Renal Hypodysplasia/Aplasia Type 3 via the GREB1L Gene

Renal hypodysplasia/aplasia type 3 (RHDA3) is an autosomal dominant disorder characterized by unilateral or bilateral renal agenesis, renal aplasia, and/or multicystic kidneys due to abnormal kidney development (Sanna-Cherchi et al. 2017. PubMed ID: 29100090; De Tomasi et al. 2017. PubMed ID: 29100091; Brophy et al. 2017. PubMed ID: 28739660). Phenotypic expression is highly variable, even within families, and incomplete penetrance is evident. Lethal in utero or in the perinatal period, bilateral renal agenesis falls at the most severe end of the spectrum of congenital anomalies of the kidney and urinary tract (CAKUT). Living carriers present with variable urogenital abnormalities including unilateral kidney agenesis, vesicoureteral reflux, horseshoe kidney, ovarian agenesis and unicornuate uterus.

Renal hypodysplasia/aplasia type 3 (RHDA3) is an autosomal dominant disorder caused by defects in the GREB1L gene (Sanna-Cherchi et al. 2017. PubMed ID: 29100090; De Tomasi et al. 2017. PubMed ID: 29100091; Brophy et al. 2017. PubMed ID: 28739660). Incomplete penetrance is evident.

The protein encoded by GREB1L (growth regulation by estrogen in breast cancer 1-like, 31 coding exons) plays a major role in early metanephros and genital development. Documented pathogenic variants in GREB1L include truncating changes (nonsense, canonical splice variants and frame-shifting small deletion/insertions) and missense substitutions (Sanna-Cherchi et al. 2017. PubMed ID: 29100090; De Tomasi et al. 2017. PubMed ID: 29100091; Brophy et al. 2017. PubMed ID: 28739660). De novo pathogenic variants in GREB1L have been reported. No large deletions or duplications at GREB1L have been reported yet.

In a study of 183 unrelated families affected by congenital anomalies of kidney and urinary tract (CAKUT), 16 (8.7%) heterozygous pathogenic or suspected pathogenic variants in GREB1L were identified, 12 of which were found in 54 cases (25.8%) with bilateral kidney agenesis in this cohort (De Tomasi et al. 2017. PubMed ID: 29100091).

In another study of 612 individuals affected by renal agenesis and hypodysplasia (RHD), 17 (2.8%) heterozygous pathogenic or suspected pathogenic variants in GREB1L were identified (Sanna-Cherchi et al. 2017. PubMed ID: 29100090).

No large deletions or duplications at GREB1L have been reported yet.

This test provides full coverage of all coding exons of the GREB1L gene plus 10 bases of flanking noncoding DNA in all available transcripts along with other non-coding regions in which pathogenic variants have been identified at PreventionGenetics or reported elsewhere. We define full coverage as >20X NGS reads or Sanger sequencing. PGnome panels typically provide slightly increased coverage over the PGxome equivalent. PGnome sequencing panels have the added benefit of additional analysis and reporting of deep intronic regions (where applicable).

Dependent on the sequencing backbone selected for this testing, discounted reflex testing to any other similar backbone-based test is available (i.e., PGxome panel to whole PGxome; PGnome panel to whole PGnome).