. 2023 Sep 4;12(10):e230029. doi: 10.1530/EC-23-0029
This work is licensed under a Table 5.
Comparison of targeted panel sequencing group (group TPS) and whole-exome sequencing group (group WES) in our cohort.
| Features | TPS (n = 92) | WES (n = 86) | P-value |
|---|---|---|---|
| Clinical manifestation | |||
| Age (years) | 8.00 (1.58, 12.00) | 8.67 (3.23, 11.79) | 0.808 |
| Micropenis, % | 50.00% | 63.95% | 0.060 |
| Cryptorchidism, % | 32.61% | 36.06% | 0.629 |
| Hypospadia, % | 19.57% | 15.12% | 0.434 |
| Genetic characteristics | |||
| Diagnosis rate, % (n/N) | 57.61% (53/92) | 40.70% (35/86) | 0.024a |
| Pathogenic mutation, % (n/N) | 39.68% (25/63) | 45.00% (18/40) | 0.594 |
| Likely pathogenic mutation, % (n/N) | 33.33% (21/63) | 37.50% (15/40) | 0.666 |
| VUS mutation, % (n/N) | 25.87% (18/63) | 15.00% (6/40) | 0.267 |
| De novo mutation, % (n/N) | 6.34% (4/63) | 32.50% (13/40) | 0.001a |
| Missense mutation, % (n/N) | 71.43% (45/63) | 72.50% (29/40) | 0.906 |
| Nonsense mutation, % (n/N) | 11.11% (7/63) | 5.00% (2/40) | 0.284 |
| Deletion mutation, % (n/N) | 15.87% (10/63) | 20.00% (8/40) | 0.591 |
Subjects between 2016 and 2018 (n = 92) underwent targeted gene panel sequencing (group TPS), those between 2019 and 2022 (n = 86) underwent whole-exome sequencing (group WES). We compared the characteristics of these two groups to both clinical phenotype and genetic degrees. *aSignificant difference between group TPS and group WES, P value by the Pearson Chi-square, P < 0.05 was considered statistically significant.
aSignificant difference between group TPS and group WES, P-value by the Pearson chi-square, P < .05 was considered statistically significant.