AKT1

Equivalencies: 0 | Classes: 0 | Children: 0 | Explore

Entity

Name: AKT1
Namespace: hgnc
Namespace Version: 20180906
Namespace URL: https://raw.githubusercontent.com/pharmacome/terminology/b46b65c3da259b6e86026514dfececab7c22a11b/external/hgnc-names.belns

Appears in Networks 3

Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies v1.0.0

TAU and Interaction Partners v1.2.5

TAU Interactions Section of NESTOR

Activity-dependent neuroprotective protein deficiency models synaptic and developmental phenotypes of autism-like syndrome v1.0.0

In-Edges 6

deg(p(HGNC:MAPT)) negativeCorrelation p(HGNC:AKT1) View Subject | View Object

Interestingly, it was recently found that reducing the levels of Akt, another client of the Hsp90/CHIP complex, facilitates tau degradation [123], suggesting a synchronized balance between competing Hsp90 substrates that may be driven, in part, by their relative abundance or susceptibility to Hsp90 binding PubMed:21882945

Appears in Networks:

Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies v1.0.0

complex(p(FPLX:HSP90), p(HGNC:STUB1)) association p(HGNC:AKT1) View Subject | View Object

Interestingly, it was recently found that reducing the levels of Akt, another client of the Hsp90/CHIP complex, facilitates tau degradation [123], suggesting a synchronized balance between competing Hsp90 substrates that may be driven, in part, by their relative abundance or susceptibility to Hsp90 binding PubMed:21882945

Appears in Networks:

Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies v1.0.0

complex(p(HGNC:CDC37), p(SFAM:"HSP90 Family")) positiveCorrelation act(p(HGNC:AKT1), ma(kin)) View Subject | View Object

This coordination of kinase triage decisions by Hsp90 requires the co-chaperone Cdc37 (cell division cycle protein 37). The Hsp90/Cdc37 machine is essential for the maturation of a number of kinases, including Akt PubMed:21367866

Appears in Networks:

TAU and Interaction Partners v1.2.5

a(PUBCHEM:9832404) decreases p(HGNC:AKT1) View Subject | View Object

In female mice, Akt1 (above) and ionized calcium–binding adapter molecule 1 (Iba1), a marker of microglial activation that crosslinks actin (42), were markedly increased in the Adnp+/– mouse spleen and normalized by NAP treatment, suggesting a potential peripheral inflammation–linked biomarker PubMed:30106381

Appears in Networks:

Activity-dependent neuroprotective protein deficiency models synaptic and developmental phenotypes of autism-like syndrome v1.0.0

Annotations

MeSH: Spleen
Gender: Female

complex(p(HGNC:ADNP), p(HGNC:AKT1)) hasComponent p(HGNC:AKT1) View Subject | View Object

Appears in Networks:

Activity-dependent neuroprotective protein deficiency models synaptic and developmental phenotypes of autism-like syndrome v1.0.0

p(HGNC:ADNP, pmod(MESH:Haploinsufficiency)) increases p(HGNC:AKT1) View Subject | View Object

In female mice, Akt1 (above) and ionized calcium–binding adapter molecule 1 (Iba1), a marker of microglial activation that crosslinks actin (42), were markedly increased in the Adnp+/– mouse spleen and normalized by NAP treatment, suggesting a potential peripheral inflammation–linked biomarker PubMed:30106381

Appears in Networks:

Activity-dependent neuroprotective protein deficiency models synaptic and developmental phenotypes of autism-like syndrome v1.0.0

Annotations

MeSH: Spleen
Gender: Female

Out-Edges 4

p(HGNC:AKT1) association complex(p(FPLX:HSP90), p(HGNC:STUB1)) View Subject | View Object

Interestingly, it was recently found that reducing the levels of Akt, another client of the Hsp90/CHIP complex, facilitates tau degradation [123], suggesting a synchronized balance between competing Hsp90 substrates that may be driven, in part, by their relative abundance or susceptibility to Hsp90 binding PubMed:21882945

Appears in Networks:

Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies v1.0.0

p(HGNC:AKT1) negativeCorrelation deg(p(HGNC:MAPT)) View Subject | View Object

Interestingly, it was recently found that reducing the levels of Akt, another client of the Hsp90/CHIP complex, facilitates tau degradation [123], suggesting a synchronized balance between competing Hsp90 substrates that may be driven, in part, by their relative abundance or susceptibility to Hsp90 binding PubMed:21882945

Appears in Networks:

Molecular chaperones and regulation of tau quality control: strategies for drug discovery in tauopathies v1.0.0

act(p(HGNC:AKT1), ma(kin)) positiveCorrelation complex(p(HGNC:CDC37), p(SFAM:"HSP90 Family")) View Subject | View Object

This coordination of kinase triage decisions by Hsp90 requires the co-chaperone Cdc37 (cell division cycle protein 37). The Hsp90/Cdc37 machine is essential for the maturation of a number of kinases, including Akt PubMed:21367866

Appears in Networks:

TAU and Interaction Partners v1.2.5

p(HGNC:AKT1) hasVariant p(HGNC:AKT1, var("?")) View Subject | View Object

Appears in Networks:

Activity-dependent neuroprotective protein deficiency models synaptic and developmental phenotypes of autism-like syndrome v1.0.0

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If you find BEL Commons useful in your work, please consider citing: Hoyt, C. T., Domingo-Fernández, D., & Hofmann-Apitius, M. (2018). BEL Commons: an environment for exploration and analysis of networks encoded in Biological Expression Language. Database, 2018(3), 1–11.