SARS surveillance during emergency public health response, United States, March-July 2003.In response to the emergence of severe acute respiratory syndrome Severe Acute Respiratory Syndrome (SARS) Definition Severe acute respiratory syndrome (SARS) is the first emergent and highly transmissible viral disease to appear during the twenty-first century. (SARS), the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. established national surveillance using a sensitive case definition incorporating clinical, epidemiologic, and laboratory criteria. Of 1,460 unexplained respiratory illnesses Noun 1. respiratory illness - a disease affecting the respiratory system respiratory disease, respiratory disorder adult respiratory distress syndrome, ARDS, wet lung, white lung - acute lung injury characterized by coughing and rales; inflammation of the reported by state and local health departments to the Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. from March 17 to July 30, 2003, a total of 398 (27%) met clinical and epidemiologic SARS case criteria. Of these, 72 (18%) were probable cases with radiographic radiographic (rā´dēōgraf´ik), adj relating to the process of radiography, the finished product, or its use. evidence of pneumonia. Eight (2%) were laboratory-confirmed SARS-coronavirus (SARS-CoV) infections, 206 (52%) were SARS-CoV negative, and 184 (46%) had undetermined SARS-CoV status because of missing convalescent-phase serum specimens. Thirty-one percent (124/398) of case-patients were hospitalized; none died. Travel was the most common epidemiologic link (329/398, 83%), and mainland China was the affected area most commonly visited. One case of possible household transmission was reported, and no laboratory-confirmed infections occurred among healthcare workers. Successes and limitations of this emergency surveillance can guide preparations for future outbreaks of SARS or respiratory diseases Noun 1. respiratory disease - a disease affecting the respiratory system respiratory disorder, respiratory illness adult respiratory distress syndrome, ARDS, wet lung, white lung - acute lung injury characterized by coughing and rales; inflammation of the of unknown etioloqy. ********** The emergence of severe acute respiratory syndrome (SARS) presented a challenge to public health and healthcare delivery systems worldwide. The previously unknown respiratory syndrome 'respiratory syndrome' A relatively specific immune response to high-dose rifampin therapy, characterized by a flu-like complex, dyspnea and wheezing, leukopenia, thrombocytopenia; other hypersensitivity reactions caused by rifampin include flushing, fever, was characterized by nonspecific nonspecific /non·spe·cif·ic/ (non?spi-sif´ik) 1. not due to any single known cause. 2. not directed against a particular agent, but rather having a general effect. nonspecific 1. clinical symptoms, was highly transmissible transmissible /trans·mis·si·ble/ (trans-mis´i-b'l) capable of being transmitted. trans·mis·si·ble adj. Capable of being conveyed from one person to another. in some circumstances, did not respond to antimicrobial antimicrobial /an·ti·mi·cro·bi·al/ (-mi-kro´be-al) 1. killing microorganisms or suppressing their multiplication or growth. 2. an agent with such effects. therapy, and could rapidly progress to severe respiratory distress Respiratory distress A condition in which patients with lung disease are not able to get enough oxygen. Mentioned in: Lung Cancer, Non-Small Cell and death. SARS appears to have originated in Guangdong Province Noun 1. Guangdong province - a province in southern China Guangdong, Kwangtung , China; however, the global importance of this illness was not recognized initially by local health authorities. When the World Health Organization (WHO) issued a historic global alert about cases of severe atypical pneumonia atypical pneumonia n. See primary atypical pneumonia. atypical pneumonia Chest medicine A clinically 'atypical' form of pneumonia, which lacks the classic signs and Sx of pneumonia Types Chlamydia pneumonia, on March 12, 2003, the outbreak had spread through international travel from Guangdong Province to at least Hong Kong Hong Kong (hŏng kŏng), Mandarin Xianggang, special administrative region of China, formerly a British crown colony (2005 est. pop. 6,899,000), land area 422 sq mi (1,092 sq km), adjacent to Guangdong prov. and Hanoi, Vietnam. There was an urgent global need for diagnosis of the etiologic agent, detection and containment of probable cases, guidance on the healthcare management of patients and potentially exposed persons, identification of measures to prevent and control infections, and timely public health communications to a wide range of audiences. On March 14, 2003, the U.S. Centers for Disease Control and Prevention (CDC See Control Data, century date change and Back Orifice. CDC - Control Data Corporation ) launched an emergency public health response and established national surveillance for SARS to identify case-patients in the United States and determine if domestic transmission was occurring. We describe the surveillance system established to detect SARS in the United States, focusing on its design, challenges, and modifications that occurred as the outbreak evolved, and characteristics of the case-patients identified. Such information is critical for preparing for possible future outbreaks of SARS or other emerging microbial microbial pertaining to or emanating from a microbe. microbial digestion the breakdown of organic material, especially feedstuffs, by microbial organisms. threats with nonspecific respiratory symptoms. Methods SARS Case Definition CDC's initial surveillance definition fur a suspect case of SARS (Table 1) was based on a definition first published by WHO (1). These definitions specified clinical criteria and required a potential exposure to SARS (epidemiologic link). WHO categorized cat·e·go·rize tr.v. cat·e·go·rized, cat·e·go·riz·ing, cat·e·go·riz·es To put into a category or categories; classify. cat all cases with x-ray or autopsy evidence of pneumonia or