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Gene Information
Gene symbol: TRIM22
Gene name: tripartite motif containing 22
HGNC ID: 16379
Synonyms: STAF50, GPSTAF50, RNF94
Related Genes
| # | Gene Symbol | Number of hits |
| 1 | ADAR | 1 hits |
| 2 | BTN2A1 | 1 hits |
| 3 | BTN3A3 | 1 hits |
| 4 | IL10RB | 1 hits |
| 5 | MX1 | 1 hits |
| 6 | PVR | 1 hits |
| 7 | PVRL1 | 1 hits |
| 8 | PVRL3 | 1 hits |
| 9 | TLR4 | 1 hits |
| 10 | TP53 | 1 hits |
| 11 | TRIM25 | 1 hits |
| 12 | TRIM5 | 1 hits |
| 13 | TRIM6 | 1 hits |
| 14 | TRIM6-TRIM34 | 1 hits |
| 15 | ZFP57 | 1 hits |
Related Sentences
| # | PMID | Sentence |
| 1 | 23416095 | A limited association was found between TRIM5 (rs7122620) and TRIM25 (rs205499) gene polymorphisms and measles-specific antibody levels. |
| 2 | 23416095 | However, many associations were found between TRIM gene SNPs and variations in cellular responses (IFN-γ Elispot and secreted cytokines IL-2, IL-6, IL-10, IFN-γ, and TNF-α). |
| 3 | 23416095 | We also identified polymorphisms in the TRIM5, TRIM22, and TRIM25 genes that were associated with significant differences in cytokine responses. |
| 4 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 5 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 6 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 7 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 8 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 9 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 10 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 11 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 12 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 13 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 14 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 15 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 16 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 17 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 18 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 19 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 20 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 21 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 22 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 23 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 24 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 25 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 26 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 27 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 28 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 29 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 30 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 31 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 32 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 33 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 34 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 35 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 36 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 37 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 38 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 39 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 40 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 41 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 42 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 43 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 44 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 45 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 46 | 23516500 | Elevated rate of fixation of endogenous retroviral elements in Haplorhini TRIM5 and TRIM22 genomic sequences: impact on transcriptional regulation. |
| 47 | 23516500 | All genes in the TRIM6/TRIM34/TRIM5/TRIM22 locus are type I interferon inducible, with TRIM5 and TRIM22 possessing antiviral properties. |
| 48 | 23516500 | Evolutionary studies involving the TRIM6/34/5/22 locus have predominantly focused on the coding sequence of the genes, finding that TRIM5 and TRIM22 have undergone high rates of both non-synonymous nucleotide replacements and in-frame insertions and deletions. |
| 49 | 23516500 | The transcribed genomic regions, including the introns, of TRIM6, TRIM34, TRIM5, and TRIM22 from ten Haplorhini primates and one prosimian species were analyzed for transposable element content. |
| 50 | 23516500 | Multiple lineage-specific endogenous retroviral long terminal repeats (LTRs) were identified in the first intron of TRIM5 and TRIM22. |
| 51 | 23516500 | In the prosimian genome, we identified a duplication of TRIM5 with a concomitant loss of TRIM22. |
| 52 | 23516500 | Furthermore, we demonstrated that one such differentially fixed LTR provides for species-specific transcriptional regulation of TRIM22 in response to p53 activation. |
| 53 | 26329766 | Of these SNPs, we detected eight in the PVRL3 gene, five in the PVRL1 gene, one in the TRIM22 gene, two in the IL10RB gene, two in the TLR4 gene, and five in other genes (PVR, ADAR, ZFP57, MX1, and BTN2A1/BTN3A3). |