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Article Dans Une Revue Development (Cambridge, England) Année : 1998

The RXRalpha ligand-dependent activation function 2 (AF-2) is important for mouse development

Résumé

We have engineered a mouse mutation that specifically deletes the C-terminal 18 amino acid sequence of the RXRalpha protein. This deletion corresponds to the last helical alpha structure (H12) of the ligand-binding domain (LBD), and includes the core of the Activating Domain of the Activation Function 2 (AF-2 AD core) that is thought to be crucial in mediating ligand-dependent transactivation by RXRalpha. The homozygous mutants (RXRalpha af2(o)), which die during the late fetal period or at birth, exhibit a subset of the abnormalities previously observed in RXRalpha -/- mutants, often with incomplete penetrance. In marked contrast, RXRalpha af2(o)/RXRbeta -/- and RXRalpha af2(o)/RXRbeta -/- /RXRgamma -/- compound mutants display a large array of malformations, which nearly recapitulate the full spectrum of the defects that characterize the fetal vitamin A-deficiency (VAD) syndrome and were previously found in RAR single and compound mutants, as well as in RXRalpha/RAR(alpha, beta or gamma) compound mutants. Analysis of RXRalpha af2(o)/RAR(alpha, beta or gamma) compound mutants also revealed that they exhibit many of the defects observed in the corresponding RXR alpha/RAR compound mutants. Together, these results demonstrate the importance of the integrity of RXR AF-2 for the developmental functions mediated by RAR/RXR heterodimers, and hence suggest that RXR ligand-dependent transactivation is instrumental in retinoid signalling during development.
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Dates et versions

hal-04057130 , version 1 (03-04-2023)

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Bénédicte Mascrez, Manuel Mark, Andree Dierich, Norbert B. Ghyselinck, Philippe Kastner, et al.. The RXRalpha ligand-dependent activation function 2 (AF-2) is important for mouse development. Development (Cambridge, England), 1998, 125 (23), pp.4691-4707. ⟨10.1242/dev.125.23.4691⟩. ⟨hal-04057130⟩
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