respiratory distress as probable, and all others meeting the case definition were classified as suspect cases. CDC initially categorized all cases as suspect, but on April 29, 2003, CDC adopted WHO's suspect and probable classifications (2). SARS-affected areas that constituted an epidemiologic link changed throughout the outbreak, requiring continual modification of the case definition. CDC considered an area SARS-affected if evidence of documented or suspected community transmission existed. Regions were removed from the list of SARS-affected areas when CDC-issued travel alerts or advisories were discontinued, which meant that the area had reported no new cases of SARS for 30 days. On April 29, 2003, after a new coronavirus coronavirus /co·ro·na·vi·rus/ (ko-ro´nah-vi?rus) any virus belonging to the family Coronaviridae. Coronavirus /Co·ro·na·vi·rus/ (ko-ro´nah-vi?rus (SARS-CoV) was identified as the etiologic agent of SARS (3-6), the case definition was changed to incorporate criteria for laboratory-confirmed illness (7). Laboratory criteria were refined near the end of the outbreak, resulting in the final case definition on July 18, 2003 (Tables 2 and 3); revision of the requirements for a convalescent-phase serum specimen from 21 to 28 days after illness onset was not applied retrospectively, consistent with the instructions accompanying release of this case definition. This definition also introduced an exclusion criterion for suspect or probable case-patients confirmed negative for SARS-CoV infection. In this analysis, we did not apply this exclusion criterion to allow for a complete presentation of suspect and probable cases captured and monitored by national surveillance. Inclusion Criteria
Inclusion criteria are a set of conditions that must be met in order to participate in a clinical trial. Case-patients were eligible for inclusion if they were U.S. residents and were present in the United States during some of their illness. Non-U.S. residents who became ill or in whom SARS was diagnosed while they were in the United States were monitored as patients of special interest until April 30, 2003, after which they were included in surveillance. U.S. citizens who were not present in the United States for any period of their illness were not included in surveillance. National Surveillance for SARS National surveillance began on March 17, 2003, 3 days after CDC initiated its emergency response. The analysis in this report covers the period March 17 through July 30, 2003, 3 weeks after WHO declared the global outbreak over. Case definitions were distributed to state and local health departments through CDC's Epidemic Information Exchange (Epi-X), a secure communications network The transmission channels interconnecting all client and server stations as well as all supporting hardware and software. for public health professionals, and through CDC's Health Alert Network. Case definitions were also posted on a CDC Web site dedicated to SARS. A case report form was developed to collect demographic and clinical data as well as information about epidemiologic links. This form was also distributed through Epi-X and by electronic mailings by the Council of State and Territorial Epidemiologists The Council of State and Territorial Epidemiologists (CSTE) was organized in the USA in the early 1950s in response to the need to have at least one person in each state and territory responsible for public health surveillance of diseases and conditions of public health (CSTE CSTE Council of State and Territorial Epidemiologists CSTE Certified Software Test Engineer CSTE Centre for the Study of Teacher Education (University of British Columbia, Vancouver) ) to its membership. The case report form was modified as the outbreak evolved. At the beginning of the outbreak, health departments were requested to report to CDC all respiratory illnesses that they thought should be evaluated for SARS. Although the communication chain for reporting these illnesses to health departments varied by state, all health departments relied on passive reporting from clinicians rather than actively seeking to identify potential cases. CDC hosted weekly teleconferences with state and local health departments to address developing issues related to the domestic surveillance and response. An Atlanta-based CDC team received illness reports by telephone or fax. State and local health department personnel collected data, completed case report forms, and determined case status in consultation with CDC. When a patient met the case definition, data about that person were added to a "line list," which was updated and analyzed daily. Hospitalized case-patients were actively monitored to establish outcomes, as were persons who had pending data that could alter case status. Illnesses that failed to meet the case definition on subsequent investigation (e.g., patient's travel history clarified) were removed from the line list. The data collection system at both the health departments and CDC was paper-based rather than electronic or online. Epidemiologic data were entered at CDC into an electronic database that was merged with laboratory data. Laboratory Confirmation of SARS Infection State and local health departments were asked to collect acute- and convalescent-phase serum and stool specimens and nasopharyngeal nasopharyngeal pertaining to the nasal and pharyngeal cavities. nasopharyngeal meatus see nasopharyngeal meatus. nasopharyngeal spasm see reverse sneeze. or oropharyngeal oropharyngeal /oro·pha·ryn·ge·al/ (-fah-rin´je-al) 1. pertaining to the mouth and pharynx. 2. pertaining to the oropharynx. swab samples from all case-patients. Before the cause of SARS was established, specimens were tested for a wide array of bacterial and viral pathogens at CDC. After SARS-CoV was discovered, serum specimens were tested for SARS-CoV antibodies, and respiratory and stool specimens were tested for SARS-CoV by polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is (PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) ) (4). Diagnostic testing Diagnostic testing Testing performed to determine if someone is affected with a particular disease. Mentioned in: Von Willebrand Disease was initially centralized cen·tral·ize v. cen·tral·ized, cen·tral·iz·ing, cen·tral·iz·es v.tr. 1. To draw into or toward a center; consolidate. 