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Gain-of-function mutations in ALPK1 cause an NF-κB-mediated autoinflammatory disease: functional assessment, clinical phenotyping and disease course of patients with ROSAH syndrome.
Kozycki, Christina Torres; Kodati, Shilpa; Huryn, Laryssa; Wang, Hongying; Warner, Blake M; Jani, Priyam; Hammoud, Dima; Abu-Asab, Mones S; Jittayasothorn, Yingyos; Mattapallil, Mary J; Tsai, Wanxia Li; Ullah, Ehsan; Zhou, Ping; Tian, Xiaoying; Soldatos, Ariane; Moutsopoulos, Niki; Kao-Hsieh, Marie; Heller, Theo; Cowen, Edward W; Lee, Chyi-Chia Richard; Toro, Camilo; Kalsi, Shelley; Khavandgar, Zohreh; Baer, Alan; Beach, Margaret; Long Priel, Debra; Nehrebecky, Michele; Rosenzweig, Sofia; Romeo, Tina; Deuitch, Natalie; Brenchley, Laurie; Pelayo, Eileen; Zein, Wadih; Sen, Nida; Yang, Alexander H; Farley, Gary; Sweetser, David A; Briere, Lauren; Yang, Janine; de Oliveira Poswar, Fabiano; Schwartz, Ida Vanessa D; Silva Alves, Tamires; Dusser, Perrine; Koné-Paut, Isabelle; Touitou, Isabelle; Titah, Salah Mohamed; van Hagen, Petrus Martin; van Wijck, Rogier T A; van der Spek, Peter J; Yano, Hiromi.
Afiliación
  • Kozycki CT; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA christina.kozycki@nih.gov dan.kastner@nih.gov.
  • Kodati S; National Institute of Allergy and Infectious Diseases, Bethesda, Maryland, USA.
  • Huryn L; National Eye Institute, Bethesda, Maryland, USA.
  • Wang H; National Eye Institute, Bethesda, Maryland, USA.
  • Warner BM; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Jani P; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Hammoud D; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Abu-Asab MS; Radiology and Imaging Sciences, National Institutes of Health Clinical Center, Bethesda, Maryland, USA.
  • Jittayasothorn Y; Section of Histopathology, National Eye Institute, Bethesda, Maryland, USA.
  • Mattapallil MJ; National Eye Institute, Bethesda, Maryland, USA.
  • Tsai WL; National Eye Institute, Bethesda, Maryland, USA.
  • Ullah E; National Institute of Arthritis and Musculoskeletal and Skin Diseases, Bethesda, Maryland, USA.
  • Zhou P; Ophthalmic Genetics & Visual Function Branch, National Eye Institute, Bethesda, Maryland, USA.
  • Tian X; National Institute of Biological Sciences Beijing, Beijing, China.
  • Soldatos A; National Institute of Biological Sciences Beijing, Beijing, China.
  • Moutsopoulos N; National Institute of Neurological Disorders and Stroke, Bethesda, Maryland, USA.
  • Kao-Hsieh M; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Heller T; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Cowen EW; National Institute of Diabetes and Digestive and Kidney Diseases, Bethesda, Maryland, USA.
  • Lee CR; Dermatology Branch, NIH, National Institute of Arthritis and Musculoskeletal and Skin Diseases, Bethesda, Maryland, USA.
  • Toro C; National Cancer Institute, Bethesda, Maryland, USA.
  • Kalsi S; Undiagnosed Diseases Program, Bethesda, Maryland, USA.
  • Khavandgar Z; National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Baer A; National Heart Lung and Blood Institute, Bethesda, Maryland, USA.
  • Beach M; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Long Priel D; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Nehrebecky M; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Rosenzweig S; Neutrophil Monitoring Laboratory, Applied/Developmental Research Directorate, Frederick National Laboratory for Cancer Research, Frederick, Maryland, USA.
  • Romeo T; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Deuitch N; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Brenchley L; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Pelayo E; Inflammatory Disease Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Zein W; Oncogenesis and Development Section, National Human Genome Research Institute, Bethesda, Maryland, USA.
  • Sen N; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Yang AH; National Institute of Dental and Craniofacial Research, Bethesda, Maryland, USA.
  • Farley G; National Eye Institute, Bethesda, Maryland, USA.
  • Sweetser DA; National Eye Institute, Bethesda, Maryland, USA.
  • Briere L; National Institute of Diabetes and Digestive and Kidney Diseases, Bethesda, Maryland, USA.
  • Yang J; Drs. Gilbert and Farley, OD, PC, Colonial Heights, Virginia, USA.
  • de Oliveira Poswar F; Massachusetts General Hospital Center for Genomic Medicine, Boston, Massachusetts, USA.
  • Schwartz IVD; Division of Medical Genetics & Metabolism, Department of Pediatrics, Massachusetts General Hospital, Boston, Massachusetts, USA.
  • Silva Alves T; Massachusetts General Hospital Center for Genomic Medicine, Boston, Massachusetts, USA.
  • Dusser P; Massachusetts Eye and Ear, Boston, Massachusetts, USA.
  • Koné-Paut I; Hospital de Clínicas de Porto Alegre, Porto Alegre, Brazil.
  • Touitou I; Post Graduate Program in Genetics and Molecular Biology, Universidade Federal do Rio Grande do Sul, Porto Alegre, Brazil.
  • Titah SM; Hospital de Clínicas de Porto Alegre, Porto Alegre, Brazil.
  • van Hagen PM; Post Graduate Program in Genetics and Molecular Biology, Universidade Federal do Rio Grande do Sul, Porto Alegre, Brazil.
  • van Wijck RTA; Hospital de Clínicas de Porto Alegre, Porto Alegre, Brazil.
  • van der Spek PJ; Service de Rhumatologie Pédiatrique, Centre de Référence des Maladies Auto-Inflammatoires de l'enfant, Hôpital Bicêtre, AP HP, Université Paris Sud, Bicetre, France.
  • Yano H; Service de Rhumatologie Pédiatrique, Centre de Référence des Maladies Auto-Inflammatoires et de l'amylose inflammatoire CEREMAIA, Hôpital Bicêtre, AP HP, Université Paris Saclay, Bicetre, France.
Ann Rheum Dis ; 81(10): 1453-1464, 2022 10.
Article en En | MEDLINE | ID: mdl-35868845
ABSTRACT

