Paul K. Sikka, Shawn T. Beaman and James A. Street (eds.)Basic Clinical Anesthesia10.1007/978-1-4939-1737-2_52

52. Infectious Diseases

Seth R. Cohen¹ and Kristin Ondecko Ligda¹

(1)

Department of Anesthesiology, University of Pittsburgh Medical Center, 1400 Locust Street, Pittsburgh, PA 15219, USA

Seth R. Cohen

Email: scohe001@gmail.com

Kristin Ondecko Ligda (Corresponding author)

Email: ondeckoligdakm@upmc.edu

Keywords

Blood-borne pathogensNosocomial infectionsHepatitisHIVPrion

Infectious disease agents include viruses, bacteria, fungi, protozoa, parasites, and proteins called prions. Some patients are asymptomatic from their infection, whereas in other patients, clinical or subclinical illness affects the patient during the perioperative period. Transmission of the agents can occur through airborne inhalation, through contact with contaminated body fluids, via food, through physical contact, or through vector organisms. Additionally, patient-patient and patient-healthcare worker (HCW) transmission of infectious diseases remain a high concern. The perioperative period represents a unique challenge in the prevention of transmission. While diligent hand washing remains a staple in the standard of care, other measures must be implemented with certain infectious agents. Several of the major infectious diseases will be reviewed in this section, and universal precautions will be examined. Careful perioperative planning and situational awareness should be practiced by the healthcare worker taking care of patients with transmissible diseases.

Human Herpes Virus

The human herpes family viruses (HHV) consist of eight separate viruses, all with potential of causing human disease. The prevalence of HSV-1 (HHV-1) and HSV-2 (HHV-2) in the general population is 65 % and 29 %, respectively. HSV-1 is mostly transmitted through nonsexual contact and is most frequently associated with oral mucosal lesions, while HSV-2 is mostly transmitted through sexual contact and commonly infects urogenital mucosa. Shortly after primary infection, the virus can be found in a dormant state in sensory neurons. Reactivation may occur at a later time. Immunocompromised patients are at increased risk for reactivation with subsequent disseminated disease. HSV reactivation in posttransplant patients can cause pneumonia, hepatitis, encephalitis, and disseminated disease. Oral acyclovir has been shown to be an effective prophylactic and treatment agent for HSV-1 and HSV-2.

Varicella zoster virus (VZV, HHV-3) is responsible for chickenpox and shingles in the healthy, immunocompetent population. However, it may cause significant, life-threatening disease in the immunocompromised population, such as posttransplant patients. Primary infection (chickenpox) or reactivation (shingles) in healthy patients with intact immune systems will manifest with a vesicular rash in a dermatomal pattern. Shortly after primary infection, VZV remains dormant in neurons of dorsal root ganglia. However, reactivation in posttransplant patients may manifest with cutaneous infection, encephalitis, myelitis, and pneumonia. Many studies have documented the efficacy of acyclovir and ganciclovir for the prophylaxis of VZV. Vaccination is available for patients and their close contacts and has shown to be effective in preventing disease.

Epstein-Barr virus (EBV, HHV-4) is the causative virus associated with infectious mononucleosis and the more serious (but rare) Burkitt’s lymphoma, nasopharyngeal carcinoma, and posttransplant lymphoproliferative disorder (PTLD). About 90 % of the general population has been found to be seropositive for EBV. While patients generally demonstrate flu-like symptoms, more significant symptoms may occur. These include encephalitis, optic neuritis, and hepatosplenomegaly with increased risk of splenic rupture. Like VZV, EBV is generally transmitted through respiratory secretions and saliva. Shortly after primary infection, EBV can be found in a dormant state in B cells of the immune system. No vaccination currently exists for EBV, although some studies have shown the effectiveness of antiviral medications for treatment.

Cytomegalovirus (CMV, HHV-5) is a common infection with a prolonged latency period. Estimates of seropositivity rates range from 40 % in young adults to above 90 % in the elderly population. While most infections occur asymptomatically in the healthy population, immunocompromised patients are at risk for disseminated disease. In particular, post-lung transplant patients are at risk for CMV pneumonitis, a common cause of bronchiolitis obliterans syndrome. Valganciclovir has been shown to be an effective prophylactic measure in these high-risk patients.