2. at CDC. Later, reagents for SARS-CoV antibody and nucleic acid nucleic acid, any of a group of organic substances found in the chromosomes of living cells and viruses that play a central role in the storage and replication of hereditary information and in the expression of this information through protein synthesis. testing were made available to state public health laboratories and the Laboratory Response Network (8). To meet U.S. Food and Drug Administration requirements for the use of nonlicensed tests in these laboratories, CDC developed informed-consent documents and informational materials that clinicians used when collecting specimens for SARS-CoV testing from their patients. Case-patients were classified as confirmed, negative, or undetermined for SARS-CoV infection (Tables 2 and 3). On July 18, 2003, the 21-day period required for convalescent-phase specimens was extended to 28 days for newly identified cases on the basis of evidence that seroconversion seroconversion /se·ro·con·ver·sion/ (-con-ver´zhun) the change of a seronegative test from negative to positive, indicating the development of antibodies in response to immunization or infection. sometimes occurred after day 21 (9). Laboratory Testing for Other Respiratory Pathogens During the course of the outbreak, testing for alternative causes that could fully explain patient illness was ordered at the discretion of local clinicians, and SARS was often excluded on the basis of local interpretations of test results. Many of these illnesses were never reported to CDC. Diagnostic testing for alternative agents was performed at CDC early in the outbreak. In addition, evaluation of acute respiratory specimens and paired serum specimens from suspect and probable case-patients for evidence of the following respiratory pathogens was completed after the outbreak was over: Mycoplasma pneumoniae Mycoplasma pneu·mo·ni·ae n. A microorganism causing primary atypical pneumonia in humans. , Streptococcus pneumoniae Streptococcus pneu·mo·ni·ae n. Pneumococcus. Streptococcus pneumoniae Microbiology A pathogenic streptococcus with 90 serotypes associated with pneumonia, bacteremia, meningitis Transmission Person to person Incidence , Chlamydia pneumoniae Chlamydia pneumoniae C psittaci TWAR A pathogen that causes pneumonia, asymptomatic RTIs, pharyngitis, otitis media , C. psittaci Noun 1. C. psittaci - bacteria responsible for the sexually transmitted disease chlamydia Chlamydia psittaci chlamydia - coccoid rickettsia infesting birds and mammals; cause infections of eyes and lungs and genitourinary tract , Legionella pneumophila Legionella pneumophila is a thin, pleomorphic, flagellated Gram-negative bacterium of the genus Legionella.[1] L. pneumophila is the primary human pathogen in this group and is the causative agent of legionellosis or Legionnaires' disease. , influenza viruses influenza virus n. Any of three viruses of the genus Influenzavirus designated type A, type B, and type C, that cause influenza and influenzalike infections. types A and B, respiratory syncytial virus respiratory syncytial virus (sĭnsĭsh`əl): see cold, common. , parainfluenza viruses parainfluenza virus n. Any of five types of viruses of the genus Paramyxovirus that are associated with various respiratory infections, especially in children. types 1, 2, and 3, human metapneumovirus (HMPV), and adenovirus adenovirus Any of a group of spheroidal viruses, made up of DNA wrapped in a protein coat, that cause sore throat and fever in humans, hepatitis in dogs, and several diseases in fowl, mice, cattle, pigs, and monkeys. . M. pneumoniae M. pneumoniae, n a species of Mycoplasma causing mycoplasma pneumonia, which is characterized by symptoms of an upper respiratory infection with a dry cough and fever. immunoglobulin immunoglobulin: see antibody; immunity; immunology. Immunoglobulin Any of the glycoproteins in the blood serum that are induced in response to invasion by foreign antigens and that protect the host by eradicating pathogens. (Ig) G and IgM antibodies were measured by using the REMEL Mycoplasma pneumoniae IgG/IgM Antibody Test System (REMEL Inc., Lenexa, KS). S. pneumoniae IgG antibodies to pneumococcal pneumococcal /pneu·mo·coc·cal/ (-kok´al) pertaining to or caused by pneumococci. surface adhesin A protein (PsaA) were measured by using a PsaA-ELISA (enzyme-linked immunosorbent assay enzyme-linked immunosorbent assay n. ELISA. Enzyme-linked immunosorbent assay (ELISA) A diagnostic blood test used to screen patients for AIDS or other viruses. ) as previously described (10). A rise in IgG antibody titers antibody titer The amount of a specific antibody present in the serum, usually as a result of an acquired infection; titers for IgM usually rise abruptly at the time of infection–acute phase and fall slowly; during the 'convalescent' phase, IgG ↑ and is of twofold or more between acute- and convalescentphase serum pairs was considered positive for a pneumococcal exposure or event. Chlamydia chlamydia (kləmĭd`ēə), genus of microorganisms that cause a variety of diseases in humans and other animals. Psittacosis, or parrot fever, caused by the species Chlamydia psittaci, IgG and IgM antibodies were measured by using a microimmunofluorescent antibody assay (Focus Technologies, Cypress, CA). L. pneumophila antibodies were measured by using an indirect immunofluorescent immunofluorescent having the characteristic of immunofluorescence. immunofluorescent antibody test see fluorescence microscopy. immunofluorescent microscopy see fluorescence microscopy. antibody assay (11). Specific IgG antibodies to the respiratory viruses (excluding influenza) were measured by using an indirect enzyme immunoassay Immunoassay An assay that quantifies antigen or antibody by immunochemical means. The antigen can be a relatively simple substance such as a drug, or a complex one such as a protein or a virus. panel, following procedures previously described for HMPV (12). A rise in IgG antibody titers of fourfold fourfold Adjective 1. having four times as many or as much 2. composed of four parts Adverb by four times as many or as much Adj. 1. or greater between acute- and convalescent-phase serum pairs was considered positive for recent virus infection. Serologic se·rol·o·gy n. pl. se·rol·o·gies 1. The science that deals with the properties and reactions of serums, especially blood serum. 