TY - JOUR AU - Hadi, Nisa Ayu Thayalisha AU - Utari, Agustini AU - Sihombing, Nydia Rena Benita AU - Winarni, Tri Indah AU - Maharani, Nani PY - 2026 DA - 2026/05/06 TI - Clinical Variabilities of <i>PTPN11</i> Pathogenic Variant in Indonesian Noonan Syndrome Patients JO - OBM Genetics SP - 338 VL - 10 IS - 02 AB - Noonan syndrome (NS) is an autosomal dominant disorder with a wide spectrum of symptoms and clinical phenotypes, including short stature, congenital heart defects (CHD), and distinctive facial features. A pathogenic variant in the PTPN11 gene is the major cause of NS. This is a preliminary study in Indonesia involving 29 patients with clinical features of NS. Detailed clinical and echocardiography data were collected. Genomic DNA was extracted from a peripheral blood sample. Exome sequencing or PCR followed by Sanger DNA sequencing was done. Variant pathogenicity was assessed using the ClinVar database, while the novel variant was analyzed in silico using PolyPhen, Rare Exome Variant Ensemble Learner (REVEL), SIFT, FATHMM Pred, and MutationTaster. Clinical findings in 18 patients showed a typical craniofacial feature of NS, including low-posteriorly rotated ear (83.3%), microcephaly, downslanted palpebral fissures, and a short-webbed neck in 50%, and hypertelorism and a depressed nasal bridge in 44.4%. Other clinical variabilities included CHD (83.3%), thoracic and musculoskeletal deformities (77.8%), short stature (72.2%), and intellectual disability (ID) (50%). A novel variant in exon 3 of PTPN11 was found in one patient: c.140G>A (p.Arg47Lys), which was predicted to be probably damaging. A variant in exon 8, the c.907G>A (p.Asp303Asn), was found in 11 patients. This variant is not in the ClinVar database yet; however, it was reported in a case report and predicted to be probably damaging. One patient has a variant c.184T>G (p.Tyr62Asp), 1 patient has c.854T>C (p.Phe285Ser), 1 patient has c.922A>G (p.Asn308Asp), 2 patients have c.1510A>G (p.Met504Val), and 1 patient has c.1517A>C (p.Gln506Pro), those variants have been previously reported. Sequencing on the remaining exons of PTPN11 is still ongoing. NS patients with PTPN11 variants demonstrate diverse clinical manifestations. Clinicians’ awareness of suspecting NS is essential for early diagnosis, particularly in children with short stature, ID, and CHD who have a distinctive facial dysmorphism at any age. SN - 2577-5790 UR - https://doi.org/10.21926/obm.genet.2602338 DO - 10.21926/obm.genet.2602338 ID - Hadi2026 ER -