HHV-6, a common infection that occurs in over 90 % of the population, causes roseola infantum which is manifested by high fevers and a viral exanthem rash. After primary infection, it remains dormant in CD4 lymphocytes. Reactivation in immunocompromised patients may lead to neurologic symptoms, gastroenteritis, pneumonitis, hepatitis, and myelosuppression. While no vaccine currently exists, antiviral agents are an effective treatment.

HHV-8 gained attention as an opportunistic disease of AIDS patients, referred to as Kaposi sarcoma. In addition, HHV-8 is a causative agent in primary effusion lymphoma and multicentric Castleman disease in immunocompromised patients. While only 1.5 % of Americans are seropositive, up to 50 % of the sub-Saharan population is infected. Treatment of these diseases appears to be a reduction in the degree of immunosuppression, chemotherapy, radiation therapy and also resection of localized tumors, and treatment of other coinfections.

Paramyxovirus

Respiratory syncytial virus (RSV) and parainfluenza are part of the paramyxovirus family that is a frequent cause of both upper and lower respiratory tract infections in children. Peak seasonal appearance occurs in the winter, similar to influenza. Immunocompromised patients, such as posttransplant and lymphopenic patients, are more likely to have progression of the infection into the lower respiratory tract with significantly higher mortality rates. The paramyxoviruses have been associated with posttransplant complications, including post-viral obliterative bronchiolitis, a cause of chronic rejection. While vaccination is not available, RSV prophylaxis can be effectively managed with immunoglobulin and monoclonal antibodies. Treatment centers on the use of ribavirin, RSV antibodies, and supportive measures. In comparison, there are no proven preventative or treatment measures for parainfluenza.

Influenza Virus

Perhaps the one virus that has gained global notoriety in history for global epidemics has been the influenza virus. Despite widespread vaccination, the potential for antigenic shift and drift exists, a situation that could contribute to worldwide pandemics. Influenza A and B are RNA viruses that cause upper and lower respiratory tract disease. Like RSV, the progression to lower respiratory tract disease is more prevalent in immunocompromised patients and disease peaks in the winter. Neuraminidase inhibitors, such as oseltamivir and zanamivir, are effective treatments, especially when begun early in the viral course. These treatments are augmented by amantadine and rimantadine. Vaccination is available, but it may not cover all strains of the virus.

Blood-Borne Viruses

Blood-borne viruses are a major concern in the hospital for both the patient and healthcare providers. Virus transmission from an infected host during percutaneous or mucosal penetration is reported to be 0.3 % for human immunodeficiency virus (HIV), 3 % for hepatitis C, and 30 % for hepatitis B. In order to calculate risk of transmission from percutaneous or mucous membrane injury, several factors must be considered, including method of transmission (needle penetration versus blood splash to mucous membrane), needle type (hollow-bore needle such as an IV needle versus solid-bore needle such as suture needle), needle gauge, penetration of needle into patient and healthcare worker, presence of blood on needle, access of the needle to the patient’s bloodstream, or whether the needle has passed through gloves or other barriers prior to entering the skin. Personal protective equipment and situational awareness remain the mainstays of prevention. Effective protection methods to minimize risk of transmission of blood-borne diseases include gloves, double gloving if needed, face shields or other eye protection, sleeve reinforcements, knee-high trauma boots, plastic aprons under surgical gowns, and avoidance of blind suturing techniques.

HIV is an RNA retrovirus that produces reverse transcriptase, which allows the creation of complimentary DNA that is substituted into the host cell. The virus attacks the host and causes cell lysis, with subsequent loss of helper CD4 T cells. Although mandatory preoperative HIV screening has been advocated by many, ethical concerns in addition to financial concerns are barriers to this screening. Furthermore, consent must be obtained before performing testing. Instead, a more accepted practice among many practitioners seems to be testing either high-risk patients or those undergoing higher risk procedures. Regardless of the patient’s infection status, universal precautions are standard practice. Upon receiving a percutaneous or mucosal injury from a patient with unknown HIV status, prophylactic treatment is begun and consent for HIV testing is obtained from the patient. If the host was determined to have asymptomatic disease, a two-drug regimen is recommended. However, if the patient was symptomatic at the time of exposure, a three-drug regimen is commenced for at least 4 weeks.

Only gold members can continue reading. Log In or Register to continue