361: Chiral Inversion Mutagenesis Reveals Structured Hotspots in LCDs

Beckner RL et al., PNAS - This episode examines a PNAS study using Chiral Inversion Mutagenesis (ChIM) to scan low-complexity domains (LCDs) of Emerin and neurofilament light chain (NEFL). Targeted L-to-D amino acid inversions reveal position-dependent, chirality-sensitive hotspots that control LCD self-association. Key terms: chiral inversion, low-complexity domains, Emerin, neurofilament light chain, synthetic protein chemistry. Study Highlights:The authors applied synthetic protein chemistry to introduce site-specific L-to-D Cα inversions (ChIM) in LCDs of Emerin (EMD) and NEFL. ChIM scans identified discrete enantioselective hotspots—EMD residues ~191–203 and NEFL residues ~22–41—where D substitutions strongly reduce self-association measured by GST pulldown and turbidity assays. Minimal inversions, including single D substitutions, can abrogate EMD self-association, while an all-D mirror-image C-terminal fragment restored activity, implicating backbone geometry and secondary-structure involvement. These results show that polypeptide homochirality and transient structure underpin certain LCD–LCD interactions. Conclusion:Cα stereochemistry is a determinant of LCD self-association at specific sequence hotspots, and ChIM provides a positional-resolution chemical approach to identify backbone-constrained elements that mediate oligomerization of disordered domains. Music:Enjoy the music based on this article at the end of the episode. Article title:Chiral inversion mutagenesis identifies geometrically constrained residues within self - associating low - complexity domains First author:Beckner RL Journal:PNAS DOI:10.1073/pnas.2535888123 Reference:Beckner RL, Kim L, Carter C, Walterscheid A, Liszczak G. Chiral inversion mutagenesis identifies geometrically constrained residues within self-associating low-complexity domains. Proc Natl Acad Sci U S A. 2026;123(19):e2535888123. doi:10.1073/pnas.2535888123 License:This episode is based on an open-access article published under the Creative Commons Attribution 4.0 International License (CC BY 4.0) – https://creativecommons.org/licenses/by/4.0/ Support:Base by Base – Stripe donations: https://donate.stripe.com/7sY4gz71B2sN3RWac5gEg00 Official website https://basebybase.com On PaperCast Base by Base you'll discover the latest in genomics, functional genomics, structural genomics, and proteomics. Episode link: https://basebybase.com/episodes/chiral-inversion-lcd-hotspots-361 QC:This episode was checked against the original article PDF and publication metadata for the episode release published on 2026-05-08. QC Scope:- article metadata and core scientific claims from the narration- excludes analogies, intro/outro, and music- transcript coverage: Audited the spoken sections describing: ChIM methodology; Emerin LCD hotspot mapping (188–201) with 3×Pro and 3×D scans; single-residue effects (1×D) and all-D mirror-image rescue; NEFL head domain hotspot (22–41) with 5×D scans; assay descriptions (GST pulldown, turbidity); cross-β/anti-selective interactions; drug-de- transcript topics: Chiral inversion mutagenesis (ChIM) methodology; Emerin (EMD) LCD self-association hotspot mapping (188–201) with Pro/ D-inversions; NEFL head domain hotspot mapping (22–41) with 5×D inversions; Mutational scan results: 3×D, 1×D, 5×D variants and effects on pulldown/turbidity; Mirror-image (all-D) fragment rescue for Emerin; Assays: GST pulldown and turbidity measurements QC Summary:- factual score: 10/10- metadata score: 10/10- supported core claims: 7- claims flagged for review: 0- metadata checks passed: 4- metadata issues found: 0 Metadata Audited:- article_doi- article_title- article_journal- license Factual Items Audite...