2. analysis for influenza was performed by hemagglutination-inhibition assay. All serum specimens were treated with receptor-destroying enzyme to remove nonspecific inhibitors before testing (13). Specimens from some or all of the following sources were tested by PCR for evidence of bacterial or viral infection viral infection, n an infection by a pathogenic virus. A virus acts on the cell nucleus, taking over the genetic material within the nucleus and replicating itself. : bronchoalveolar fluid, sputum sputum /spu·tum/ (spu´tum) [L.] expectoration; matter ejected from the trachea, bronchi, and lungs through the mouth. sputum cruen´tum bloody sputum. , tracheal tracheal pertaining to or emanating from trachea. tracheal aspiration see transtracheal aspiration. tracheal band sign on contrast radiography of a dilated esophagus, the impression made ventrally by the trachea. aspirates, nasal washings, and nasal, nasopharyngeal, and oropharyngeal swab samples. All the bacterial methods used have been described previously (11,14-16) except the L. pneumophila real-time PCR assay (Online Appendix). Total nucleic acid was extracted from 100 [micro]L of specimen by using the QIAamp Virus BioRobot MDx kit (QIA-GEN Inc., Valencia, CA). Reverse transcriptase Reverse transcriptase Any of the deoxyribonucleic acid (DNA) polymerases present in particles of retroviruses which are able to carry out DNA synthesis using an RNA template. (RT)-PCR assays for influenza A influenza A n. Influenza caused by infection with a strain of influenza virus type A. influenza A Infectious disease An avian virus, especially of ducks–which in China live near the pig reservoir and 'vector'; and B viruses; respiratory syncytial virus; human parainfluenza viruses Human parainfluenza viruses (HPIVs) are a group of four distinct serotypes of single-stranded RNA viruses belonging to the paramyxovirus family. They are the second most common cause of lower respiratory tract infection in younger children. 1, 2, and 3 (17); and HMPV (12) were performed as previously described. RT-PCR RT-PCR reverse transcriptase-polymerase chain reaction. See PCR1. assays for adenovirus and picornavirus picornavirus Any of a group of the smallest known animal viruses. (Pico refers to their small size, rna to their core of RNA.) This group of spheroidal viruses includes viruses that attack the vertebrate intestinal tract and often invade the central nervous system as well (inclusive of inclusive of prep. Taking into consideration or account; including. rhinovirus rhinovirus Any of a group of picornaviruses capable of causing common colds in humans. The virus is thought to be transmitted to the upper respiratory tract by airborne droplets. and enterovirus enterovirus /en·tero·vi·rus/ (en´ter-o-vi?rus) any virus of the genus Enterovirus. enterovi´ral Enterovirus /En·tero·vi·rus/ (en´ter-o-vi?rus ) were performed by using these same amplification conditions with primer pairs to the conserved regions of the hexon gene and the 5'-untranslated region: adenovirus [(+) 5'-CCC(AC)TT(CT)AACCACCACCG-3'; (-) 5'-ACATCCTT(GCT (programming, tool) GCT - A test-coverage tool by Brian Marick <marick@testing.com>, based on GNU C. Version 1.4 was ported to Sun-3, Sun-4, RS/6000, 68000, 88000, HP-PA, IBM 3090, Ultrix, Convex, SCO but not Linux, Solaris, or Microsoft Windows. )C(GT) GAAGTTCCA-3'] and picornavirus [(+) 5'-GGCCCCTGAATG (CT)GGCTAA-3'; (-) 5'-GAAACACGGACACCCAAA GTA-3']. All nucleic acid extracts were also tested by RT-PCR for the GAPDH GAPDH Glyceraldehyde-3-Phosphate Dehydrogenase (also seen as G3PDH) housekeeping gene to ensure RNA RNA: see nucleic acid. RNA in full ribonucleic acid One of the two main types of nucleic acid (the other being DNA), which functions in cellular protein synthesis in all living cells and replaces DNA as the carrier of genetic integrity and absence of RT-PCR inhibitors. Results From March 17 to July 30, 2003, CDC received reports of 1,460 respiratory illnesses under evaluation for SARS, of which 398 (27%) met the case definition for suspect or probable SARS before laboratory-based exclusion criteria exclusion criteria AIDS Donor exclusion criteria, see there for SARS-CoV-negative status were applied (Figure 1). Seventy-two (18%) of those meeting the case definition had chest x-ray chest x-ray, n an examination of the chest using x-rays. Routinely performed in patients complaining of chest pain to rule out respiratory or heart disease. chest X-ray Chest film, see there evidence of pneumonia and were classified as probable case-patients. Eight case-patients (2%) were confirmed to be positive for SARS-CoV, 206 (52%) were confirmed to be negative for SARS-CoV by serologic testing serologic test Lab medicine A test that measures components–eg, antibodies, complement, and reactions–eg, complement fixation, agglutination, precipitation, etc, that reflect immune status, especially antibody titers. Cf Seroconversion. , and 184 (46%) had undetermined SARS-CoV status because of the absence of convalescent-phase serum samples. Cases were reported from 41 states and Puerto Rico Puerto Rico (pwār`tō rē`kō), island (2005 est. pop. 3,917,000), 3,508 sq mi (9,086 sq km), West Indies, c.1,000 mi (1,610 km) SE of Miami, Fla. , with the highest case counts in California (74), New York New York, state, United States New York, Middle Atlantic state of the United States. It is bordered by Vermont, Massachusetts, Connecticut, and the Atlantic Ocean (E), New Jersey and Pennsylvania (S), Lakes Erie and