptidome analysis of amniotic fluid spanning 140 evaluable fetuses with CAKUT. We identified a signature of 98 endogenous amniotic fluid peptides, mainly composed of fragments from extracellular matrix proteins and from the actin binding protein thymosin-β4. The peptide signature predicted postnatal kidney outcome with an area under the curve of 0.96 in the holdout validation set of patients with CAKUT with definite endpoint data. Additionally, this peptide signature was validated in a geographically independent sub-cohort of 12 patients (area under the curve 1.00) and displayed high specificity in non-CAKUT pregnancies (82 and 94% in 22 healthy fetuses and in 47 fetuses with congenital cytomegalovirus infection respectively). Change in amniotic fluid thymosin-β4 abundance was confirmed with ELISA. Knockout of thymosin-β4 in zebrafish altered proximal and distal tubule pronephros growth suggesting a possible role of thymosin β4 in fetal kidney development. Thus, recognition of the 98-peptide signature in amniotic fluid during diagnostic workup of prenatally detected fetuses with CAKUT can provide a long-sought evidence base for accurate management of the CAKUT disorder that is currently unavailable.

Keywords: amniotic fluid; congenital anomalies of the kidney and the urinary tract; infants; management; peptides; prediction; termination of pregnancy.

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