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IRF4 haploinsufficiency in a family with Whipple's disease.

Authors :: Guérin A
Kerner G
Marr N
Markle JG
Fenollar F
Wong N
Boughorbel S
Avery DT
Ma CS
Bougarn S
Bouaziz M
Béziat V
Della Mina E
Oleaga-Quintas C
Lazarov T
Worley L
Nguyen T
Patin E
Deswarte C
Martinez-Barricarte R
Boucherit S
Ayral X
Edouard S
Boisson-Dupuis S
Rattina V
Bigio B
Vogt G
Geissmann F
Quintana-Murci L
Chaussabel D
Tangye SG
Raoult D
Abel L
Bustamante J
Casanova JL
Source :: ELife [Elife] 2018 Mar 14; Vol. 7. Date of Electronic Publication: 2018 Mar 14.
Publication Year :: 2018
Abstract: Most humans are exposed to Tropheryma whipplei (Tw). Whipple's disease (WD) strikes only a small minority of individuals infected with Tw (<0.01%), whereas asymptomatic chronic carriage is more common (<25%). We studied a multiplex kindred, containing four WD patients and five healthy Tw chronic carriers. We hypothesized that WD displays autosomal dominant (AD) inheritance, with age-dependent incomplete penetrance. We identified a single very rare non-synonymous mutation in the four patients: the private R98W variant of IRF4, a transcription factor involved in immunity. The five Tw carriers were younger, and also heterozygous for R98W. We found that R98W was loss-of-function, modified the transcriptome of heterozygous leukocytes following Tw stimulation, and was not dominant-negative. We also found that only six of the other 153 known non-synonymous IRF4 variants were loss-of-function. Finally, we found that IRF4 had evolved under purifying selection. AD IRF4 deficiency can underlie WD by haploinsufficiency, with age-dependent incomplete penetrance.<br />Competing Interests: AG, GK, NM, JM, FF, NW, SB, DA, CM, SB, MB, VB, ED, CO, TL, LW, TN, EP, CD, RM, SB, XA, SE, SB, VR, BB, GV, FG, LQ, DC, ST, DR, LA, JB, JC No competing interests declared<br /> (Copyright © 2018, Guérin et al.)