Adult cases of late-onset congenital central hypoventilation syndrome and paired-like homeobox 2B-mutation carriers: an additional case report and pooled analysis

Aoi Hino; Jiro Terada; Hajime Kasai; Hikaru Shojima; Keiko Ohgino; Ayako Sasaki; Kiyoshi Hayasaka; Koichiro Tatsumi

doi:10.5664/jcsm.8732

Adult cases of late-onset congenital central hypoventilation syndrome and paired-like homeobox 2B-mutation carriers: an additional case report and pooled analysis

J Clin Sleep Med. 2020 Nov 15;16(11):1891-1900. doi: 10.5664/jcsm.8732.

Authors

Aoi Hino¹, Jiro Terada¹, Hajime Kasai¹, Hikaru Shojima², Keiko Ohgino³, Ayako Sasaki⁴, Kiyoshi Hayasaka^{4

5}, Koichiro Tatsumi¹

Affiliations

¹ Department of Respirology, Graduate School of Medicine, Chiba University, Chiba, Japan.
² School of Medicine, Chiba University, Chiba, Japan.
³ Department of Respiratory Medicine, Kawasaki Municipal Hospital, Kawasaki City, Japan.
⁴ Department of Pediatrics, Yamagata University School of Medicine, Yamagata City, Japan.
⁵ Department of Pediatrics, Miyukikai Hospital, Kaminoyama, Japan.

Abstract

Study objectives: Congenital central hypoventilation syndrome (CCHS) is caused by the paired-like homeobox 2B (PHOX2B) mutation and predominantly diagnosed during the neonatal period. Although late-onset CCHS and PHOX2B mutation carriers have been reported, the features of these disease states in adults remain uncertain. This study aimed to identify the characteristics of adult-onset CCHS and PHOX2B-mutation carriers in adult.

Methods: We mainly searched the PubMed/Medline and Cochrane Databases and classified our target patients into 2 groups: group A, symptomatically diagnosed with late-onset CCHS in adulthood; group B, adult PHOX2B-mutation carriers. Then, clinical characteristics, including the onset, treatment, long-term course, and pattern of the PHOX2B mutation in both groups were analyzed. Additionally, a new adult-case of late-onset CCHS was added to the analysis.

Results: Group A was comprised of 12 patients. The onset triggers of illness included a history of respiratory compromise following general anesthesia and respiratory tract infections. All patients in group A had 20/25 polyalanine repeat mutations and required some chronic ventilatory support at least during sleep, including portable positive pressure ventilator via tracheostomy or noninvasive positive pressure ventilation. In these patients with ventilatory support during sleep, sudden death or poor prognosis was not reported. Group B was comprised of 33 adults from 24 families with PHOX2B mutations. Nine patients in group B were confirmed with the diagnosis of CCHS. Although polyalanine repeat mutations 20/25 represented the most common gene mutation, diverse mutations, including mosaicism, were observed. Hypoventilation of several cases in group B were underdiagnosed by overnight polysomnography without monitoring for CO₂.

Conclusion: Alveolar hypoventilation with unknown origin can be caused by the PHOX2B mutation even in adult cases. Both the identification of the PHOX2B mutation and the incorporation of capnography in polysomnography are important for adult cases with unexplained alveolar hypoventilation or asymptomatic mutation carriers.

Keywords: CCHS; PHOX2B; congenital central hypoventilation syndrome; late-onset CCHS; polysomnography; transcutaneous carbon dioxide monitoring.

Publication types

Case Reports
Research Support, Non-U.S. Gov't

MeSH terms

Adult
Genes, Homeobox*
Homeodomain Proteins / genetics
Humans
Hypoventilation / congenital
Hypoventilation / genetics
Infant, Newborn
Mutation / genetics
Sleep Apnea, Central* / genetics
Sleep Apnea, Central* / therapy

Substances

Homeodomain Proteins

Supplementary concepts

Congenital central hypoventilation syndrome