Objective: It is aimed to point out the importance of advanced genetic testing in fetuses with cystic hygroma. Case: A pregnant woman aged 33 years, G1P0, 20 weeks and 5 days referred to us from an external center was evaluated. She had chorionic villus sampling because of a cystic hygroma seen in the first trimester sonographic screening. Fetal karyotype and microarray analysis results had been reported as normal so a genetic mutation panel had been studied for Noonan syndrome. Pathogenic missence variant was found in PTPN11 gene and pathogenic splice acceptor variant in MYBPC3 gene. The ultrasonographic findings were thought to be related to the heterozygous pathogenic variant detected in the PTPN11 gene. In the ultrasonographic evaluation of the fetus, it was observed that the nuchal fold was 8.7 mm, with septation and cystic appearance, and the lower poles of the fetal kidneys merged at the level of the aortic bifurcation. Fetal gender was female. Fetal echocardiography revealed subvalvular aortic stenosis. By reason of clinical findings and genetic examination results were thought to be compatible with the autosomal inherited Noonan syndrome, termination of pregnancy was offered to the family by the perinatology council. The family accepted the option of termination of pregnancy. Discussion: Noonan syndrome is a common autosomal-dominant condition clinically and genetically heterogeneous and two-thirds of patients are the first affected person in their family due to a de novo pathogenic variant. Although so many gene mutations are described for this syndrome, approximately %50 of patients have a pathogenic variant in protein tyrosine phosphatase, nonreceptor type 11 (PTPN11).[1] Fetuses with Noonan syndrome may present with manifestations of disordered lymphatic development, which include most commonly increased nuchal translucency. Renal and valvular cardiac anomalies may represent, too.[2] Clinical features such as difficulties with feeding in early life; vision, hearing, and growth problems; specific learning difficulties may develop in the postnatal period. Conclusion: Even if fetal karyotyping is normal in cystic hygroma cases detected in the first trimester screening, it should be kept in mind that genetic mutations that may accompany related syndromes may also be present. [ABSTRACT FROM AUTHOR]