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NM_138636.5(TLR8):c.1295C>T (p.Pro432Leu) AND INFLTR8

Germline classification:
Pathogenic (1 submission)
Review status:
(0/4) 0 stars out of maximum of 4 stars
no assertion criteria provided
Somatic classification
of clinical impact:
None
Review status:
(0/4) 0 stars out of maximum of 4 stars
no assertion criteria provided
Somatic classification
of oncogenicity:
None
Review status:
(0/4) 0 stars out of maximum of 4 stars
no assertion criteria provided
Record status:
current
Accession:
RCV001526670.1

Allele description [Variation Report for NM_138636.5(TLR8):c.1295C>T (p.Pro432Leu)]

NM_138636.5(TLR8):c.1295C>T (p.Pro432Leu)

Genes:
TLR8-AS1:TLR8 antisense RNA 1 [Gene - HGNC]
TLR8:toll like receptor 8 [Gene - OMIM - HGNC]
Variant type:
single nucleotide variant
Cytogenetic location:
Xp22.2
Genomic location:
Preferred name:
NM_138636.5(TLR8):c.1295C>T (p.Pro432Leu)
HGVS:
  • NC_000023.11:g.12920335C>T
  • NG_012882.2:g.18716C>T
  • NM_016610.4:c.1349C>T
  • NM_138636.5:c.1295C>TMANE SELECT
  • NP_057694.2:p.Pro450Leu
  • NP_619542.1:p.Pro432Leu
  • NC_000023.10:g.12938454C>T
  • NC_000023.10:g.12938454C>T
  • NM_016610.3:c.1349C>T
Protein change:
P432L; PRO432LEU
Links:
OMIM: 300366.0001; dbSNP: rs2147258995
NCBI 1000 Genomes Browser:
rs2147258995
Molecular consequence:
  • NM_016610.4:c.1349C>T - missense variant - [Sequence Ontology: SO:0001583]
  • NM_138636.5:c.1295C>T - missense variant - [Sequence Ontology: SO:0001583]
Functional consequence:
gain_of_function_variant [Sequence Ontology: SO:0002053]

Condition(s)

Name:
INFLTR8
Identifiers:

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Assertion and evidence details

Help
Submission AccessionSubmitterReview Status
(Assertion method)		Clinical Significance
(Last evaluated)		OriginMethodCitations
SCV001652777Megan Cooper Lab, Washington University School of Medicine in St Louis
no assertion criteria provided
Pathogenicgermlinecase-control

PubMed (1)
[See all records that cite this PMID]

Help

Summary from all submissions

EthnicityOriginAffectedIndividualsFamiliesChromosomes testedNumber TestedFamily historyMethod
not providedgermlineyes44not providednot providednot providedcase-control

Citations

PubMed

Immunodeficiency and bone marrow failure with mosaic and germline TLR8 gain of function.

Aluri J, Bach A, Kaviany S, Chiquetto Paracatu L, Kitcharoensakkul M, Walkiewicz MA, Putnam CD, Shinawi M, Saucier N, Rizzi EM, Harmon MT, Keppel MP, Ritter M, Similuk M, Kulm E, Joyce M, de Jesus AA, Goldbach-Mansky R, Lee YS, Cella M, Kendall PL, Dinauer MC, et al.

Blood. 2021 May 6;137(18):2450-2462. doi: 10.1182/blood.2020009620.

PubMed [citation]
PMID:
33512449
PMCID:
PMC8109013

Details of each submission

From Megan Cooper Lab, Washington University School of Medicine in St Louis, SCV001652777.1

#EthnicityIndividualsChromosomes TestedFamily HistoryMethodCitations
1not provided4not providednot providedcase-control PubMed (1)

Description

We identified 6 unrelated males with neutropenia, infections, lymphoproliferation, humoral immune defects, and in some cases bone marrow failure associated with 3 different variants in the X-linked gene TLR8, encoding the endosomal Toll-like receptor 8 (TLR8). Interestingly, 5 patients had somatic variants in TLR8 with <30% mosaicism, suggesting a dominant mechanism responsible for the clinical phenotype. Mosaicism was also detected in skin-derived fibroblasts in 3 patients, demonstrating that mutations were not limited to the hematopoietic compartment. All patients had refractory chronic neutropenia, and 3 patients underwent allogeneic hematopoietic cell transplantation. All variants conferred gain of function to TLR8 protein, and immune phenotyping demonstrated a proinflammatory phenotype with activated T cells and elevated serum cytokines associated with impaired B-cell maturation. Differentiation of myeloid cells from patient-derived induced pluripotent stem cells demonstrated increased responsiveness to TLR8. Together, these findings demonstrate that gain-of-function variants in TLR8 lead to a novel childhood-onset IEI with lymphoproliferation, neutropenia, infectious susceptibility, B- and T-cell defects, and in some cases, bone marrow failure. Somatic mosaicism is a prominent molecular mechanism of this new disease.

#SampleMethodObservation
OriginAffectedNumber testedTissuePurposeMethodIndividualsAllele frequencyFamiliesCo-occurrences
1germlineyesnot providednot providednot provided4not provided4not provided

Last Updated: Oct 13, 2024