The metabesity factor HMG20A potentiates astrocyte survival and reactive astrogliosis preserving neuronal integrity

Lorenzo, Petra I.; Vázquez, Eugenia Martin; López-Noriega, Livia; Fuente-Martín, Esther; Mellado-Gil, José Manuel; Franco, Jaime M.; Cobo-Vuilleumier, Nadia; Guerrero-Martínez, José A.; Romero-Zerbo, Silvana Y.; Perez-Cabello, Jesús A; Rivero, Sabrina; Campos‐Caro, Antonio; Lachaud, Christian Claude; Barreda, Alejandra Crespo; Aguilar‐Diosdado, Manuel; Fuentes, Esther; Martín-Montalvo, Aléjandro; Álvarez‐Dolado, Manuel; Martı́n, Franz; Rojo‐Martínez, Gemma; Pozo, David; Bermúdez‐Silva, Francisco Javier; Comaills, Valentine; Reyes, José Carlos Castañeda; Gauthier, Benoît

doi:10.7150/thno.57237

Cited by 17 publications

(14 citation statements)

References 86 publications

(115 reference statements)

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“…As the LSD1/Co-REST complex is essential for REST-dependent repression, an antagonist of LSD1/Co-REST should improve neuronal differentiation. Consistent with this, HMG20A is highly expressed in the brain ( 1 , 7 ) and is required for human neuronal differentiation in vitro and neuronal differentiation in ovo in the chicken neural tube ( 5 ).…”

Section: Introductionsupporting

confidence: 56%

The high mobility group protein HMG20A cooperates with the histone reader PHF14 to modulate TGFβ and Hippo pathways

Gómez-Marín

Posavec-Marjanović

Zarzuela

et al. 2022

Nucleic Acids Research

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High mobility group (HMG) proteins are chromatin regulators with essential functions in development, cell differentiation and cell proliferation. The protein HMG20A is predicted by the AlphaFold2 software to contain three distinct structural elements, which we have functionally characterized: i) an amino-terminal, intrinsically disordered domain with transactivation activity; ii) an HMG box with higher binding affinity for double-stranded, four-way-junction DNA than for linear DNA; and iii) a long coiled-coil domain. Our proteomic study followed by a deletion analysis and structural modeling demonstrates that HMG20A forms a complex with the histone reader PHF14, via the establishment of a two-stranded alpha-helical coiled-coil structure. siRNA-mediated knockdown of either PHF14 or HMG20A in MDA-MB-231 cells causes similar defects in cell migration, invasion and homotypic cell–cell adhesion ability, but neither affects proliferation. Transcriptomic analyses demonstrate that PHF14 and HMG20A share a large subset of targets. We show that the PHF14-HMG20A complex modulates the Hippo pathway through a direct interaction with the TEAD1 transcription factor. PHF14 or HMG20A deficiency increases epithelial markers, including E-cadherin and the epithelial master regulator TP63 and impaired normal TGFβ-trigged epithelial-to-mesenchymal transition. Taken together, these data indicate that PHF14 and HMG20A cooperate in regulating several pathways involved in epithelial–mesenchymal plasticity.

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Section: Introductionsupporting

confidence: 56%

The high mobility group protein HMG20A cooperates with the histone reader PHF14 to modulate TGFβ and Hippo pathways

Gómez-Marín

Posavec-Marjanović

Zarzuela

et al. 2022

Nucleic Acids Research

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“…Cell death (apoptosis) was measured using the Cell Death Detection ELISA kit (Merck/Roche Diagnostics, Madrid, Spain) ( Lorenzo et al., 2021 ).…”

Section: Methodsmentioning

confidence: 99%

NR5A2/LRH-1 regulates the PTGS2-PGE2-PTGER1 pathway contributing to pancreatic islet survival and function

et al. 2022

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“…In the hypothalamus, HFD treatment in adults was found to produce astrogliosis as well as reduce the protein expression of vesicular glutamate transporter and GABA transporters, possibly reducing the availability of excitatory and inhibitory vesicles for neurotransmission [ 127 , 149 ]. However, no significant impact of HFD treatment was seen on the expression of synaptic proteins, neuronal integrity and microgliosis [ 104 , 127 , 147 ].…”

Section: Impact Of a High-fat Diet Treatment On Molecular Correlates ...mentioning

confidence: 99%

Neurobiological Mechanisms Modulating Emotionality, Cognition and Reward-Related Behaviour in High-Fat Diet-Fed Rodents

Ziemens

Touma

Rappeneau

2022

IJMS

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Affective and substance-use disorders are associated with overweight and obesity-related complications, which are often due to the overconsumption of palatable food. Both high-fat diets (HFDs) and psychostimulant drugs modulate the neuro-circuitry regulating emotional processing and metabolic functions. However, it is not known how they interact at the behavioural level, and whether they lead to overlapping changes in neurobiological endpoints. In this literature review, we describe the impact of HFDs on emotionality, cognition, and reward-related behaviour in rodents. We also outline the effects of HFD on brain metabolism and plasticity involving mitochondria. Moreover, the possible overlap of the neurobiological mechanisms produced by HFDs and psychostimulants is discussed. Our in-depth analysis of published results revealed that HFDs have a clear impact on behaviour and underlying brain processes, which are largely dependent on the developmental period. However, apart from the studies investigating maternal exposure to HFDs, most of the published results involve only male rodents. Future research should also examine the biological impact of HFDs in female rodenrts. Further knowledge about the molecular mechanisms linking stress and obesity is a crucial requirement of translational research and using rodent models can significantly advance the important search for risk-related biomarkers and the development of clinical intervention strategies.

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The metabesity factor HMG20A potentiates astrocyte survival and reactive astrogliosis preserving neuronal integrity

Cited by 17 publications

References 86 publications

The high mobility group protein HMG20A cooperates with the histone reader PHF14 to modulate TGFβ and Hippo pathways

The high mobility group protein HMG20A cooperates with the histone reader PHF14 to modulate TGFβ and Hippo pathways

NR5A2/LRH-1 regulates the PTGS2-PGE2-PTGER1 pathway contributing to pancreatic islet survival and function

Neurobiological Mechanisms Modulating Emotionality, Cognition and Reward-Related Behaviour in High-Fat Diet-Fed Rodents

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