Kayhan, GülsümKazan, Hasan HüseyinÖztürk, KübraSezer, AbdullahPerçin, Ferda2025-02-242025-02-2420222147-929110.5336/caserep.2022-89352https://doi.org/10.5336/caserep.2022-89352https://search.trdizin.gov.tr/tr/yayin/detay/1167323https://hdl.handle.net/20.500.14440/354Auriculocondylar syndrome is a rare autosomal dominant or recessive disorder characterized by question-mark ears, a small mandibular condyle, and micrognathia. From a molecular perspective, auriculocondylar syndrome arises due to mutations in the PLCB4, GNAI3, and EDN1 genes that play roles in the endothelin signaling pathway. Here, we report a patient with findings of auriculocondylar syndrome and an additional mild intellectual disability. The patient’s whole exome sequencing analyses revealed a novel homozygous frameshif t mutation in the PLCB4 gene related to auriculocondylar syndrome Type 2. Our molecular studies indicated that this mutation caused a downreg ulation of PLCB4. This type of PLCB4 mutation has seldom been reported in auriculocondylar syndrome-2 patients and only 2 of them have hadneurode- velopmental anomalies, as in our patient. We think that this study supports the possibility of intellectual disability in indiv iduals with a ho- mozygous truncating variant in the PLCB4 gene and contributes to the literature.eninfo:eu-repo/semantics/openAccessNörolojik BilimlerPediatriArticle2624258116732330