Ontario and the Canadian province of (51), and Washington (30); no cases were reported from 9 states or the District of Columbia District of Columbia, federal district (2000 pop. 572,059, a 5.7% decrease in population since the 1990 census), 69 sq mi (179 sq km), on the east bank of the Potomac River, coextensive with the city of Washington, D.C. (the capital of the United States). (Figure 2). [FIGURES 1-2 OMITTED] Of the eight confirmed SARS-CoV-positive case-patients, all had radiographic evidence of pneumonia and six were identified in the first month of surveillance (Table 4). Five traveled to Hong Kong, two to Toronto, and one to Singapore. Further case details have been presented elsewhere (18-21). Among the eight confirmed SARS-CoV-positive ease-patients, seven had illnesses that were associated solely with travel to an affected area. Although the eighth ease-patient traveled with her spouse (subsequently confirmed as a case-patient) to an affected area (Hong Kong, where both stayed in a hotel in which intense local transmission occurred [22]), the epidemiologic link was classified as close contact because the onset of illness occurred 13 days after the couple's return to the United States (18,20). The median age of all suspect and probable case-patients was 39 years (range 3 months to 91 years), and 53% were male (Table 4). Almost one third (124/398, 31%) of the patients were hospitalized. The median length of hospitalization hospitalization /hos·pi·tal·iza·tion/ (hos?pi-t'l-i-za´shun) 1. the placing of a patient in a hospital for treatment. 2. the term of confinement in a hospital. for the 90 persons with adequate hospitalization duration data was 3 days (range 1-14). Twenty-one percent of hospitalized patients (19/91 patients with data on intensive care unit admissions) were admitted to an intensive care unit; only 2 of the 8 SARS-CoV-positive case-patients were admitted to intensive care units. Among all 398 suspect and probable case-patients, 4 (1%) required mechanical ventilation mechanical ventilation n. A mode of assisted or controlled ventilation using mechanical devices that cycle automatically to generate airway pressure. , one of whom was SARS-CoV positive (Table 4). No deaths were reported. Travel to an affected area was the most commonly reported epidemiologic link (83% of cases). Mainland China was the most frequent destination (39% of travelers), followed by Hong Kong (38%), and Toronto (18%); 22% of case-patients traveled to more than one affected area. The frequency of travel to China, Hong Kong, and Toronto among SARS case-patients is shown by date of illness onset in Figure 3; the periods during which these areas were considered SARS-affected for surveillance purposes are also shown. [FIGURE 3 OMITTED] No healthcare workers with suspect or probable SARS (n = 31) were confirmed to be SARS-CoV positive; 17 (55%) were confirmed SARS-CoV negative, and the remainder had undetermined SARS-CoV status. The only possible case of recognized secondary transmission was between the married couple described above. Number of Illnesses Reported and Completeness of Surveillance Data The number of illnesses reported was highest during the first 6 weeks of surveillance and varied over the course of the outbreak (Figure 1). Among suspect and probable cases, the completeness of critical surveillance variables related to case definition and severity of illness was as follows: date of symptom onset, 98%; radiologic chest imaging for pneumonia, 80%; hospitalization status, 99%; hospital discharge date for admitted case-patients, 73%; and healthcare worker as occupation, 94%. Although collection of convalescent-phase sera was essential for assessing infection with SARS-CoV, samples needed for definitive laboratory determination of case status were not obtained from 46% of patients (probable case-patients: 35%; suspect case-patients: 49%; chi-square = 4.68; p = 0.03). Surveillance System Sensitivity and Predictive Value pre·dic·tive value n. The likelihood that a positive test result indicates disease or that a negative test result excludes disease. predictive value a measure used by clinicians to interpret diagnostic test results. Sensitivity refers to the proportion of SARS-CoV cases in the population that were detected by the surveillance system (23). Because SARS-CoV confirmatory laboratory testing was performed only on patients identified by the surveillance system, we cannot evaluate sensitivity for the system overall. If we limit analysis to the population of suspect and probable cases with definitive laboratory results (N = 214), we can evaluate the sensitivity of the probable case definition; all the confirmed SARS-CoV positive patients (N = 8) had been classified as probable cases, leading to a sensitivity of 100%. The predictive value positive refers to the proportion of reported cases that actually have the health-related event under surveillance (SARS-CoV infection). The predictive value positive among cases with definitive laboratory results was 4% (8/214). The predictive value positive among the 47 probable cases with definitive laboratory results was 17%. Flexibility and Timeliness of Surveillance The United States was one of many countries reporting SARS cases to WHO, which established international case definitions and reporting standards. Although flexibility was limited by the need to maintain harmonized har·mo·nize v. har·mo·nized, har·mo·niz·ing, har·mo·niz·es v.tr. 1. To bring or come into agreement or harmony. See Synonyms at agree. 