Clinicogenomic associations in childhood Langerhans cell histiocytosis: an international cohort study.
Paul Geraeds KempsTimo Ce ZondagHelga Björk ArnardóttirNienke Solleveld-WesterinkJelske BorstEline Christine SteenwijkDemi van EgmondJoost F SwennenhuisEllen StellooIrene TrambustiRobert M VerdijkCarel Jm van NoeselArjen Hg ClevenMarijn Scheijde-VermeulenMarco J KoudijsLenka KrskováCynthia HawkinsRudolph Maarten EgelerJesper BrokTatiana von Bahr GreenwoodKarel SvojgrAuke BeishuizenJan A M van LaarUlrike PoetschgerCaroline HutterElena SieniMilen MinkovOussama AblaJ Tom van WezelCor van den BosAstrid G S van HalterenPublished in: Blood advances (2022)
Langerhans cell histiocytosis (LCH) is a rare neoplastic disorder caused by somatic genetic alterations in hematopoietic precursor cells differentiating into CD1a+/CD207+ histiocytes. LCH clinical manifestation is highly heterogeneous. BRAF and MAP2K1 mutations account for approximately 80% of genetic driver alterations in neoplastic LCH-cells. However, their clinical associations remain incompletely understood. Here, we present an international clinicogenomic study of childhood LCH, investigating 377 patients genotyped for at least BRAFV600E. MAPK pathway gene alterations were detected in 300 (79.6%) patients, including 191 (50.7%) with BRAFV600E, 54 with MAP2K1 mutations, 39 with BRAF exon 12 mutations, 13 with rare BRAF alterations, and 3 with ARAF or KRAS mutations. Our results confirm that BRAFV600E associates with lower age at diagnosis and higher prevalence of multisystem LCH, high-risk disease, and skin involvement. Furthermore, BRAFV600E appeared to correlate with a higher prevalence of central nervous system (CNS)-risk bone lesions. In contrast, MAP2K1 mutations associated with a higher prevalence of SS-bone LCH, and BRAF exon 12 deletions seemed to correlate with more lung involvement. Although BRAFV600E correlated with reduced event-free survival (EFS) in the overall cohort, neither BRAF nor MAP2K1 mutations associated with EFS when patients were stratified by disease extent. Thus, the correlation of BRAFV600E with inferior clinical outcome is (primarily) driven by its association with disease extents known for high rates of progression or relapse, including multisystem LCH. These findings advance our understanding of factors underlying the remarkable clinical heterogeneity of LCH, but also question the independent prognostic value of lesional BRAFV600E status.
Keyphrases
- end stage renal disease
- ejection fraction
- newly diagnosed
- chronic kidney disease
- free survival
- peritoneal dialysis
- risk factors
- prognostic factors
- stem cells
- magnetic resonance
- mesenchymal stem cells
- signaling pathway
- blood brain barrier
- computed tomography
- cell cycle arrest
- bone marrow
- pi k akt
- soft tissue
- cell death
- cell proliferation
- early life