Open AccessGermline SAMD9L truncation variants trigger global translational repression
Author(s) -
Eric J. Allenspach,
Frank Soveg,
Laura S. Finn,
Lomon So,
Jacquelyn A. Gorman,
Aaron B.I. Rosen,
Suzanne Skoda-Smith,
Marsha M. Wheeler,
Kaitlyn A Barrow,
Lucille M. Rich,
Jason S. Debley,
Michael J. Bamshad,
Deborah A. Nickerson,
Ram Savan,
Troy R. Torgerson,
David J. Rawlings
Publication year - 2021
Publication title -
the journal of experimental medicine/the journal of experimental medicine
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 8.483
H-Index - 448
eISSN - 1540-9538
pISSN - 0022-1007
DOI - 10.1084/jem.20201195
Subject(s) - biology , frameshift mutation , interferon , immunology , phenotype , genetics , gene
SAMD9L is an interferon-induced tumor suppressor implicated in a spectrum of multisystem disorders, including risk for myeloid malignancies and immune deficiency. We identified a heterozygous de novo frameshift variant in SAMD9L in an infant with B cell aplasia and clinical autoinflammatory features who died from respiratory failure with chronic rhinovirus infection. Autopsy demonstrated absent bone marrow and peripheral B cells as well as selective loss of Langerhans and Purkinje cells. The frameshift variant led to expression of a truncated protein with interferon treatment. This protein exhibited a gain-of-function phenotype, resulting in interference in global protein synthesis via inhibition of translational elongation. Using a mutational scan, we identified a region within SAMD9L where stop-gain variants trigger a similar translational arrest. SAMD9L variants that globally suppress translation had no effect or increased mRNA transcription. The complex-reported phenotype likely reflects lineage-dominant sensitivities to this translation block. Taken together, our findings indicate that interferon-triggered SAMD9L gain-of-function variants globally suppress translation.