2. Music To provide harmony for (a melody). international surveillance, U.S. surveillance remained flexible enough to incorporate frequent modifications rapidly. For example, when mainland China was added to the list of SARS-affected areas, within hours, case-patients who traveled to provinces other than Guangdong were added to the line list, and travel to mainland China quickly became the most common travel exposure (Figure 3). The median time between symptom onset and reporting suspect or probable cases to CDC decreased during the first 12 weeks of national surveillance from 8 to 3 days. After week 12, the median time to national reporting increased to a median of 15 days, with 40% (30/76) of cases reported >50 days after illness onset. Data on date illness was reported to local and state health departments were not collected. Evaluation of Alternative Respiratory Pathogens Among the 201 suspect and probable case-patients for whom serologic or PCR testing was performed at CDC, 95 (47%) demonstrated evidence of at least one alternative respiratory infection Noun 1. respiratory infection - any infection of the respiratory tract respiratory tract infection infection - the pathological state resulting from the invasion of the body by pathogenic microorganisms . Among specimens tested picornavirus (enterovirus/rhinovirus) was the most common pathogen Pathogen Any agent capable of causing disease. The term pathogen is usually restricted to living agents, which include viruses, rickettsia, bacteria, fungi, yeasts, protozoa, helminths, and certain insect larval stages. identified (29 of 114, 25%), followed by human influenza A or B virus (25/166 [15%]) and M. pneumoniae (22/200, 11%; Table 5). Patients with probable and suspect cases of SARS were equally likely to have an alternate cause identified (46% each). SARS-CoV negative case-patients and those with unknown SARS-CoV status were also equally likely to have an alternate cause identified (45% and 49%, respectively). Adequate specimens were available for only two of the eight SARS-CoV positive case-patients, one of whom also showed a fourfold or greater rise in antibodies to influenza B influenza B n. Influenza caused by infection with influenza virus type B. influenza B Infectious disease An influenza virus which causes epidemics in 3-5 yr cycles. Cf Influenza A, Influenza C. . Discussion During the U.S. emergency public health response to SARS, >1,000 unexplained respiratory illnesses were reported by state and local health departments to CDC. Countless additional illnesses were investigated and rapidly ruled out for SARS by state and local health departments. Despite the large surveillance burden, discovery of the etiologic agent for SARS and development of effective diagnostic tests showed that the United States experienced limited SARS activity during the global outbreak, similar to much of Europe, Africa, Australia, and South America South America, fourth largest continent (1991 est. pop. 299,150,000), c.6,880,000 sq mi (17,819,000 sq km), the southern of the two continents of the Western Hemisphere. . There was no evidence of community transmission in the United States even though SARS-affected countries were common travel destinations for U.S. residents. Investigation of close contacts of the eight U.S. SARS-CoV-infected patients yielded one instance of secondary domestic transmission, although travel-related exposure cannot be definitively excluded for this case (18,20), and the source of exposure is considered undetermined by WHO. in addition, no healthcare workers identified by national surveillance had laboratory evidence of SARS infection, despite evidence of unprotected exposures to confirmed case-patients (24). While effective surveillance and timely infection-control measures likely helped limit transmission, why the United States experienced few SARS-CoV infections despite opportunities for importation and spread remains unclear. National surveillance during the emergency response met important surveillance objectives. It identified illness clusters for further investigation, tracked progression of the epidemic in the United States, and facilitated specimen collection from suspect and probable case-patients for SARS diagnosis. This surveillance allowed for rapid and frequent updates to the healthcare and public health communities and to the public on the status of the outbreak. Despite these successes, the system had several important limitations. Like all passive systems, it relied on astute healthcare providers to detect and report illnesses that might have been SARS. The lack of a rapid diagnostic test that could reliably diagnose SARS-CoV infection during the early phase of illness increased the workload and anxiety of clinicians, public health personnel, patients, their contacts, and the general public. Frequent, labor-intensive contact with healthcare providers was needed to obtain updated clinical information for reported case-patients. As a result, classification of patients as suspect and probable case-patients was dynamic and often changed as new information became available. This situation sometimes created seeming discrepancies between national and state and local health department case counts, which in turn complicated public communication. The evolution of the worldwide outbreak required frequent modifications of the case definition, and establishing consistent criteria to define a SARS-affected area on the basis of community transmission was difficult. Finally, the paper-based reporting system increased the difficulty of reporting to CDC and delayed timeliness of reports, and the resulting database did not allow states immediate access to their own information. The time between disease onset and reporting to CDC increased in the latter phase of the outbreak. This increased reporting lag may reflect the growing surveillance workload as the outbreak progressed, delays in reporting until alternative diagnoses were evaluated, or a decreasing sense of urgency fueled by low disease rates and low likelihood of confirmed SARS among U.S. case-patients and lack of evidence for community transmission. The value of remaining vigilant throughout all stages of an outbreak should not be underestimated. It was critical in the context of this outbreak that infection-control measures be rapidly implemented for all suspect and probable case-patients since a single case in any area could quickly have a global impact. Evidence from Toronto, Hong Kong, Hanoi, Singapore, and Taiwan suggests that in some circumstances a single patient led to a large number of secondary cases and chains of transmission (25,26). Moreover, although most patients with SARS show radiographic evidence of pneumonia, as was observed for all the confirmed U.S. case-patients with SARS-CoV disease, in an outbreak setting, heightened vigilance and infection-control measures should be maintained for suspect as well as probable case-patients because of growing evidence that a small proportion of patients may not exhibit evidence of pneumonia and because features of pneumonia often do not develop until days 4-7 of illness (27,28). The timeliness of infection-control measures implemented for U.S. case-patients could not be assessed because relevant data were not collected as part of national surveillance. The clinical signs and symptoms of SARS infections are similar to that of other respiratory illnesses. Empiric em·pir·ic n. 1. One who is guided by practical experience rather than precepts or theory. 