Publication for RECQL4 and RTEL1
| Species | Symbol | Function* | Entrez Gene ID* | Other ID | Gene coexpression |
CoexViewer |
|---|---|---|---|---|---|---|
| hsa | RECQL4 | RecQ like helicase 4 | 9401 |  |
[link] | |
| hsa | RTEL1 | regulator of telomere elongation helicase 1 | 51750 | |
| Pubmed ID | Priority | Text |
|---|---|---|
| 31597307 | 0.98 | RTEL1 and RECQL4. |
| 0.98 | RTEL1, RECQL4, BLM, DNA2, FEN1, Timeless, or TOP2A) results in replication stress characterized by multiple telomeric signals and sister-telomere associations during metaphase, a phenotype defined as fragile telomere. | |
| 0.94 | RTEL1, and RECQL4), either helping in G4 unwinding or in D-loop unlocking, are depicted. | |
| 23300679 | 0.97 | RECQL4 region had the strongest association with the risk of melanoma (gene-based P-value = 2.5x10-3; Table 2, Table S2 and Figure S2) and the RTEL1 region had the strongest association with risk of dysplastic nevi (gene-based P-value = 0.004; Table 3, Table S3 and Figure S4). |
| 0.97 | RECQL4, RTEL1 and TERF2 were associated with melanoma, the presence of dysplastic nevi and number of nevi, respectively, in the Italian combined study. | |
| 0.95 | RECQL4, a gene involved in genome stability, RTEL1, a gene regulating telomere elongation, and TERF2, a gene implicated in the protection of telomeres, were associated with melanoma, the presence of dysplastic nevi and number of nevi, respectively. | |
| 27342280 | 0.97 | RECQ4, RTEL1 and PIF1, have been implicated in the unwinding of G-quadruplexes as well, and mutations in these helicases are similarly associated with genome instability and genetic disorders. |
| 0.94 | RTEL1; the RecQ-family helicases BLM, WRN and RECQ4; and PIF1. | |
| 29895583 | 0.97 | RECQL4), Shelterin (ACD, TINF2), and Telomerase (DKC1, WRAP53) pathways; 10 DNA repair genes linked to telomeres (BTBD12, DCLRE1C, DDB1, FEN1, HMBOX1, MSH2, PARP3, RAD51L3, RAD54L, and SIRT6); and seven other TRGs (BICD1, CLPTM1L, MAD1L1, MTRR, MYC, RTEL1, and SIP1). |
| 0.93 | RECQL4), Shelterin (ACD), and Telomerase (DKC1) pathways; eight CpGs on six TRGs in the DNA repair pathway (DCLRE1C, DDB1, MSH2, PARP3, RAD51L3, and SIRT6); and one CpG on each of BICD1, CLPTM1L, MAD1L1, MTRR, RTEL1, and SIP1. | |
| 27308340 | 0.97 | RECQ4, RECQ5, RTEL1, and WRN (Table 1) (Rogers, van Kessel, and Bochman, in press). |
| 28981702 | 0.97 | RecQL4, RecQL1, RTEL1 have been tightly implicated in telomere maintenance mediated by TRF2. |
| 29255170 | 0.97 | RECQ4, RECQ5, RTEL1) and analysed RPA-positive UFB formation. |
| 29273621 | 0.97 | RECQL4, and RECQL5) and Fe-S (FANCJ, RTEL1, XPD, and DDX11) families to act on unique structures in nucleic acid metabolism. |
| 31287417 | 0.97 | RECQL4, RTEL1 and DHX36, alongside many others with no known G4 link (see Figure 10A). |
| 25990736 | 0.80 | RecQL4, RecQL1 and RTEL1 have been implicated in telomere maintenance. |
| 20637196 | 0.54 | RecQ4 Mm, BAD11131; RecQ5 ce, CAA86232; RecQ5 Dm, AAD43051; RecQ5 Gg, BAI79325; RecQ5 Hs, NP_004250; RecQ5 Mm, BAD11130; Rqh Sp, CAA91177.1; RTEL1 Hs, NP_116575; RTEL1 Ce, NP_492769; RTEL1 Mm, AAI44979; Sgs1 Sc, AAB60289.1; WRN Gg, BAI79323; WRN Hs, AAC63361; WRN Mm, AAH60700; WRN Xl, NP_001081838; WRN1 Ce, NP_495324. |
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