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High tyrosine hydroxylase (TH) upstream-inhibited ubiquitin protein ligase E3 component n-recognin 5 (UBR5) molecular subnetwork was constructed, including feedback sulfotransferase family 1A member 2 (SULT1A2); downstream chromosome 10 open reading frame 10 (C10orf10), heterogeneous nuclear ribonucleoprotein H3 (HNRPH3), UPF3 regulator of nonsense transcripts homolog A (yeast) (UPF3A) reported relation with learning in human left hemisphere. The common biology process of TH upstream-inhibited UBR5 subnetwork was identified by DAVID, containing feedback SULT1A2, downstream HNRPH3, downstream UPF3A, second-core UBR5, first-core TH as protein binding; downstream HNRPH3, downstream UPF3A, second-core UBR5 as RNA binding; feedback SULT1A2, first-core TH as small molecule metabolic process; downstream HNRPH3, downstream UPF3A as nucleotide binding; The common cellular component of downstream HNRPH3, downstream UPF3A, second-core UBR5, first-core TH as nucleus; feedback SULT1A2, downstream UPF3A, first-core TH as cytosol; downstream HNRPH3, downstream UPF3A, second-core UBR5 as nucleoplasm; downstream UPF3A, second-core UBR5, first-core TH as cytoplasm; downstream C10orf10, first-core TH as mitochondrion; The common tissue distributions as Prostate_3rd maybe exist the same pattern with human left hemisphere. We propose and mutual positively verify tyrosine hydroxylase (TH) upstream-inhibited ubiquitin protein ligase E3 component n-recognin 5 (UBR5) subnetwork for learning in human left hemisphere|Prostate via nucleus to cytoplasm protein binding. |
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Keywords:TH upstream-inhibited UBR5 subnetwork for learning; human left hemisphere|Prostate; nucleus to cytoplasm; protein binding |
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