2. An unqualified or dishonest practitioner; a charlatan. adj. 1. Empirical. 2. management of patients with respiratory illness, limited state and local capacity to perform reliable respiratory diagnostics, and lack of national surveillance for respiratory syndromes, such as pneumonia, complicated the challenge of rapid identification of SARS patients. Comprehensive testing for a variety of respiratory pathogens among patients with suspect and probable cases found that 46% had evidence of a possible infection with bacterial and viral respiratory pathogens other than SARS-CoV. Our finding that one case-patient with confirmed SARS-CoV also tested positive for influenza B infection is consistent with accumulating evidence that co-infections involving SARS-CoV and other bacterial or viral respiratory pathogens occur (29,30). This underscores the importance of obtaining convalescent-phase serum samples to make final determinations about infection with SARS-CoV and of maintaining infection-control measures despite identification of alternative agents. Moreover, in determining alternative diagnoses, the strength of the epidemiologic exposure criteria for SARS, the specificity of the diagnostic test, and the compatibility of the clinical signs and symptoms and course of illness for the alternative diagnosis should be taken into account (Tables 2 and 3). Testing for respiratory pathogens could not be completed until after the outbreak; this precluded timely re-assessment of case-patients to determine if an agent other then SARS-CoV was most likely responsible for the clinical illness. To help facilitate more timely diagnostic evaluation diagnostic evaluation Workup Medtalk An evaluation used to diagnose disease Components Medical Hx, CXR or other images, collection of specimens from blood for lab analysis , CDC plans to develop real-time PCR assays fur important respiratory pathogens for use by public health laboratories. Improving local capacity for diagnosing respiratory illness should strengthen national preparedness for respiratory illness threats. In June 2003, the Council of State and Territorial Epidemiologists (CSTE) added respiratory illness due to SARS-CoV to the list of nationally reportable diseases reportable diseases, n.pl contagious diseases that must be reported by the physician to public health authorities. They include but are not limited to malaria, influenza, poliomyelitis, relapsing fever, typhus, yellow fever, cholera, and bubonic plague. . CDC has adopted the case definitions detailed in the CSTE position statement (31). This new definition, which was updated again on October 30, 2003, will improve the predictive value positive of national surveillance by considering "reports under investigation" that require monitoring and infection control as separate from cases of confirmed SARS-CoV disease that will be reported to the national system. The statement sets the stage for future SARS surveillance. CDC has developed a SARS preparedness plan for the United States that outlines in more detail recommendations for surveillance (32); as part of preparedness efforts, a Web-based surveillance module for SARS-CoV disease reporting is now in place. In the absence of recognized SARS cases, initial surveillance will likely consist of sentinel case detection with a focus on unexplained illnesses in healthcare workers and travelers returning from areas that were affected by SARS in the recent global outbreak. Because hospitals experienced high rates of transmission in affected areas, infection-control teams may additionally institute passive or active surveillance for pneumonia or fevers among staff and patients, combined with diagnostic testing for SARS-CoV. The intensity of surveillance efforts will need to be tailored to the degree of local transmission within both the community and healthcare facilities. Contact tracing In epidemiology, contact tracing is the identification and diagnosis of persons who may have come into contact with an infected person. For sexually transmitted diseases, this is generally limited to sexual partners but for highly virulent diseases such as Ebola and tuberculosis, a should rapidly identify possible early cases of secondary SARS and any unrecognized sources of infection for persons without epidemiologic links. Challenges remain, including how best to allocate limited public health resources for preparedness planning in light of the world's limited experience with SARS infections and how to synchronize See synchronization. national case definitions and reporting requirements with the systems established by international agencies, such as WHO. Although whether SARS will become a recurring problem is unclear, lessons learned while preparing for that eventuality e·ven·tu·al·i·ty n. pl. e·ven·tu·al·i·ties Something that may occur; a possibility. eventuality Noun pl -ties will be important for other global infectious disease Infectious disease A pathological condition spread among biological species. Infectious diseases, although varied in their effects, are always associated with viruses, bacteria, fungi, protozoa, multicellular parasites and aberrant proteins known as prions. outbreaks.
