Healthcare-Associated MRSA (HA-MRSA) versus Community-Associated MRSA (CA-MRSA) - LabCE.com, Laboratory Continuing Education

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The page below is a sample from the LabCE course Drug-Resistant Superbugs, Multi-drug Resistant Organisms: MRSA, VRE, Clostridioides difficile, and CRE. Access the complete course and earn ASCLS P.A.C.E.-approved continuing education credits by subscribing online.

Learn more about Drug-Resistant Superbugs, Multi-drug Resistant Organisms: MRSA, VRE, Clostridioides difficile, and CRE (online CE course)

Healthcare-Associated MRSA (HA-MRSA) versus Community-Associated MRSA (CA-MRSA)

As mentioned in the course introduction, MRSA infections fall into two general types:

HA-MRSA -Infections that occur in people who are, or have recently been, hospitalized.
CA-MRSA - Infections that are acquired in the community.

Table 1 summarizes a number of factors that distinguish HA-MRSA from CA-MRSA isolates.

Table 1. HA-MRSA vs. CA-MRSA.

Factor	HA-MRSA	CA-MRSA
Origin of strains	Nosocomial infections Five isolates associated with healthcare settings: USA100, -200, -500, -600, -800 USA100 is the predominant isolate while USA 200 is the second most common isolate. USA700 has been isolated in both healthcare and community settings.	Evolved from endemic methicillin-susceptible S. aureus (MSSA) strains. Two clones, USA300 and USA400, are associated with the majority of CA-MRSA infections in the United States. USA300 has emerged as the most prominent clone and is not found among hospital strains.
Genetic lineage	Isolates usually carry large SCCmec types I, II, or III (34-67 kb). The larger size of SCCmec II and III permits the inclusion of other non-beta-lactam resistance genes so that HA-MRSA strains tend to be multi-drug resistant.	Isolates carry a smaller SCCmec variant, predominantly type IV (24 kb), less often type V or variant VT. SCCmec IV (except for mecA) does not permit the inclusion of other non-beta lactam resistance genes so that CA-MRSA isolates exhibit resistance to only methicillin and erythromycin and are more often susceptible to other non-beta lactam antibiotics (e.g., trimethoprim/sulfamethoxazole [SXT] and clindamycin).
Affected population	Largely affects older adults and people with weakened immune systems; those who have undergone surgical procedures are at increased risk.	Healthy persons in the general population without established risk factors for MRSA acquisition.
Clinical syndromes	Found at multiple sites, most commonly bloodstream infections, urinary tract infections (UTI), and respiratory tract infections.	Predominantly skin and soft tissue infections (SSTIs), such as abscesses, cellulitis, folliculitis, and impetigo, and a serious form of pneumonia. Genes for Panton-Valentine leukocidin (PVL) are associated with SCCmec IV; the clinical spectrum of infections caused by CA-MRSA is directly related to the presence of PVL genes, coding for the production of a cytotoxin that causes tissue necrosis and leukocyte destruction.