Sphingomonas paucimobilis-Introduction, Morphology, Pathogenicity, Lab Diagnosis, Treatment, Prevention, and Keynotes
Sphingomonas paucimobilis colony morphology on CLED agar
Introduction
Table of Contents
Sphingomonas paucimobilis (formerly classified as Pseudomonas paucimobilis) is a strictly aerobic, non-fermenting, Gram-negative bacillus. It is an environmental oligotroph found widely in soil and water systems. It serves as a stealthy opportunistic pathogen in clinical settings. It can survive in nutrient-poor conditions and form robust biofilms in hospital water networks, on medical equipment, and in dialysis solutions.
Morphology and Characteristics
Cell Morphology
Gram Stain: Gram-negative straight or slightly curved rod cells.
Size: Small, measuring approximately 0.7 × 1.4 μm.
Motility: Slowly motile via a single polar flagellum (the species name “paucimobilis” denotes its limited motility).
Spores: Non-spore-forming.
Cultural and Biochemical Profiles
Colony Appearance: Characterized by yellow-pigmented colonies due to carotenoid pigments when grown on non-selective media like blood or chocolate agar.
Selective Media: It does not grow on MacConkey agar or standard enterobacterial selective media.
Temperature: Grows optimally at 30°C to 37°C but fails to grow at 5°C or 42°C.
Fig. Sphingomonas paucimobilis colony morphology on CLED agar
Cell Envelope Novelty
No Lipopolysaccharide (LPS): Unlike typical Gram-negative rods, it lacks endotoxic LPS in its outer membrane.
Glycosphingolipids (GSL): It replaces LPS with sphingolipids/glycosphingolipids. This reduces its endotoxic potential but alters how it interacts with human immune cells.
Pathogenicity and Clinical Features
Low Virulence: Because it lacks traditional endotoxins, it triggers a weaker inflammatory response, resulting in a favorable prognosis and lower mortality rates.
Target Populations: Primarily affects immunocompromised individuals, individuals with chronic diseases (e.g., diabetes, kidney disease), or hospitalized patients with indwelling medical hardware.
Associated Infections:
Bacteremia and Septicemia: Frequently traced to contaminated IV fluids, medications, or catheter lines.
Catheter-Related Infections: Driven by strong biofilm attachment capabilities.
Other Presentations: Peritonitis (especially in peritoneal dialysis), meningitis, septic arthritis, osteomyelitis, and ventilator-associated pneumonia.
Laboratory Diagnosis
Specimen Collection: Blood, cerebrospinal fluid (CSF), peritoneal fluid, sputum, urine, or catheter tips depending on symptoms.
Microscopy: Direct Gram-stain shows Gram-negative rods, but further testing is required since it looks identical to other bacilli.
Culture: Inoculated onto blood or chocolate agar; checked for smooth, circular, yellow-pigmented colonies after 24–48 hours.
Biochemical Identification: Identification via API 20NE (Non-Enteric) strips or conventional phenotypic systems tracking its oxidase/catalase positivity.
Advanced Identification (Gold Standard): Identification is best achieved using MALDI-TOF Mass Spectrometry or 16S rRNA gene sequencing to differentiate it accurately from other non-fermenters.
Treatment
There are no definitive international guidelines for S. paucimobilis; management relies entirely on individualized, in-vitro susceptibility profiling.
Preferred Antibiotic Classes
Fluoroquinolones: Options like Ciprofloxacin or Levofloxacin show high efficacy.
Carbapenems & Carbapenem combinations: Meropenem and Imipenem are highly effective for severe infections or septic presentations.
Beta-lactamase Combinations: Piperacillin-tazobactam functions reliably against many clinical strains.
Aminoglycosides & TMP-SMX: Often show strong in vitro action.
Resistance Red Flags
Intrinsic Resistance: Strains produce chromosomally encoded beta-lactamases, rendering them inherently resistant to penicillins and first-generation cephalosporins.
Multidrug Resistance (MDR): Emerging isolates demonstrate resistance to colistin, aminoglycosides, or third-generation cephalosporins.
Source Control
If the infection stems from an indwelling device (e.g., CVCs, implants), complete removal of the hardware is critical to bypass the protective bacterial biofilm.
Prevention
Water System Monitoring: Implement routine chlorination, filtration, and microbiological surveillance of hospital tap water, distilled water lines, and hemodialysis loops.
Sterile Fluid Protocols: Strict quality control during the preparation and compounding of multi-dose sterile drug solutions (like IV fentanyl or saline flushes).
Disinfection of Equipment: Rigorous maintenance and sterilization of mechanical ventilators, nebulizers, and endoscopes.
Catheter Care: Adherence to aseptic techniques during central and peripheral venous line insertion and maintenance.
Keynotes
Signature Feature: Unique Gram-negative outer envelope lacking Lipopolysaccharide (LPS), replacing it with glycosphingolipids.
Visual Clue: Produces distinctive yellow-pigmented colonies on standard blood agar, but fails to grow on MacConkey agar.
Niche: An oligotrophic organism that thrives in low-nutrient, aqueous hospital environments by building resilient biofilms.
Clinical Outlook: Acts as an opportunistic pathogen with low virulence; while invasive cases do occur, mortality directly attributable to this bacterium remains exceedingly rare.