Prevention and Control of Healthcare-Acquired Infections in the Intensive Care Unit

Mireya Wessolossky

Richard T. Ellison III

Introduction

Preventing healthcare-acquired infections in intensive care units (ICUs) is a daily concern of physicians providing care for critically ill patients. Patients in ICUs are at increased risk for infection for multiple reasons, including their underlying illness, the use of medical devices for organ system support and hemodynamic monitoring, impaired nutritional status that contributes immune function compromise, and ongoing exposure to hospital antibiotic-resistant bacterial flora. The focus of this chapter is to review the general epidemiology of these infections, the factors contributing to their development, preventative strategies, and important characteristics of key healthcare-acquired pathogens.

Epidemiology of Healthcare-Acquired ICU Infections

Studies performed over the last two decades have found that infections in ICU patients are both common and significant. Work by Craven and colleagues in the early 1980s at Boston City Hospital in adult medical and surgical ICUs found that
overall 28% of the patients developed at least one nosocomial infection, and once infected patients had threefold increases in mortality [1]. Similarly, in 1995, European investigators assessed the prevalence of nosocomial infections in a multinational survey of 1,417 ICUs in 17 nations on one single day (the EPIC Study), and found an overall prevalence of ICU-acquired infection of 21% [2]. A more recent study in a single US medical ICU performed over 20 months in 2000 to 2001 found that 42% of patients requiring at least 48 hours of ICU care had a microbiologically confirmed infection, and patients with infection had a 1.9-fold increased risk of in-hospital mortality (p < 0.001) [3].

The types of infection seen in ICU patients have varied slightly over time and between types of ICU units, but several types of infections have predominated. In the Boston City Hospital study, the incidence of infections was higher in surgical ICU than in medical ICU patients; and pneumonia, surgical wound infections, urinary tract infections (UTIs), and bloodstream infections (BSIs) were the most frequent infections [1]. In the European Prevalence of Infection in Intensive Care (EPIC) study, the principal infections identified were ventilator-associated pneumonia (47% of infections), tracheobronchitis (18%), UTI (18%), and bacteremias (12%) [2]. Klevens and others, using a multistep approach, estimated 394,288 hospital-associated infections among adults and children in ICU in 2002 from US hospitals. The infection rate per 1,000 patient-days was 13.0: among all, UTI was the highest (3.38) followed by pneumonia (3.33) and BSI (2.71) [4]. The use of medical devices is a predominant cause of infection with the majority of episodes of nosocomial pneumonia associated with mechanical ventilation, healthcare-acquired infection (HAI) UTIs associated with urinary catheterization, and primary BSIs linked to central venous catheters.

Additional data through the National Nosocomial Infection Surveillance (NNIS) system of the Centers for Disease Control and Prevention (CDC) has assessed nosocomial infections in differing types of ICUs, and found that trauma/surgical and neurosurgical ICUs tend to have more nosocomial pneumonia than medical or coronary care ICUs; and that pediatric, trauma, and burn ICUs have more BSIs than medical ICUs [5,6]. The differences in infection rates noted are likely related to the size of the unit (small vs. large), the type of more predominant device use (urinary catheters, endotracheal tubes, and vascular catheters), the age group of the patients (pediatric vs. adults), and the most predominant illness of the patients (coronary, surgical, burn, medical, and pediatric).

Pediatric intensive care units differ from adult ICUs in many ways. First, they are typically combined units (medical and surgical). Second, their beds are not commonly physically separated as adults ICU beds. Third, pediatric patients usually have less comorbidity than adults. Data from the CDC NNIS system during the years 1992 through 1997 found a mean overall patient infection rate of 6.1%, with the principal infections being venous catheter–associated BSIs, followed by pneumonia and UTIs [6].

Microbiology of ICU Infections

The predominant causes of ICU infections are a limited number of bacterial and fungal pathogens. In general, the pathogens that are seen can be characterized as those that survive well in a moist environment (e.g., Gram-negative bacteria including Enterobacter strains, Pseudomonas aeruginosa, and Acinetobacter species), those that colonize the skin and produce biofilm to allow adherence to catheters and other devices (e.g., Staphylococcus aureus and coagulase-negative staphylococci), and those which are resistant to commonly used antibiotics (e.g., methicillin-resistant S. aureus [MRSA], vancomycin-resistant enterococci [VRE], multidrug-resistant Gram-negative bacteria, and Candida species). In the EPIC study, the predominant pathogens were Enterobacteriaceae (34.4%), S. aureus (30.1%), and P. aeruginosa (28.7%) [2]. It was notable that 60% of the S. aureus isolates were MRSA, and that coagulase-negative staphylococci (19.1%) and fungi (17.1%) were common [2]. During the last 12 years, there has been an increasing trend toward highly antibiotic-resistant pathogens in the ICU setting. Data from the NNIS system on US ICUs comparing data from 1998 through 2003 has shown a progressive rise in the prevalence of MRSA to 60%, as well as dramatic increases in the prevalence of Klebsiella strains resistant to third-generation cephalosporins and P. aeruginosa resistant to cephalosporins and imipenem (Fig. 78.1) [5].

