UCSF Krogan Lab - CRL5_HIV_interactome

UCSF Krogan Lab - CRL5_HIV_interactome
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figure7_DIA_samples.sky.zip2024-04-09 15:12:492212125133
figure6_PRM_system_suitability_2024-02-05_19-48-55.sky.zip2024-04-09 15:12:422171718948
figure6_DIA_samples_2024-02-06_13-03-26.sky.zip2024-04-09 15:12:2722121251157
figure5_DIA_samples.sky.zip2024-04-09 15:12:182212125115
figure5_PRM_system_suitability.sky.zip2024-04-09 15:12:18217171896
figure4_PRM_system_suitability.sky.zip2024-04-09 15:12:092171718914
figure4_DIA_samples.sky.zip2024-04-09 15:12:092212125132
figure3_PRM_system_suitability.sky.zip2024-04-09 15:12:042171718937
figure2_PRM_system_suitability_2024-02-02_13-59-23.sky.zip2024-04-09 15:11:542171718985
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XW0008-Myc248_DIAassayLIB_OmBcells_17Nov2023_2024-02-16_10-02-13.sky.zip2024-02-16 15:02:065,20383,67483,675605,04024
Lumos-Jax-Cortex-DIA-ind-8mz-ovlp-400to1000-C1_B11.sky.zip2024-02-16 11:03:589,778127,624127,624966,34716
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Lumos-Jax-Cortex-DIA-ind-8mz-ovlp-400to1000-C1_B02.sky.zip2024-02-15 13:44:359,778127,624127,624966,34716
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AutoQC-lumos-PCs-MouAD-PFC-C2-B5-B7.sky.zip2024-02-14 16:42:502141417344
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AutoQC-lumos-SysS-MouAD-PFC-C1-B17-B20.sky.zip2024-02-14 14:48:381889410
ZipChip_HR_Metabolomics_2024Protocol_2024-02-05_17-24-05.sky.zip2024-02-05 14:24:28100821594
22AminoAcids_Fully13CLabeled_2024-01-29_14-30-52.sky.zip2024-01-29 11:32:1410444936
RBD_M_Glyco_2024-01-25_15-29-41.sky.zip2024-01-26 17:23:2672923972,3829
20240104_Neg_FMT_MCBAs_isoRemove_Cleaned_Final_2024-01-25_21-40-19.sky.zip2024-01-26 16:43:471010030056
20231220_Neg_FMT_BA_Full_reduce_Res50_High_final_2024-01-04_15-44-59.sky.zip2024-01-26 16:43:47405112176
P179_UNCSet1_ACE_v0p3_2024-01-24_22-42-18.sky.zip2024-01-24 19:51:4423034963724
P179_UNCSet2_ACE_v0p3_2024-01-24_22-37-25.sky.zip2024-01-24 19:40:1117021336726
New_iRBD2024-01-15 23:30:5233474794292
Paired_CSF_Plasma_Serum2024-01-15 23:30:523347479460
Initial_Targeted_Proteomics2024-01-15 23:30:5233474794441
TPAD_VL_CSF_PRTC_APOA1_2024-01-07_23-01-46.sky.zip2024-01-07 23:08:493464642412
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173_peptides_iRTs_chromatogram_library_2023-12-22_00-47-19.sky.zip2023-12-22 01:06:36311833561,0822
Figure_8B_Freiburg_ALG1-CDG-Patients_Comparison_2023-12-22_02-34-55.sky.zip2023-12-22 01:06:2022691284006
Figures_4_5_6_7_8A_Heidelberg_CDG-Patients_2023-12-22_02-32-43.sky.zip2023-12-22 01:06:20206712439014
Figure_S5_Freiburg_ALG11_I-CDG_Natural_Variant_2023-12-22_01-59-41.sky.zip2023-12-22 01:06:2021112146
Figure_9_Freiburg_ALG11_I-CDG_Natural_Variant_2023-12-22_01-53-52.sky.zip2023-12-22 01:06:2021418404
Figures_3_and_S3_HEK_293T_Fibroblasts_HeLa_2023-12-22_01-03-03.sky.zip2023-12-22 01:06:2023701303989
20210301 Calibration Dev_DilutionOil_2023-12-11_10-57-35.sky.zip2023-12-20 00:34:263482654
20210607 Calibration Curve_DilutionDigest_2023-12-11_10-50-40.sky.zip2023-12-20 00:34:2634824108
20210212 Low range exploration 140K-fragmod_Pub_2023-12-08_16-04-13.sky.zip2023-12-20 00:34:263482456
HeatedOilSpike-LowTemp_HighTemp_Combined_Final_2022-05-26_12-00-47.sky.zip2023-12-20 00:34:26591548204
20200715_PeptideSpecificity_SignalRatio_2022-05-25_16-33-02.sky.zip2023-12-20 00:34:2611202212044
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SARSCov2_CHAPS_2023-08-10_17-09-26.sky.zip2023-10-19 19:19:3311241
ARIH2 is a Vif-dependent regulator of CUL5-mediated APOBEC3G degradation in HIV infection
  • Organism: Human immunodeficiency virus 1, Homo sapiens
  • Instrument: TSQ Quantiva
  • SpikeIn: No
  • Keywords: Host-virus interactions, ARIH2, HIV, vif, CUL5, AP-MS, APOBEC3G
  • Submitter: Ruth Huttenhain
Abstract
The Cullin-RING E3 ligase (CRL) family is commonly hijacked by pathogens to redirect the host ubiquitin proteasome machinery to specific targets. During HIV infection, CRL5 is hijacked by HIV Vif to target viral restriction factors of the APOBEC3 family for ubiquitination and degradation. Here, using a quantitative proteomics approach, we identify the E3 ligase ARIH2 as a regulator of CRL5-mediated APOBEC3 degradation. The CUL5Vif/CBFß complex recruits ARIH2 where it acts to transfer ubiquitin directly to the APOBEC3 targets. ARIH2 is essential for CRL5- dependent HIV infectivity in primary CD4+ T cells. Furthermore, we show that ARIH2 cooperates with CRL5 to prime other cellular substrates for polyubiquitination, suggesting this may represent a general mechanism beyond HIV infection and APOBEC3 degradation. Taken together, these data identify ARIH2 as a co-factor in the Vif-hijacked CRL5 complex that contributes to HIV infectivity and demonstrate the operation of the E1-E2-E3/E3-substrate ubiquitination mechanism in a viral infection context.
Experiment Description
We generated three stable Jurkat T cell lines, each expressing a tetracycline-inducible affinity-tagged version of CUL5, ELOB, and CBFß. Cells expressing the tagged proteins as well as parental Jurkat T cells were subjected to infection with replication-deficient, Vesicular Stomatitis Virus Glycoprotein (VSVg) pseudotyped HIV-1 NL4-3 virus, a Vif-deficient version of the same virus strain (HIV ∆Vif), or a mock serving as a non-infection condition (mock). Following 24h of infection, anti-FLAG immune complexes were purified and subjected to global, quantitative analysis by MS. Specific interactors of the three bait proteins were determined using SAINT high confidence interactor scoring by comparing affinity purifications from bait-expressing versus parental Jurkat T cells. Proteins with a false discovery rate (FDR) below 0.15 were subsequently validated using a targeted proteomics approach, which allows for accurate, reproducible and consistent quantification across samples and conditions.
Created on 6/28/19, 11:11 PM