Pathogenic variants in HGF give rise to childhood-to-late onset primary lymphoedema by loss of function.
Murat AlpaslanElodie FastréSandrine MestreArie van HaeringenGabriela M RepettoKathelijn KeymolenLaurence M BoonFlorence BelvaGuido GiacaloneNicole RevencuYves SznajerKatie RichesVaughan KeeleyShehla MohammedKristiana GordonSilvia Martin-AlmedinaSara E DobbinsPia OstergaardIsabelle QuéréPascal BrouillardMiikka VikkulaPublished in: Human molecular genetics (2024)
Developmental and functional defects in the lymphatic system are responsible for primary lymphoedema (PL). PL is a chronic debilitating disease caused by increased accumulation of interstitial fluid, predisposing to inflammation, infections and fibrosis. There is no cure, only symptomatic treatment is available. Thirty-two genes or loci have been linked to PL, and another 22 are suggested, including Hepatocyte Growth Factor (HGF). We searched for HGF variants in 770 index patients from the Brussels PL cohort. We identified ten variants predicted to cause HGF loss-of-function (six nonsense, two frameshifts, and two splice-site changes; 1.3% of our cohort), and 14 missense variants predicted to be pathogenic in 17 families (2.21%). We studied co-segregation within families, mRNA stability for non-sense variants, and in vitro functional effects of the missense variants. Analyses of the mRNA of patient cells revealed degradation of the nonsense mutant allele. Reduced protein secretion was detected for nine of the 14 missense variants expressed in COS-7 cells. Stimulation of lymphatic endothelial cells with these 14 HGF variant proteins resulted in decreased activation of the downstream targets AKT and ERK1/2 for three of them. Clinically, HGF-associated PL was diverse, but predominantly bilateral in the lower limbs with onset varying from early childhood to adulthood. Finally, aggregation study in a second independent cohort underscored that rare likely pathogenic variants in HGF explain about 2% of PL. Therefore, HGF signalling seems crucial for lymphatic development and/or maintenance in human beings and HGF should be included in diagnostic genetic screens for PL.
Keyphrases
- copy number
- endothelial cells
- late onset
- genome wide
- growth factor
- induced apoptosis
- lymph node
- signaling pathway
- oxidative stress
- intellectual disability
- dna methylation
- end stage renal disease
- depressive symptoms
- ejection fraction
- gene expression
- cell cycle arrest
- autism spectrum disorder
- small molecule
- peritoneal dialysis
- transcription factor
- patient reported outcomes
- pi k akt
- protein protein