In the NNIS pediatric ICU study noted previously, for primary BSIs, coagulase-negative staphylococci were the most common pathogens (38%) followed by Gram-negative bacilli (25%) [6]. For nosocomial pneumonia, P. aeruginosa (22%) was the most frequent pathogen followed by S. aureus (17%), and for UTI, Gram-negative aerobic bacilli were the most frequent pathogens (57%) followed by fungi, most frequently Candida albicans (14%).

In addition to these predominant pathogens, there are several situations where other pathogens are a concern in the ICU. A number of institutions have noted the emergence of extended-spectrum β-lactamases (ESBL) producing Klebsiella and Escherichia coli strains [7,8]. In addition, in a few institutions that have used carbapenems extensively (often to try to treat ESBL-positive Gram-negative bacilli), the carbapenem-resistant Gram-negative pathogens Stenotrophomonas maltophilia, Klebsiella pneumoniae, Acinetobacter baumannii, and Burkholderia cepacia have emerged [9,10,11,12,13]. Finally, the fungal pathogens Candida parapsilosis and Malassezia furfur have been seen in patients receiving total parenteral nutrition, the latter being seen only with lipid supplementation [14,15].

Risk Factors

The length of ICU stay is the predominant risk factor for nosocomial infection followed by the use of medical devices [2,3,6]. In the NNIS surveillance studies and subsequent studies by the CDC’s current National Healthcare Safety Network (NHSN), nosocomial infection rates for nosocomial pneumonia, BSIs, and UTIs have correlated strongly with device use [4,16]. Other risk factors include the patient’s underlying illness, selected medications, and the type of healthcare facility. In the EPIC study, seven risk factors were determined for ICU-acquired infection: increased length of stay (> 48 hours), mechanical ventilation, diagnosis of trauma, central venous, pulmonary artery, urinary catheterization, and stress ulcer prophylaxis [2]. Teaching hospitals with higher rates of device utilization have had higher device-associated infection rates [4,16]. As in adult ICUs, the most important risk factors for nosocomial infection in pediatric ICUs appears to be the length of ICU stay and rate of device utilization [2,6].

A potential risk factor undergoing intense study at this time is hyperglycemia. Hyperglycemia is common in the ICU setting due to underlying disease, physiologic stress, and parenteral nutritional support. In vitro investigations suggest that hyperglycemia can impair polymorphonuclear leukocyte and monocyte phagocytic and bactericidal activities [17]. A large randomized trial performed in a single surgical ICU found that tight control of blood glucose during the ICU stay (maintaining blood glucose 80 to 110 mg per dL) reduced overall mortality, the incidence of bacteremias, and the number of patients who required more than 10 days of antibiotic therapy [18].
However, a subsequent study of the impact of tight glycemic control on outcomes in a medical ICU did not find the same benefit, and further investigation of both the risk of infection with hyperglycemia and optimal treatment is needed [19].

Figure 78.1. Selected antimicrobial-resistant pathogens associated with nosocomial infections in ICU patients, comparison of resistance rates from January through December 2003 with 1998 through 2002, NNIS System. CNS, coagulase-negative staphylococci; 3rd Ceph, resistance to 3rd-generation cephalosporins (ceftriaxone, cefotaxime, or ceftazidime); Quinolone, resistance to either ciprofloxacin or ofloxacin. *Percent (%) increase in resistance rate of current year (January–December 2003) compared with mean rate of resistance over previous 5 years (1998–2002): [(2003 rate – previous 5-year mean rate)/previous 5-year mean rate] × 100. **“Resistance” for Escherichia coli or Klebsiella pneumoniae is the rate of nonsusceptibility of these organisms to either 3rd group or aztreonam. [From the American Journal of Infection Control 2004; 32: 470–485. A report from the NNIS System. This report is public domain and can be copied freely.]

Preventive and Control Measures

A number of approaches have been found to help prevent ICU-associated infections. The comprehensive use of standard infection control practices as well as enhanced infection control precautions for selected pathogens, limiting the use of medical devices, and careful attention to architectural design are key components of strategies to prevent ICU infections. In addition, the implementation of targeted quality improvement programs for central vascular catheter infections and ventilator-associated pneumonia have been shown to be highly effective approaches to decreasing infection rates.

