# Small-molecule membrane interactions as a driver of bacterial outer membrane vesicle biogenesis across species

> **NIH NIH R15** · STATE UNIVERSITY OF NY,BINGHAMTON · 2020 · $448,200

## Abstract

Abstract
Gram-negative pathogens use outer membrane vesicles (OMVs) to kill host cells and competitors, avoid and
interfere with the immune response, transfer antibiotic resistance genes, sequester and destroy antibiotics, and
traffic both cell-to-cell communication signals and small RNAs. Despite their direct contribution to so many
pathogenesis-related behaviors, our understanding of how OMVs are produced remains surprisingly incomplete.
Several models of OMV biogenesis have been proposed using different organisms and identifying inputs from
varying cellular pathways. Our team studies OMV biogenesis at the molecular level and uses this approach to
discover features that drive OMV formation regardless of the input signal. Our Bilayer-Couple model describes
how intercalation of a self-produced small molecule preferentially into the outer leaflet of the membrane causes
it to expand relative to the inner leaflet and thereby induce membrane curvature. This framework can already
explain models that have subsequently been put forth in other species. This proposal aims to unify disparate and
species-specific models by expanding our understanding of molecular interactions between small molecule OMV
inducers and outer membrane lipids. We will integrate molecular simulation and physical experiment to discover
the role of chemical variations in controlling molecule-lipid association and curvature induction. We will exploit
our recently developed all-atom molecular dynamics model of the outer membrane to make atomistic-level
predictions about how different molecule derivatives drive curvature induction in membranes with different lipid
chemotypes. Our established experimental approaches for assessing OMV production from different bacterial
species and mutants will be used to test the in silico predictions.
In the context of our recent discovery that many Gram-negative organisms, including important clinical
pathogens, secrete factors to induce cross-species stimulation of OMV production, we will pursue two specific
aims to characterize how variations in the chemical structure of an OMV inducer molecule influences its specific
interactions with different outer membrane lipids that are found across species: (1) Characterize nanoscale
interactions of OMV-inducing factors and molecular derivatives with outer membrane lipids and quantify
membrane response to the interactions in all-atom simulations, (2) Make use of specific mutants and related
species to test the predictions of the in silico model and demonstrate control of OMV biogenesis by small
molecule-lipid interactions in vitro. The findings of the proposed work will help us bring together parallel and
species-specific ideas about OMV biogenesis into a fundamental and robust model that can generalize across
species. We will gain an important understanding about how pathogens interact to manifest negative clinical
consequences and move toward the larger goal of tailoring treatments to disrupt detrimental pa...

## Key facts

- **NIH application ID:** 9880749
- **Project number:** 1R15GM135862-01
- **Recipient organization:** STATE UNIVERSITY OF NY,BINGHAMTON
- **Principal Investigator:** Jeffrey Schertzer
- **Activity code:** R15 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $448,200
- **Award type:** 1
- **Project period:** 2020-06-01 → 2024-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9880749

## Citation

> US National Institutes of Health, RePORTER application 9880749, Small-molecule membrane interactions as a driver of bacterial outer membrane vesicle biogenesis across species (1R15GM135862-01). Retrieved via AI Analytics 2026-05-26 from https://api.ai-analytics.org/grant/nih/9880749. Licensed CC0.

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