OBJECTIVES:

To test the hypothesis that ROSAH (retinal dystrophy, optic nerve oedema, splenomegaly, anhidrosis and headache) syndrome, caused by dominant mutation in ALPK1, is an autoinflammatory disease.

METHODS:

This cohort study systematically evaluated 27 patients with ROSAH syndrome for inflammatory features and investigated the effect of ALPK1 mutations on immune signalling. Clinical, immunologic and radiographical examinations were performed, and 10 patients were empirically initiated on anticytokine therapy and monitored. Exome sequencing was used to identify a new pathogenic variant. Cytokine profiling, transcriptomics, immunoblotting and knock-in mice were used to assess the impact of ALPK1 mutations on protein function and immune signalling.

RESULTS:

The majority of the cohort carried the p.Thr237Met mutation but we also identified a new ROSAH-associated mutation, p.Tyr254Cys.Nearly all patients exhibited at least one feature consistent with inflammation including recurrent fever, headaches with meningeal enhancement and premature basal ganglia/brainstem mineralisation on MRI, deforming arthritis and AA amyloidosis. However, there was significant phenotypic variation, even within families and some adults lacked functional visual deficits. While anti-TNF and anti-IL-1 therapies suppressed systemic inflammation and improved quality of life, anti-IL-6 (tocilizumab) was the only anticytokine therapy that improved intraocular inflammation (two of two patients).Patients' primary samples and in vitro assays with mutated ALPK1 constructs showed immune activation with increased NF-κB signalling, STAT1 phosphorylation and interferon gene expression signature. Knock-in mice with the Alpk1 T237M mutation exhibited subclinical inflammation.Clinical features not conventionally attributed to inflammation were also common in the cohort and included short dental roots, enamel defects and decreased salivary flow.

CONCLUSION:

ROSAH syndrome is an autoinflammatory disease caused by gain-of-function mutations in ALPK1 and some features of disease are amenable to immunomodulatory therapy.
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Texto completo: 1 Bases de datos: MEDLINE Asunto principal: Proteínas Quinasas / FN-kappa B / Enfermedades Autoinflamatorias Hereditarias Tipo de estudio: Etiology_studies / Incidence_studies / Observational_studies / Prognostic_studies / Risk_factors_studies Límite: Animals / Humans Idioma: En Revista: Ann Rheum Dis Año: 2022 Tipo del documento: Article
Texto completo
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Texto completo: 1 Bases de datos: MEDLINE Asunto principal: Proteínas Quinasas / FN-kappa B / Enfermedades Autoinflamatorias Hereditarias Tipo de estudio: Etiology_studies / Incidence_studies / Observational_studies / Prognostic_studies / Risk_factors_studies Límite: Animals / Humans Idioma: En Revista: Ann Rheum Dis Año: 2022 Tipo del documento: Article