open access publication

Article, 2024

Structural and mechanistic insights into Quinolone Synthase to address its functional promiscuity

Communications Biology, ISSN 2399-3642, Volume 7, 1, Page 566, 10.1038/s42003-024-06152-2

Contributors

Vijayanathan, Mallika 0000-0001-9806-3736 [1] [2] Vadakkepat, Abhinav Koyamangalath 0000-0001-8202-7757 [3] [4] Mahendran, Kozhinjampara Radhakrishnan [1] Sharaf, Abdoallah Aboelnasr 0000-0002-3436-9290 [5] [6] Frandsen, Kristian Erik Høpfner 0000-0002-7136-9820 [2] Bandyopadhyay, Debashree [7] Pillai, Madhavan Radhakrishna [1] Soniya, Eppurath Vasudevan (Corresponding author) [1]

Affiliations

  1. [1] Rajiv Gandhi Centre for Biotechnology
    2. [NORA names: India; Asia, South];
  2. [2] University of Copenhagen
    3. [NORA names: KU University of Copenhagen; University; Denmark; Europe, EU; Nordic; OECD];
  3. [3] Indian Institute of Science Bangalore
    4. [NORA names: India; Asia, South];
  4. [4] University of Leicester
    5. [NORA names: United Kingdom; Europe, Non-EU; OECD];
  5. [5] Ain Shams University
    6. [NORA names: Egypt; Africa];

Abstract

Quinolone synthase from Aegle marmelos (AmQNS) is a type III polyketide synthase that yields therapeutically effective quinolone and acridone compounds. Addressing the structural and molecular underpinnings of AmQNS and its substrate interaction in terms of its high selectivity and specificity can aid in the development of numerous novel compounds. This paper presents a high-resolution AmQNS crystal structure and explains its mechanistic role in synthetic selectivity. Additionally, we provide a model framework to comprehend structural constraints on ketide insertion and postulate that AmQNS’s steric and electrostatic selectivity plays a role in its ability to bind to various core substrates, resulting in its synthetic diversity. AmQNS prefers quinolone synthesis and can accommodate large substrates because of its wide active site entrance. However, our research suggests that acridone is exclusively synthesized in the presence of high malonyl-CoA concentrations. Potential implications of functionally relevant residue mutations were also investigated, which will assist in harnessing the benefits of mutations for targeted polyketide production. The pharmaceutical industry stands to gain from these findings as they expand the pool of potential drug candidates, and these methodologies can also be applied to additional promising enzymes.

Keywords

Aegle, Aegle marmelos, acridone, acridone compounds, benefits, benefits of mutations, candidates, compounds, concentration, constraints, core substrate, crystal structure, development, diversity, drug candidates, electrostatic selectivity, entrance, enzyme, findings, framework, functional promiscuity, implications, industry, insertion, interaction, ketide, malonyl-CoA concentration, methodology, model, modeling framework, molecular underpinnings, mutations, novel compound, pharmaceutical industry, polyketide products, polyketide synthase, pool, potential drug candidates, potential implications, presence, production, promiscuity, quinolone synthase, quinolones, research, residue mutations, residues, selection, specificity, structural constraints, structure, substrate, substrate interactions, synthase, synthesis, synthetic diversity, synthetic selection, type, type III polyketide synthase, underpinnings

Funders

  • Department of Biotechnology
  • Novo Nordisk Foundation
  • Council of Scientific and Industrial Research
  • The Velux Foundations

Data Provider: Digital Science

LINKS
-

Matching Records in NORA

SUBJECTS
+

METRICS
+