Division of Dermatology, Tel-Aviv Sourasky Medical Center, Tel-Aviv, Israel.
Sackler Faculty of Medicine, Tel-Aviv University, Tel Aviv, Israel.
Br J Dermatol. 2022 Sep;187(3):392-400. doi: 10.1111/bjd.21674. Epub 2022 Jun 17.
The coexistence of pachyonychia congenita (PC) and hidradenitis suppurativa (HS) has been described in case reports. However, the pathomechanism underlying this association and its true prevalence are unknown.
To determine the genetic defect underlying the coexistence of PC and HS in a large kindred, to delineate a pathophysiological signalling defect jointly leading to both phenotypes, and to estimate the prevalence of HS in PC.
We used direct sequencing and a NOTCH luciferase reporter assay to characterize the pathophysiological basis of the familial coexistence of HS and PC. A questionnaire was distributed to patients with PC registered with the International Pachyonychia Congenita Research Registry (IPCRR) to assess the prevalence of HS among patients with PC.
Direct sequencing of DNA samples obtained from family members displaying both PC and HS demonstrated a missense variant (c.275A>G) in KRT17, encoding keratin 17. Abnormal NOTCH signalling has been suggested to contribute to HS pathogenesis. Accordingly, the KRT17 c.275A>G variant resulted in a significant decrease in NOTCH activity. To ascertain the clinical importance of the association of HS with PC, we distributed a questionnaire to all patients with PC registered with the IPCRR. Seventy-two of 278 responders reported HS-associated clinical features (25·9%). Disease-causing mutations in KRT17 were most prevalent among patients with a dual phenotype of PC and HS (43%).
The coexistence of HS and KRT17-associated PC is more common than previously thought. Impaired NOTCH signalling as a result of KRT17 mutations may predispose patients with PC to HS. What is already known about this topic? The coexistence of pachyonychia congenita (PC) and hidradenitis suppurativa (HS) has been described in case reports. However, the pathomechanism underlying this association and its true prevalence are unknown. What does this study add? A dual phenotype consisting of PC and HS was found to be associated with a pathogenic variant in KRT17. This variant was found to affect NOTCH signalling, which has been previously implicated in HS pathogenesis. HS was found to be associated with PC in a large cohort of patients with PC, especially in patients carrying KRT17 variants, suggesting that KRT17 variants causing PC may also predispose to HS. What is the translational message? These findings suggest that patients with PC have a higher prevalence of HS than previously thought, and hence physicians should have a higher level of suspicion of HS diagnosis in patients with PC.
先天性厚甲症(PC)和化脓性汗腺炎(HS)共存的情况已有病例报告。然而,这种关联的发病机制及其真实患病率尚不清楚。
确定一个大家族中 PC 和 HS 共存的遗传缺陷,描绘共同导致两种表型的病理生理信号缺陷,并估计 PC 中 HS 的患病率。
我们使用直接测序和 NOTCH 荧光素酶报告基因测定来表征 HS 和 PC 家族共存的病理生理基础。我们向国际先天性厚甲症研究登记处(IPCRR)登记的 PC 患者分发了一份问卷,以评估 PC 患者中 HS 的患病率。
对表现出 PC 和 HS 的家族成员的 DNA 样本进行直接测序,发现编码角蛋白 17 的 KRT17 中有一个错义变异(c.275A>G)。异常的 NOTCH 信号已被认为有助于 HS 的发病机制。因此,KRT17 c.275A>G 变异导致 NOTCH 活性显著降低。为了确定 HS 与 PC 关联的临床重要性,我们向 IPCRR 登记的所有 PC 患者分发了一份问卷。在 278 名应答者中,有 72 名报告了与 HS 相关的临床特征(25.9%)。在具有 PC 和 HS 双重表型的患者中,KRT17 的致病变异最为常见(43%)。
HS 和 KRT17 相关 PC 的共存比以前认为的更为常见。KRT17 突变导致的 NOTCH 信号受损可能使 PC 患者易患 HS。
已知该主题的内容?先天性厚甲症(PC)和化脓性汗腺炎(HS)共存的情况已有病例报告。然而,这种关联的发病机制及其真实患病率尚不清楚。
本研究有哪些新发现?发现由 KRT17 引起的双重表型(PC 和 HS)与一种致病性变异有关。该变异被发现影响 NOTCH 信号,该信号先前与 HS 的发病机制有关。在大量 PC 患者中发现 HS 与 PC 相关,尤其是在携带 KRT17 变异的患者中,这表明导致 PC 的 KRT17 变异也可能导致 HS 易感性。
这有什么临床意义?这些发现表明,PC 患者的 HS 患病率高于以前的认识,因此医生在诊断 PC 患者时应更怀疑 HS 的诊断。
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