Infection Control Precautions

The CDC and the Hospital Infection Control Practices Advisory Committee have prepared guidelines on isolation precautions to prevent the transmission of microorganisms from colonized or infected patients to other patients, visitors, and healthcare workers [20]. The current guidelines were last updated in 2007 and recommend a two-tiered approach to patient care. Standard precautions are used for the care for all patients. Additional, more stringent transmission-based precautions are used for the care of patients who are suspected or known to be colonized or infected with specific pathogens that are readily transmitted through direct contact, through large respiratory droplets, or through smaller airborne particles. The current guidelines are summarized in Table 78.1.

A key component of these guidelines is the need for healthcare workers to practice good hand hygiene [20,21]. Approaches that have been shown to improve compliance with this practice have included the provision of water free alcohol-based hand rubs throughout institutions as well as intensified educational and monitoring programs on hand hygiene. Alcohols have excellent in vitro germicidal activity against Gram-positive and Gram-negative pathogens, fungi, and many viruses including human immunodeficiency virus, influenza virus, and respiratory syncytial virus.

There have been several additional approaches recently developed to further control of healthcare-acquired infection that should be considered in the ICU setting, particularly in the setting of high infection rates. The performance of daily bathing of patients with chlorhexidine gluconated using either impregnated clothes or dilute bathing solutions has been associated with reductions in rates of MRSA and VRE acquisition and central line–associated BSIs, potentially by decreasing the bioburden of microbial pathogens on the body surface [22,23,24]. Although not associated with alterations in infection rates, the institution of programs to monitor the actual performance of housekeeping staff has been found to improve the disinfection of the hospital environment in ICUs, including disinfection of computer stations [25]. Finally, equipment has been developed that allows for the use of total room disinfection with a hydrogen peroxide mist which can eradicate vegetative bacteria, fungi, spores, viruses, and prions. While its use as part of routine care remains unclear, it may be of value in controlling outbreaks due to Clostridium difficile or multidrug-resistant Gram-negative bacteria [26,27].

Architectural Design and Hospital Construction

Modern ICU design includes the use of single-patient rooms, adequate physical space for equipment and personnel, individual patient sinks, adequate hand hygiene stations, and adequate room ventilation with filtered air and at least six air changes per hour [28]. In addition, there are defined guidelines
for the design of airborne isolation infection rooms for patients requiring management of tuberculosis or other infections readily transmitted by the airborne route.

Table 78.1 Isolation Precautions

		Transmission based
	Standard	Airborne	Droplet	Contact
Definition	Reduce risk of transmission of blood-borne pathogens and pathogens from moist body substances, and applies to all patients	Prevent transmission of disease by airborne droplet nuclei (≤5 μm size)	Reduce risk of transmission of microorganism by droplets (≥5 μm size) generated by the patient sneezing, coughing, talking, or performance of procedure	Reduce transmission of epidemiologic important organism from an infected or colonized patient through direct or indirect contact
Room		Private-negative pressure room with air exhausted to outdoors or through high-efficient filtration; door kept closed	Private room; door may remain open	Private room or cohorted with a patient with similar organism. Patient care items should be dedicated to a single patient
Mask	Mask, goggles, and face shields provide barrier protection to reduce the transmission of pathogens when splashes or spray of blood, body fluids, secretions, or excretions are likely	N95 mask or comparable respirator. Surgical mask should be worn by the patient during transportation outside the negative pressure room	Mask if entering the room
Gown	Provide barrier protection, prevents contamination of clothing, and protects the skin of personnel from blood and body fluid exposures
Gloves	Anticipated blood, body fluid, secretions/excretions, nonintact skin, contaminated items, and mucous membranes
Hand hygiene	Before and after patient contact; immediately after glove removal; after contact with blood, body fluids, secretions/excretions, or mucous membranes
Suspected or confirmed pathogens	Used for all patients independent of the presence of known pathogens	Tuberculosis Varicella (including disseminated zoster) SARS Measles Disseminated zoster Viral hemorrhagic fevers Smallpox Monkeypox Varicella Avian influenza	Meningitis due to Neisseria meningitides or Haemophilus influenzae Diphtheria (pharyngeal) Pertussis Mumps Mycoplasma pneumoniae Pneumonic plague Streptococcal (Group A) pharyngitis, pneumonia Influenza Rubella Parvovirus B19	MDR bacterial (MRSA, VRE, GISA, VRSA, Gram-negative bacilli) Clostridium difficile Viral hemorrhagic fevers Scabies Lice HSV (neonatal; disseminated) Disseminated zoster
GISA, glycopeptide-intermediate Staphylococcus aureus; MDR, multidrug resistant; MRSA, methicillin-resistant; Staphylococcus aureus SARS, severe acute respiratory syndrome; VRE, vancomycin-resistant enterococci; VRSA, vancomycin-resistant Staphylococcus aureus.