Yildirim Sema, Bekis Bozkurt Hayrunnisa, Erguven Muferet
Department of Pediatrics, Göztepe Prof. Dr. Süleyman Yalçın City Hospital, 34722 İstanbul, Turkey.
Department of Pediatrics, Faculty of Medicine, Kafkas University, 36000 Kars, Turkey.
J Clin Med. 2025 Jan 22;14(3):712. doi: 10.3390/jcm14030712.
: Studies have shown that some mutations, especially M694V, are correlated with renal RI and/or AA. There are limited data about rare mutations on severity of the disease and RI. Today, evaluating genotype-phenotype correlations in rare mutations is important to better understand FMF. We aimed to evaluate clinical, demographic and genetic changes and genotype-phenotype correlations in pediatric patients with FMF over thirty years as well as the importance of the rare mutations. : A total of 2765 pediatric patients with FMF were included in this study. Genetic results were firstly divided into ten groups including rare mutations. Rare mutations were seen in 2% of all patients and divided into eight groups. : There was a significant increase in compound heterozygous mutations, E148Q het/hom, R202Q het/hom, complex mutations and rare mutations in the last decade. RI wo AA was 5.8% and AA was 1% in the patients with rare mutations. While M694V and compound het with M694V were positively correlated with severe PRAS, E148Q and V726A were negatively correlated with severe PRAS ( < 0.05, R = 0.137, R = -0.077, R= -0.05, respectively). Although K695R mutation was negatively correlated with severe PRAS ( < 0.05, R = -0.04), the rate of RI was 20%. Although the rare mutation R761H was negatively correlated with severe PRAS ( < 0.05, R = -0.051), the colchicine resistance rate was 8.3%. : It may be misleading for clinicians that mutations which have increased in frequency over the years are clinically mild. RI and AA rates in rare mutations are not less than the related rates in common mutations.
研究表明,一些突变,尤其是M694V,与肾RI和/或淀粉样变性(AA)相关。关于罕见突变对疾病严重程度和RI影响的数据有限。如今,评估罕见突变中的基因型-表型相关性对于更好地理解家族性地中海热(FMF)很重要。我们旨在评估30多年来FMF儿科患者的临床、人口统计学和基因变化以及基因型-表型相关性,以及罕见突变的重要性。:本研究共纳入2765例FMF儿科患者。基因结果首先分为包括罕见突变在内的十组。在所有患者中有2%出现罕见突变,并分为八组。:在过去十年中,复合杂合突变、E148Q杂合/纯合、R202Q杂合/纯合、复杂突变和罕见突变显著增加。在罕见突变患者中,无AA的RI为5.8%,AA为1%。虽然M694V和与M694V的复合杂合与严重的阵发性腹膜炎相关综合征(PRAS)呈正相关,但E148Q和V726A与严重的PRAS呈负相关(分别为P<0.05,R = 0.137,R = -0.077,R = -0.05)。虽然K695R突变与严重的PRAS呈负相关(P<0.05,R = -0.04),但RI发生率为20%。虽然罕见突变R761H与严重的PRAS呈负相关(P<0.05,R = -0.051),但秋水仙碱耐药率为8.3%。:多年来频率增加的突变在临床上是轻度的,这可能会误导临床医生。罕见突变中的RI和AA发生率并不低于常见突变中的相关发生率。
