Evaluation of the Clinical and Genetic Characteristics of Primary Ciliary Dyskinesia Patients With Situs Inversus Totalis

被引:0
|
作者
Kahraman, Feyza Ustabas [1 ]
Jafarov, Uzeyir [2 ]
Yazan, Hakan [3 ]
Yurtsever, Ismail [4 ]
Cakir, Erkan [5 ]
Sayin, Gozde Yesil [6 ]
机构
[1] Istanbul Medipol Univ, Medipol Mega Hosp, Dept Child Hlth & Dis, Istanbul, Turkiye
[2] Avrasya Hosp, Dept Child Hlth & Dis, Istanbul, Turkiye
[3] Istanbul Medipol Univ, Medipol Mega Hosp, Dept Pediat Pulmonol, Istanbul, Turkiye
[4] Bezmialem Vakif Univ, Vocat Sch Hlth Serv, Dept Med Serv & Tech, Med Imaging Tech Program, Istanbul, Turkiye
[5] Istinye Univ, Dept Pediat Pulmonol, Liv Hosp, Istanbul, Turkiye
[6] Istanbul Univ, Fac Med, Dept Med Genet, Istanbul, Turkiye
来源
BIRTH DEFECTS RESEARCH | 2025年 / 117卷 / 02期
关键词
genetic testing; PICADAR; primary ciliary dyskinesia; situs inversus; DIAGNOSIS; FEATURES; AGE;
D O I
10.1002/bdr2.2444
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
BackgroundSitus inversus totalis (SIT) is present in approximately 40%-50% of patients with primary ciliary dyskinesia (PCD). We evaluated the relationships between novel genetic results and the clinical and radiological characteristics of PCD patients with SIT. MethodsThe study included 48 patients diagnosed with PCD and SIT. Demographic and clinical features, disease-related scores (Bhalla, Primary Ciliary Dyskinesia Rule [PICADAR], and American Thoracic Society [ATS]), and genetic analyses were retrospectively assessed. ResultsThe median age of patients was 13 (6.5-16) years, and parental consanguinity was observed in 43 (89.58%) patients. Bhalla score was available in 31 patients and "moderate and severe" score was observed in 19 (61.29%) patients. The median PICADAR score was 10 (8-11), and 34 (70.83%) patients had a high (>= 10) PICADAR score. The ATS score was found to be 4 in 24 (50%) patients and 3 in 20 (43.75%) patients. Genetic data were available in 40 patients and mutations were found in 27 (67.5%) patients. The most common pathogenic variants were DNAH5 in 8 (20%), CCDC103 in 4 (10%), and CCDC39 in 3 (7.5%) patients. Subjects with any genetic variants may be older, have a greater frequency of parental consanguinity, higher Bhalla score, and higher ATS score (p < 0.05). DNAH5 mutation was associated with a lower likelihood of neonatal ICU stay and neonatal respiratory distress-related symptoms (p = 0.036 and 0.015, respectively). ConclusionsSitus abnormalities may be a warning sign for the early diagnosis of PCD. Early diagnosis of PCD through genetic analysis is important for preventing chronic lung pathologies and predicting prognosis and may improve the quality of life.
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