Catalytic site mutations confer multiple states of G protein activation.

Heterotrimeric guanine nucleotide-binding proteins (G proteins) that function as molecular switches for cellular growth and metabolism are activated by GTP and inactivated by GTP hydrolysis. In uveal melanoma, a conserved glutamine residue critical for GTP hydrolysis in the G protein α subunit is often mutated in Gαq or Gα11 to either leucine or proline. In contrast, other glutamine mutations or mutations in other Gα subtypes are rare. To uncover the mechanism of the genetic selection and the functional role of this glutamine residue, we analyzed all possible substitutions of this residue in multiple Gα isoforms. Through cell-based measurements of activity, we showed that some mutants were further activated and inactivated by G protein-coupled receptors. Through biochemical, molecular dynamics, and nuclear magnetic resonance-based structural studies, we showed that the Gα mutants were functionally distinct and conformationally diverse, despite their shared inability to hydrolyze GTP. Thus, the catalytic glutamine residue contributes to functions beyond GTP hydrolysis, and these functions include subtype-specific, allosteric modulation of receptor-mediated subunit dissociation. We conclude that G proteins do not function as simple on-off switches. Rather, signaling emerges from an ensemble of active states, a subset of which are favored in disease and may be uniquely responsive to receptor-directed ligands.

Molecular annotation of G protein variants in a neurological disorder.

Heterotrimeric G proteins transduce extracellular chemical messages to generate appropriate intracellular responses. Point mutations in GNAO1, encoding the G protein αo subunit, have been implicated in a pathogenic condition characterized by seizures, movement disorders, intellectual disability, and developmental delay (GNAO1 disorder). However, the effects of these mutations on G protein structure and function are unclear. Here, we report the effects of 55 mutations on Gαo conformation, thermostability, nucleotide binding, and hydrolysis, as well as interaction with Gßγ subunits, receptors, and effectors. Our effort reveals four functionally distinct groups of mutants, including one group that sequesters receptors and another that sequesters Gßγ, both acting in a genetically dominant manner. These findings provide a more comprehensive understanding of disease-relevant mutations and reveal that GNAO1 disorder is likely composed of multiple mechanistically distinct disorders that will likely require multiple therapeutic strategies.

Diastereoselective alkylation reactions of 1-methylcyclohexa-2,5-diene-1-carboxylic acid.

The deprotonation and alkylation of 1-methylcyclohexa-2,5-diene-1-carboxylic acid has been investigated under a range of conditions. In all cases, the formation of compounds 14 was found to be completely stereoselective, although compound 14c was formed as an impurity when alkyl iodides were used as electrophiles, and doubly-alkylated compounds 17 were formed in some cases when alkyl bromides were used.

Ammonium treatments to suppress toxic blooms of Prymnesium parvum in a subtropical lake of semi-arid climate: results from in situ mesocosm experiments.

Prymnesium parvum is a haptophyte alga that forms toxic, fish-killing blooms in a variety of brackish coastal and inland waters. Its abundance and toxicity are suppressed by ammonium additions in laboratory cultures and aquaculture ponds. In a cove of a large reservoir (Lake Granbury, Texas, USA) with recurring, seasonal blooms of P. parvum, ammonium additions were tested in mesocosm enclosures for their ability to suppress blooms and their effects on non-target planktonic organisms. One experiment occurred prior to the peak abundance of a P. parvum bloom in the cove, and one encompassed the peak abundance and decline of the bloom. During 21-day experiments, weekly doses raised ammonium concentrations by either 10 or 40 µM. The added ammonium accumulated in experimental mesocosms, with little uptake by biota or other losses. Effects of ammonium additions generally increased over the course of the experiments. The higher ammonium dose suppressed the abundance and toxicity of P. parvum. The biomass of non-haptophyte algae was stimulated by ammonium additions, while positive, negative and neutral effects on zooplankton taxa were observed. Low ammonium additions insufficient to control P. parvum exacerbated its harmful effects. Our results indicate a potential for mitigating blooms of P. parvum with sufficient additions of ammonium to coves of larger lakes. However, factors excluded from mesocosms, such as dilution of ammonium by water exchange and sediment ammonium uptake, could reduce the effectiveness of such additions, and they would entail a risk of eutrophication from the added nitrogen.