Publication for DDX58 and PARP10
| Species | Symbol | Function* | Entrez Gene ID* | Other ID | Gene coexpression |
CoexViewer |
|---|---|---|---|---|---|---|
| hsa | DDX58 | DExD/H-box helicase 58 | 23586 |  |
[link] | |
| hsa | PARP10 | poly(ADP-ribose) polymerase family member 10 | 84875 | |
| Pubmed ID | Priority | Text |
|---|---|---|
| 32232013 | 0.93 | PARP10, GBP1, and RIG-I could significantly increase the expression of HTNV NP (Figures 6B,C), suggesting these mRNAs could play a role in the cellular response against HTNV infection. |
| 0.71 | PARP10, SAMD9, GBP1, and RIG-I) involved in the ceRNA network upon HTNV infection. | |
| 0.69 | PARP10, GBP1, and RIG-I) and circ_0000479 could dramatically increase HTNV NP expression, suggesting that these RNAs are potential inhibitors of HTNV infection. | |
| 0.67 | PARP10, GBP1, and RIG-I), circRNAs (circ_0000479), miRNAs (miR-149-5p, miR-411-3p, and miR-330-5p) in the ceRNA network were found effective to inhibit or promote virus replication. | |
| 0.63 | RIG-I, SAMD9, GBP1, and PARP10) and measured their expression levels after HTNV infection by RT-qPCR (Figure 3C). | |
| 31467282 | 0.92 | PARP10, DDX58, and OASL have been already described as antiviral effectors. |
| 30641411 | 0.54 | PARP-10, and PAPR-14, together with the RNA helicase DEAD-box proteins, such as DDX58 and DDX60. |
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