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Biofilm formation stages

Biofilm formation stages

Biofilm formation stages

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Initial Attachment - The First Handshake

  • Planktonic (free-floating) bacteria approach a submerged surface, often pre-conditioned by host-derived molecules (e.g., fibronectin, saliva).
  • Initial adhesion is weak and reversible, mediated by physicochemical forces:
    • van der Waals forces
    • Electrostatic interactions
    • Hydrophobic interactions
  • Bacterial appendages like fimbriae, pili, and flagella play a key role in overcoming repulsive forces and initiating contact.

Biofilm formation stages

⭐ Surface conditioning is critical; on intravenous catheters, host proteins like fibronectin coat the plastic, creating a perfect docking site for pathogens like S. aureus.

Maturation - Building the Slime Fortress

  • EPS Matrix Secretion: Bacteria ramp up production of the Extracellular Polymeric Substance (EPS), the "slime" that forms the biofilm's architecture.

    • Components: Polysaccharides, proteins, lipids, and extracellular DNA (eDNA).
    • 📌 People Prefer Large Estates (Polysaccharides, Proteins, Lipids, eDNA).
    • Function: Provides structural stability, adhesion, and protection from host defenses and antimicrobials.
  • Structural Development:

    • Microcolonies grow and merge, forming complex, three-dimensional structures.
    • Characteristic mushroom- or tower-like structures emerge, separated by water channels.
    • These channels allow for nutrient delivery, waste removal, and communication.

High-Yield: The dense, negatively charged EPS matrix is a primary mechanism of antibiotic resistance. It physically blocks antibiotic penetration and can bind and inactivate charged antimicrobial molecules.

  • Quorum Sensing (QS) Coordination: Cell-to-cell communication via QS orchestrates the expression of genes required for matrix production and mature biofilm architecture.

Biofilm Formation Stages

Dispersal - The Great Escape

Final stage of the biofilm life cycle, enabling bacteria to escape and colonize new surfaces. This transition from a sessile to a planktonic (free-swimming) state is crucial for the spread of chronic infections.

  • Triggers:
    • Nutrient depletion or accumulation of toxic byproducts.
    • Quorum sensing signals reaching a critical threshold.
  • Mechanism:
    • Enzymatic degradation of the extracellular polymeric substance (EPS) matrix.
    • Key enzymes: DNases, proteases, and glycoside hydrolases like dispersin B.
  • Outcome:
    • Release of motile bacteria.
    • Seeding of infection at distant sites.

High-Yield: Pseudomonas aeruginosa, a major pathogen in cystic fibrosis, uses quorum sensing not just for biofilm formation but also to precisely time the release of cells for dispersal, promoting systemic infection.

Biofilm formation, maturation, and dispersion cycle

High‑Yield Points - ⚡ Biggest Takeaways

  • Reversible attachment of free-floating planktonic bacteria to a surface is the initial step.
  • This is followed by irreversible attachment via adhesins, leading to microcolony formation.
  • Quorum sensing (cell-to-cell communication) coordinates gene expression and maturation.
  • The Extracellular Polymeric Substance (EPS) matrix provides structural integrity and protection.
  • The EPS matrix is a primary driver of antibiotic resistance and shields from host defenses.
  • Dispersion allows bacteria to detach and colonize new sites, spreading infection.

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