BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Obesity, Pancreas, Personalized medicine, Rosiglitazone, rs4950928, ERBB2)
Bookmark Forward

Thiopurine Prodrugs Mediate Immunosuppressive Effects by Interfering with Rac1 Protein Function.

Jin-Young Shin, Michael Wey, Hope G Umutesi, Xiangle Sun, Jerry Simecka, Jongyun Heo

The Journal of biological chemistry 2016 Jun 24


filter terms:
  • adduct (4)
  • amino acid motifs (1)
  • CD28 (1)
  • CD3 (1)
  • CD4 (1)
  • cdc42 (5)
  • GTP (4)
  • gtpase (2)
  • humans (1)
  • other organ cells (1)
  • performs role (1)
  • prodrugs (4)
  • protein human (1)
  • Rac1 (13)
  • rac1 protein (3)
  • Rho GTPases (4)
  • RhoA (5)
  • RhoGAP (2)
  • RhoGEF (2)
  • suggest (1)
  • t lymphocytes (4)
  • thionucleosides (2)
    • Sizes of these terms reflect their relevance to your search.

    6-Thiopurine (6-TP) prodrugs include 6-thioguanine and azathioprine. Both are widely used to treat autoimmune disorders and certain cancers. This study showed that a 6-thioguanosine triphosphate (6-TGTP), converted in T-cells from 6-TP, targets Rac1 to form a disulfide adduct between 6-TGTP and the redox-sensitive GXXXXGK(S/T)C motif of Rac1. This study also showed that, despite the conservation of the catalytic activity of RhoGAP (Rho-specific GAP) on the 6-TGTP-Rac1 adduct to produce the biologically inactive 6-thioguanosine diphosphate (6-TGDP)-Rac1 adduct, RhoGEF (Rho-specific GEF) cannot exchange the 6-TGDP adducted on Rac1 with free guanine nucleotide. The biologically inactive 6-TGDP-Rac1 adduct accumulates in cells because of the ongoing combined actions of RhoGEF and RhoGAP. Because other Rho GTPases, such as RhoA and Cdc42, also possess the GXXXXGK(S/T)C motif, the proposed mechanism for the inactivation of Rac1 also applies to RhoA and Cdc42. However, previous studies have shown that CD3/CD28-stimulated T-cells contain more activated Rac1 than other Rho GTPases such as RhoA and Cdc42. Accordingly, Rac1 is the main target of 6-TP in activated T-cells. This explains the T-cell-specific Rac1-targeting therapeutic action of 6-TP that suppresses the immune response. This proposed mechanism for the action of 6-TP on Rac1 performs a critical role in demonstrating the capability to design a Rac1-targeting chemotherapeutic agent(s) for autoimmune disorders. Nevertheless, the results also suggest that the targeting action of other Rho GTPases in other organ cells, such as RhoA in vascular cells, may be linked to cytotoxicities because RhoA plays a key role in vasculature functions. © 2016 by The American Society for Biochemistry and Molecular Biology, Inc.

    Citation

    Jin-Young Shin, Michael Wey, Hope G Umutesi, Xiangle Sun, Jerry Simecka, Jongyun Heo. Thiopurine Prodrugs Mediate Immunosuppressive Effects by Interfering with Rac1 Protein Function. The Journal of biological chemistry. 2016 Jun 24;291(26):13699-714

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 27189938

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.