ESPE2023 Rapid Free Communications Growth and syndromes (to include Turner syndrome) (6 abstracts)
Molecular genetic diagnosis in children with Idiopathic Short Stature: Single Center Experience
Emrullah Arslan 1 , Aslı Ece Solmaz 2 , Enise Avci 3 , Hanife Gul Balkı 1 , Deniz Ozalp Kızılay 1 , Arzu Jalilova 1 , Eren Er 1 , Damla Goksen 1 , Samim Ozen 1 & Sukran Darcan 1
1Ege University Faculty of Medicine, Pediatric Endocrinology and Diabetes, Izmir, Turkey. 2Ege University Faculty of Medicine, Department of Medical Genetic, Izmir, Turkey. 3Ege University Faculty of Medicine, Department of Pediatric Genetic, Izmir, Turkey
Introduction: Idiopathic short stature(ISS) refers to children who are short because there is no identifiable defect in the growth hormone (GH)/insulin-like growth factor(IGF) axis and no other endocrine or genetic disorders. The genetic etiology of ISS in children was investigated in this study using targeted next-generation sequencing(NGS).
Method: Eighty patients with short stature of unknown etiology were included in the study. Variants in 23 genes associated with ISS were screened with a panel of targeted NGS.
Results: Aclinical variant was detected in46% of the patients (Group 1); of these, 6 (7.5%) pathogenic, 12 (15%) likely pathogenic, and 19 (24.0%) variants of uncertain significance (VUS), and 54% (Group 2) no variant detected. At the time of admission, height SDS of group 1 (-3.1±0.9) was lower than that of group 2 (-2.5±0.66) (p:0.004). While the rate of growth hormone use was 76% in group 1, it was 64% in group 2. In addition, the first-year of group 1 after growth hormone treatment was -2,7 (-3.1/-2), group 2 -2 (-2.48/-1.5) (p:0.01). The final height SDS of group1 was -2.25 (-2.9/-2.1), while it was -1.7 (-2.1/-1) lower than that of group 2 (p:0, 04). In the first year after treatment, IGF-1SDS was 1.56 (0.4/4) higher in group 1 and 0.64 (-0.8/1.8) higher than group 2 (p:0.018). Characteristics of variants classified as likely pathogenic/pathogenic are summarized in Table 1.
| Gene | Variant | Zygosity | ACGM | Clinic |
| FGFR3 | c.1620C>A | Het | Pathogenic | Hypochondroplasia |
| IFT57 | c.569T>C | Hom | Likely Pathogenic | Orofasiodigital Syndrome Type8 |
| ANKRD11 | c.1372C>T | Het | Pathogenic | KBG Syndrome |
| COL2A1 | c.2356-3C>G | Het | Likely Pathogenic | Spondyloepiphyseal Dysplasia Congenita |
| TRPV4 | c.838G>A | Het | Pathogenic | Spondylometaphyseal Dysplasia, Kozlowski Type |
| CSGALNACT1 | c.1151C>G | Hom | Likely Pathogenic | Mild Skeletal Dysplasia, Joint Looseness, Advanced Bone Age Syndrome |
| GYS2 | c.1451G>C | Hom | Pathogenic | Glycogen Storage Type0 |
| HMGA2 | c.30delG | Het | Likely Pathogenic | Silver Russell Syndrome |
| GHR | c.674A>G | Het | Likely Pathogenic | GH Resistance Tip2 |
| AIRD2 | c.5371_5372del | Het | Likely Pathogenic | Coffin Siris Syndrome |
| PCNT | c.8326C>T | Het | Pathogenic | Microcephalic Osteodysplastic Primordial Dwarfism Type2 |
| GLI2 | c.3799C>G | Het | Likely Pathogenic | Culler Jones Syndrome |
| FGFR2 | c.24+2T>G | Het | Likely Pathogenic | Apert Syndrome |
| ACAN | c.7122C>A | Het | Likely Pathogenic | Advanced Bone Age, Early Osteoarthrosis, Osteochondrosis Syndrome |
| PROKR2 | c.254G>A | Het | Likely Pathogenic | Pituitary Insufficiency |
| FBN1 | c.5351A>G | Het | Likely Pathogenic | Acromicric Dysplasia |
| FGFR3 | c.445+2_445+5del | Het | Likely Pathogenic | Hypochondroplasia |
| OBSL1 | c.1273dupA | Hom | Pathogenic | 3M Syndrome |
Conclusion: TargetedNGS panels can be used successfully to brighten the genetic cause in patients with idiopathic short stature.In patients with mild and heterogeneous clinical findings, the treatment andfollow-up of the cases can be managed more accurately with NGS panels and genetic diagnosis.
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