What are the main challenges?

Engineered probiotics holds broad prospects for treating human diseases. The field faces several key challenges:

  • Lacks a  unified and  standardized  development workflow.
  • Efforts remain  fragmented ,  experience-dependent , and  difficult to reproduce .
Final consequence: Significantly slows the translation of innovative therapies from lab to clinic.

Our story unfolds in three parts:

Platform Design
PD Treatment
Wet-Lab Execution
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Building the ProbiEase
Architecture and Development Pipeline

The Closed-Loop Paradigm

We adopted an evidence-based closed-loop paradigm.

We first developed basic and professional versions of a Q&A system. Using Node.js, we built a web-based interactive interface that supports retrieval and explanation of domain-specific questions, thereby enabling online data querying and AI-assisted Q&A services on a unified platform. This provided an innovative approach for "disease-probiotic" association analysis.

1. Raw Data

Gathering 211 bacterial strains

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During the data collection phase, we internally compiled and integrated data on edible probiotics, gathering 211 bacterial strains. In the data cleaning process, we strictly adhered to the principle of evidence prioritization, first evaluating each strain's safety for consumption, potential benefits, and relevance to target diseases. We then systematically searched professional literature databases such as PubMed, selecting only entries with clear theoretical foundations and peer-reviewed evidence while excluding records lacking reliable support. This minimized bias and ensured high credibility and traceability of the data.

2. Literature Support

(1) Extracted "strain-disease" relationships from papers → The knowledge graph
(2) used gutSMASH and antiSMASH → predict the static metabolic potential and specialized pathways
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In the subsequent data processing and functional annotation stage, we extracted "strain-disease" relationships from papers to lay the foundation for node connections in the knowledge graph. Additionally, we used tools such as gutSMASH and antiSMASH to predict the static metabolic potential and specialized pathways of the strains. We also integrated professional databases to supplement phylogenetic, phenotypic, and safety information, thereby forming comprehensive functional profiles of the strains.

3. Database Construction

We constructed a structured triple database centered on "strain-disease-paper" as the knowledge foundation for the ProbiEase online Q&A platform. This database supports both the general retrieval and the professional version.

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Based on this, we constructed a structured triple database centered on "strain-disease-paper" as the knowledge foundation for the AI-PPDD online Q&A platform. This database supports both the general retrieval and interpretation functions of the basic version and the evidence strength evaluation, mechanism inference, and comparative analysis of solutions in the professional version. It also enables bidirectional queries, allowing users to "search for diseases by strain" and "search for strains by disease." In practical applications, our system can provide targeted inquiries and recommendations from diseases to strains, outputting literature-verified candidate strain sets along with their potential mechanisms of action. It clearly specifies applicable scopes and uncertainties, delivering comprehensive professional responses to queries.

4. Modeling & Simulation

We employed dFBA methods to simulate community dynamics of candidate strains.

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Subsequently, we employed dFBA methods to simulate community dynamics of candidate strains, quantitatively analyzing resource competition, metabolic interactions, and potential conflicts to evaluate the feasibility of co-culture. This provided parameter guidance for designing combination strategies and optimizing experimental conditions, thereby preemptively excluding high-risk options at the computational level and prioritizing pathways with strong synergistic potential.

5. Experimental Validation

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We validated co-culture of the two engineered strains and made a preliminary assessment of their coexistence using fluorescence-based cell counting. Targeting Parkinson’s disease as the indication, we further modularized and engineered the consortium to enhance therapeutic performance: strengthening target-specific colonization, increasing therapeutic output, implementing division-of-labor control between strains, and incorporating biosafety safeguards to prevent escape.
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The Application of the ProbiEase
Addressing the Parkinson's Challenge

Characteristics of Parkinson's Disease

  • A  neurodegenerative  disease
  • Progresses  slowly  and silently
  • Mainly attacks the body's  motor system 
  • Particularly plagues  elderly groups 
  • The morbidity and mortality situation is  grim 
Strategy 1
Current Approach
Oral Administration
  • Convenient and non-invasive
  • High patient compliance
  • Applicable to various PD drugs
  • Blood-brain barrier
  • First-pass hepatic metabolism
  • Frequent dosing
Strategy 2
Alternative Route
Intranasal Delivery
  • Bypassing the blood-brain barrier
  • Rapid onset of action
  • Efficient absorption
  • Short residence time
  • Unstable and poorly sustained drug levels
  • Low targeting specificity
Strategy 3
Our Solution
Intranasal Delivery of Engineered Probiotics

More than just:

  • Convenient and non-invasive
  • High patient compliance
  • Applicable to various PD drugs
  • Bypassing the blood-brain barrier
  • Rapid onset of action
  • Efficient absorption

We further added:

  • Precise Targeting
  • Sustained and Controlled Drug Release
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Implement of Our ProbiEase
Engineered Nasal Probiotics for Brain-Targeted Therapy.

Overview

We introduce a novel therapeutic strategy for Parkinson's Disease based on a three-strain nasal-adhesive probiotic consortium comprising two engineered starins of E. coli Nissle 1917 and one Lactiplantibacillus plantarum WCFS1. These strains were co-engineered with four functional modules that enable sustained release of two therapeutic molecules and promote colonization of the nasal mucosa.

1. Adhesion Module

Enables stable consortium residence in the nasal cavity.

(1) Utilizes the OppA protein for specific host receptor binding.
(2) Enhances bacterial cohesion via an antigen-antibody system, forming a robust community.
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2. Drug Delivery Module

Enables local synthesis of Parkinson's therapeutics.

(1) Produces L-DOPA to replenish dopamine levels in the brain.
(2) Simultaneously delivers glutathione to combat oxidative stress and protect neurons.
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3. Control Module

Achieves on-demand drug release via bacterial communication.

(1) Establishes a cross-species signaling circuit using AHL and AIP.
(2) Tightly couples therapeutic production with successful colonization.
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4. Safety Module

Incorporates multiple biocontainment strategies for enhanced safety.

(1) Includes thermo- and hypoxia-sensitive suicide switches to prevent escape.
(2) Features an inducible kill switch as an emergency brake.
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DETAILS - Adhesion Module
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Adhesion Module
DETAILS - Drug Delivery Module
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Drug Delivery Module
DETAILS - Control Module
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Control Module
DETAILS - Safety Module
Explore Our Design
Safety Module
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