Redox-and ligand binding-dependent conformational ensembles in the human apoptosis-inducing factor regulate its pro-life and cell death functions
Villanueva, Raquel ; Romero-Tamayo, Silvia (Universidad de Zaragoza) ; Laplaza, Ruben ; Martinez-Olivan, Juan ; Velazquez-Campoy, Adrián (Universidad de Zaragoza) ; Sancho, Javier (Universidad de Zaragoza) ; Ferreira, Patricia (Universidad de Zaragoza) ; Medina, Milagros (Universidad de Zaragoza)
Resumen: Aims: The human apoptosis-inducing factor (hAIF) supports OXPHOS biogenesis and programmed cell death, with missense mutations producing neurodegenerative phenotypes. hAIF senses the redox environment of cellular compartments, stabilizing a charge transfer complex (CTC) dimer that modulates the protein interaction network. In this context, we aimed to evaluate the subcellular pH, CTC formation, and pathogenic mutations effects on hAIF stability, and a thermal denaturation high-throughput screening (HTS) assay to discover AIF binders.
Results: Apoptotic hAIF(Delta 1-101) is not stable at intermembrane mitochondrial space (IMS) pH, but the 77-101 residues confer stability to the mitochondrial isoform. hAIF and its CTC populate different conformational ensembles with redox switch to the CTC producing a less stable and compact protein. The pathogenic G308E, Delta R201, and E493V mutations modulate hAIF stability; particularly, Delta R201 causes a population shift to a less stable conformation that remodels active site structure and dynamics. We have identified new molecules that modulate the hAIF reduced nicotinamide adenine dinucleotide (NADH)/oxidized nicotinamide adenine dinucleotide (NAD(+)) association/dissociation equilibrium and regulate its catalytic efficiency.
Innovation: Biophysical methods allow evaluating the regulation of hAIF functional ensembles and to develop an HTS assay to discover small molecules that might modulate hAIF stability and activities.
Conclusions: The mitochondrial soluble 54-77 portion stabilizes hAIF at the IMS pH. NADH-redox-linked conformation changes course with strong NAD(+) binding and protein dimerization, but they produce a negative impact in overall hAIF stability. Loss of functionality in the R201 deletion is due to distortion of the active site architecture. We report molecules that may serve as leads in the development of hAIF bioactive compounds.
Idioma: Inglés
DOI: 10.1089/ars.2018.7658
Año: 2019
Publicado en: Antioxidants & redox signaling 30, 18 (2019), 2013-2029
ISSN: 1523-0864
Factor impacto JCR: 7.04 (2019)
Categ. JCR: ENDOCRINOLOGY & METABOLISM rank: 13 / 143 = 0.091 (2019) - Q1 - T1
Categ. JCR: BIOCHEMISTRY & MOLECULAR BIOLOGY rank: 35 / 297 = 0.118 (2019) - Q1 - T1
Factor impacto SCIMAGO: 2.163 - Biochemistry (Q1) - Cell Biology (Q1) - Physiology (Q1) - Medicine (miscellaneous) (Q1) - Molecular Biology (Q1) - Clinical Biochemistry (Q1)
Financiación: info:eu-repo/grantAgreement/ES/DGA/E35-17R
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-17R
Financiación: info:eu-repo/grantAgreement/ES/MINECO/BFU2016-78232-P
Financiación: info:eu-repo/grantAgreement/ES/MINECO-FEDER/BIO2016-75183-P
Tipo y forma: Article (PostPrint)
Área (Departamento): Área Bioquímica y Biolog.Mole. (Dpto. Bioq.Biolog.Mol. Celular)
All rights reserved by journal editor
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Results: Apoptotic hAIF(Delta 1-101) is not stable at intermembrane mitochondrial space (IMS) pH, but the 77-101 residues confer stability to the mitochondrial isoform. hAIF and its CTC populate different conformational ensembles with redox switch to the CTC producing a less stable and compact protein. The pathogenic G308E, Delta R201, and E493V mutations modulate hAIF stability; particularly, Delta R201 causes a population shift to a less stable conformation that remodels active site structure and dynamics. We have identified new molecules that modulate the hAIF reduced nicotinamide adenine dinucleotide (NADH)/oxidized nicotinamide adenine dinucleotide (NAD(+)) association/dissociation equilibrium and regulate its catalytic efficiency.
Innovation: Biophysical methods allow evaluating the regulation of hAIF functional ensembles and to develop an HTS assay to discover small molecules that might modulate hAIF stability and activities.
Conclusions: The mitochondrial soluble 54-77 portion stabilizes hAIF at the IMS pH. NADH-redox-linked conformation changes course with strong NAD(+) binding and protein dimerization, but they produce a negative impact in overall hAIF stability. Loss of functionality in the R201 deletion is due to distortion of the active site architecture. We report molecules that may serve as leads in the development of hAIF bioactive compounds.
Idioma: Inglés
DOI: 10.1089/ars.2018.7658
Año: 2019
Publicado en: Antioxidants & redox signaling 30, 18 (2019), 2013-2029
ISSN: 1523-0864
Factor impacto JCR: 7.04 (2019)
Categ. JCR: ENDOCRINOLOGY & METABOLISM rank: 13 / 143 = 0.091 (2019) - Q1 - T1
Categ. JCR: BIOCHEMISTRY & MOLECULAR BIOLOGY rank: 35 / 297 = 0.118 (2019) - Q1 - T1
Factor impacto SCIMAGO: 2.163 - Biochemistry (Q1) - Cell Biology (Q1) - Physiology (Q1) - Medicine (miscellaneous) (Q1) - Molecular Biology (Q1) - Clinical Biochemistry (Q1)
Financiación: info:eu-repo/grantAgreement/ES/DGA/E35-17R
Financiación: info:eu-repo/grantAgreement/ES/DGA/E45-17R
Financiación: info:eu-repo/grantAgreement/ES/MINECO/BFU2016-78232-P
Financiación: info:eu-repo/grantAgreement/ES/MINECO-FEDER/BIO2016-75183-P
Tipo y forma: Article (PostPrint)
Área (Departamento): Área Bioquímica y Biolog.Mole. (Dpto. Bioq.Biolog.Mol. Celular)
All rights reserved by journal editorExportado de SIDERAL (2020-12-15-12:29:31)
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Record created 2020-05-07, last modified 2020-12-15