Structures of the PKA RIα holoenzyme with the FLHCC driver J-PKAcα or wild type PKAcα

Cao, Bin; Lu, Tung‐Wu; Fiesco, Juliana A. Martinez; Tomasini, Michael D.; Li, Fan; Simon, Sanford M.; Taylor, Susan S.; Zhang, Ping

doi:10.1101/505347

Cited by 5 publications

(6 citation statements)

References 49 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…3 H and I). Molecule A features an N3A-N3A′ interface similar to what was described earlier in the RIα homodimer (13), and this was also seen in a recent holoenzyme structure with a cancer-driving fusion protein of the C-subunit (45). Hydrophobic and hydrogen bonding interactions both contribute to the N3A-N3A′ interface.…”

Section: Resultssupporting

confidence: 75%

Two PKA RIα holoenzyme states define ATP as an isoform-specific orthosteric inhibitor that competes with the allosteric activator, cAMP

Aoto

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

Protein kinase A (PKA) holoenzyme, comprised of a cAMP-binding regulatory (R)-subunit dimer and 2 catalytic (C)-subunits, is the master switch for cAMP-mediated signaling. Of the 4 R-subunits (RIα, RIβ, RIIα, RIIβ), RIα is most essential for regulating PKA activity in cells. Our 2 RIα2C2 holoenzyme states, which show different conformations with and without ATP, reveal how ATP/Mg2+ functions as a negative orthosteric modulator. Biochemical studies demonstrate how the removal of ATP primes the holoenzyme for cAMP-mediated activation. The opposing competition between ATP/cAMP is unique to RIα. In RIIβ, ATP serves as a substrate and facilitates cAMP-activation. The isoform-specific RI-holoenzyme dimer interface mediated by N3A–N3A′ motifs defines multidomain cross-talk and an allosteric network that creates competing roles for ATP and cAMP. Comparisons to the RIIβ holoenzyme demonstrate isoform-specific holoenzyme interfaces and highlights distinct allosteric mechanisms for activation in addition to the structural diversity of the isoforms.

show abstract

Section: Resultssupporting

confidence: 75%

Two PKA RIα holoenzyme states define ATP as an isoform-specific orthosteric inhibitor that competes with the allosteric activator, cAMP

Aoto

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

show abstract

“…This study is the first to evaluate the therapeutic potential for PRKACA inhibition in FLC. We characterized and validated an FLC PDX mouse model ( 27 (40). In addition, primary and metastatic FLC were shown to be sensitive to clinically available inhibitors of topoisomerase 1 and histone deacetylases, and to napabucasin (41), suggesting these agents as potential therapeutic strategies for FLC.…”

Section: Discussion/conclusionmentioning

confidence: 99%

“…PRKACA is expressed in virtually all tissues and plays a critical role in cardiac function, making a strategy to selectively inhibit DNAJB1-PRKACA while sparing WT PRKACA desirable. The alternative conformation of the holoenzyme containing the DNAJB1-PRKACA fusion protein and the PKA regulatory subunit may constitute a strategy for selectively targeting the activity of the DNAJB1-PRKACA fusion protein (40). In addition, primary and metastatic FLC were shown to be sensitive to clinically available inhibitors of topoisomerase 1 and histone deacetylases, and to napabucasin (41), suggesting these agents as potential therapeutic strategies for FLC.…”

Section: Discussion/conclusionmentioning

confidence: 99%

Evaluation of PRKACA as a Therapeutic Target for Fibrolamellar Carcinoma

Schalm

O’Hearn

Wilson

et al. 2022

Preprint

View full text Add to dashboard Cite

Background & Aims: Fibrolamellar carcinoma (FLC) is a rare, difficult-to-treat liver cancer primarily affecting pediatric and adolescent patients, and for which precision medicine approaches have historically not been possible. The DNAJB1-PRKACA gene fusion was identified as a driver of FLC pathogenesis. We aimed to assess whether FLC tumors maintain dependency on this gene fusion and determine if PRKACA is a viable therapeutic target. Methods: FLC patient-derived xenograft (PDX) shRNA cell lines were implanted subcutaneously into female NOD-SCID mice and tumors were allowed to develop prior to randomization to doxycycline (to induce knockdown) or control groups. Tumor development was assessed every 2 days. To assess the effect of treatment with novel selective PRKACA small molecule kinase inhibitors, BLU0588 and BLU2864, FLC PDX tumor cells were implanted subcutaneously into NOD-SCID mice and tumors allowed to develop. Mice were randomized to treatment (BLU0588 and BLU2864, orally, once daily) or control groups and tumor size determined as above. Results: Knockdown of DNAJB1-PRKACA reversed a FLC-specific gene signature and reduced PDX tumor growth in mice compared to the control group. Furthermore, FLC PDX tumor growth was significantly reduced with BLU0588 and BLU2864 treatment versus control (P = 0.003 and P = 0.0005, respectively). Conclusions: We demonstrated, using an inducible knockdown and small molecule approaches, that FLC PDX tumors were dependent upon DNAJB1-PRKACA fusion activity. In addition, this study serves as a proof-of-concept that PRKACA is a viable therapeutic target for FLC and warrants further investigation.

show abstract

“…From the stability essays, ATP binding assays and the studies of the kinetics, the fusion tetramer did not differ significantly from the wild-type tetramer. The addition of the J domain might create more interaction surfaces with other proteins 75 .…”

Section: Allostery In the Pka R2c2 Heterotetramer Complexmentioning

confidence: 99%