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MALDI-TOF Mass Spectrometry

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Principle & Basics - Microbial Fingerprinter

  • MALDI-TOF MS (Matrix-Assisted Laser Desorption/Ionization Time-of-Flight Mass Spectrometry): Rapid, accurate microbial identification based on unique protein (mainly ribosomal) profiles.
  • Core Principle: "Soft" ionization of whole microbial cells or extracts, generating a characteristic mass spectrum (fingerprint).
    • Matrix: Sample mixed with matrix (e.g., α-cyano-4-hydroxycinnamic acid); co-crystallizes.
    • Laser Desorption/Ionization: Pulsed laser desorbs and ionizes matrix & sample molecules (mostly singly charged, [M+H]$^+$).
    • Time-of-Flight (TOF) Analyzer: Ions accelerated into a flight tube. Smaller ions travel faster.
      • $t = d \sqrt{m/(2zV)}$, where $t$=time, $d$=distance, $m$=mass, $z$=charge, $V$=voltage.
    • Detector: Records ion arrival times.
    • Mass Spectrum: Plot of ion intensity vs. mass-to-charge ratio (m/z), creating a unique "fingerprint".

MALDI-TOF MS Principle Diagram

⭐ MALDI-TOF MS primarily analyzes ribosomal proteins due to their abundance and conservation within species, yet sufficient variability between species for discrimination. This makes them ideal biomarkers for microbial identification.

Workflow & Steps - Sample to Spectrum

Rapid microbial ID via protein fingerprinting (mainly ribosomal proteins).

  • 1. Sample Prep:
    • Direct Colony Transfer (DCT): Pure colony smeared on MALDI plate.
    • Extraction: For yeasts, mycobacteria; uses formic acid/acetonitrile for protein release.
  • 2. Matrix & Co-crystallization:
    • Sample + Matrix (e.g., HCCA - α-cyano-4-hydroxycinnamic acid).
    • Air-dry: Forms sample-matrix co-crystals.
  • 3. MALDI-TOF MS:
    • Laser Desorption/Ionization: UV laser hits crystals → gas-phase ions (mostly proteins).
    • Ion Acceleration: Electric field accelerates ions into flight tube.
    • Time-of-Flight (TOF): Ions separated by mass-to-charge ($m/z$); smaller ions faster.
  • 4. Spectrum & ID:
    • Mass spectrum generated (peak pattern = fingerprint).
    • Compared to database for species identification.

MALDI-TOF MS workflow for microbial ID

⭐ The most abundant ions detected in MALDI-TOF MS of bacteria are ribosomal proteins, which are conserved yet species-specific, providing a reliable "fingerprint".

Clinical Applications - Microbe ID Ace

  • Core Function: Rapid, precise identification of cultured microorganisms.
    • Bacteria: Wide range (aerobes, anaerobes, Gram +ve/-ve).
    • Yeasts: Common species (e.g., Candida spp.).
    • Filamentous Fungi: Expanding databases.
    • Mycobacteria: With specific extraction protocols.
  • Specimen Versatility:
    • Colonies from culture media (solid/liquid).
    • Directly from positive blood culture broths (crucial for sepsis).
  • Impact on Workflow:
    • Speed: Identification in minutes.
    • Accuracy: High for routine isolates.
    • Efficiency: Reduces reliance on numerous biochemical tests.
  • Developing Frontiers:
    • Rapid Antimicrobial Susceptibility Testing (AST) (e.g., β-lactamase detection).
    • Epidemiological strain typing.

⭐ MALDI-TOF MS enables identification of bacteria and yeasts directly from positive blood cultures, often within 15-30 minutes of a positive signal.

Advantages & Limitations - Balancing Act

  • Advantages:
    • Speed: Rapid ID (minutes vs. hours/days).
    • Accuracy: High for common, well-characterized isolates.
    • Cost-Effective: Low consumable cost; ↓ long-term lab costs.
    • Automation: Suitable for high-throughput workflows.
    • Minimal Sample Prep: Direct colony testing often feasible.
  • Limitations:
    • Database Dependency: Performance relies on database quality & updates.
    • Initial Cost: Significant capital investment.
    • Differentiation: Struggles with closely related species/subspecies.
    • Culture Requirement: Needs isolated colonies, not direct polymicrobial samples.
    • No Susceptibility Data: Cannot provide antimicrobial resistance (AST).

⭐ MALDI-TOF identifies microbes via their unique protein fingerprint, mainly ribosomal proteins.

High‑Yield Points - ⚡ Biggest Takeaways

  • MALDI-TOF MS identifies microbes by analyzing ribosomal protein profiles.
  • It measures the mass-to-charge ratio (m/z) of these proteins.
  • A matrix (e.g., HCCA) is crucial for desorption and ionization.
  • Time-of-Flight (TOF) analyzer separates ions based on their travel time.
  • Enables rapid identification of bacteria and fungi, often to species level.
  • Database comparison of protein spectra is key for identification.
  • Limited for direct specimen analysis; typically requires prior culture.

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