Table 1. Initial SARS case definition, U.S. surveillance,
March 17, 2003 (a)
Clinical criteria
Respiratory illness of unknown etiology with onset since February 1,
2003, including:
Measured temperature >38[degrees]C
Findings of respiratory illness (b)
Epidemiologic link criteria
Travel within 10 days of symptom onset to area with documented or
suspected community transmission of SARS (c)
OR
Close contact (d) within 10 days of symptom onset with either a
person with respiratory illness who had traveled to SARS area or
a person suspected to have SARS
(a) SARS, severe acute respiratory syndrome.
(b) For example, cough, shortness of breath, difficulty breathing,
hypoxia, or radiographic findings of either pneumonia or acute
respiratory distress syndrome; suspect cases with either radiographic
evidence of pneumonia or respiratory distress syndrome or evidence of
unexplained respiratory discuss syndrome by autopsy are designated
"probable" cases by the WHO case definition.
(c) Hong Kong Special Administrative Region and Guangdong Province,
Peoples' Republic of China; Hanoi, Vietnam; and Singapore.
(d) Having cared for, having lived with, or having had direct contact
with respiratory secretions or body fluids of patient suspected to
have SARS.
Table 2. CDC SARS case definition, United States, as of July 31,
2003 (a)
Case classification (b)
Probable case: meets the clinical criteria for severe respiratory
illness of unknown etiology and epidemiologic criteria; laboratory
criteria confirmed or undetermined
Suspect case: meets the clinical criteria for moderate respiratory
illness of unknown etiology and epidemiologic criteria; laboratory
criteria confirmed or undetermined
Clinical criteria
Asymptomatic or mild respiratory illness
Moderate respiratory illness: temperature >38[degrees]C (c) and one
or more clinical findings of respiratory illness (e.g., cough,
shortness of breath, difficulty breathing, hypoxia)
Severe respiratory illness: criteria for moderate respiratory
illness with radiographic evidence of pneumonia, respiratory
distress syndrome, or autopsy findings consistent with pneumonia or
respiratory distress syndrome without an identifiable cause
Epidemiologic link criteria
Travel (including airport transit) within 10 days of onset of
symptoms to area with current or recently documented or suspected
community transmission of SARS (Table 3) or close contact (d) within
10 days of symptom onset with person known or suspected to have
SARS
Laboratory criteria (e)
Confirmed: detection of antibody to SARS-CoV in a serum sample;
detection of SARS CoV RNA by RT-PCR confirmed by a second
PCR assay by using a second aliquot of the specimen and a different
set of PCR primers; or isolation of SARS-CoV
Negative: absence of antibody to SARS-CoV in convalescent serum
obtained >28 days after symptom onset (f)
Undetermined: laboratory testing not performed or incomplete
Exclusion criteria
Illness fully explained by alternative diagnosis (g)
Convalescent-phase serum sample (obtained >28 days after
symptom onset) negative for antibody to SARS-CoV.
Case reported on basis of contact with index case subsequently
excluded as SARS, provided other epidemiologic exposure criteria
are not present
(a) CDC, Centers for Disease Control and Prevention; SARS,
severe acute respirator syndrome: CoV, coronavirus; RT PCR,
reverse transcriptase-polymerase chain reaction.
(b) Asymptomatic SARS-CoV infection or clinical manifestations other
than respiratory illness might be identified as more is learned about
SARS-CoV infection.
(c) Measured documented temperature of >38[degrees]C is preferred;
however, clinical judgment should be used when evaluating patients
for whom temperature of>38[degrees]C has not been documented. Factors
that might be considered include patient self-report of lever, use of
antipyretics, presence of immunocompromising conditions or therapies,
lack of access to health care, or inability to obtain a measured
temperature. Reporting authorities should consider these factors
when classifying patients who do not strictly meet the clinical
criteria for this case definition.
(d) Close contact is defined as having cared for or lived with a
person known to have SARS or having a high likelihood of direct
contact with respiratory secretions or body fluids of a patient
with SARS. Examples of close contact include kissing or embracing,
sharing eating or drinking utensils, close conversation (<3 feel),
physical examination, and any other direct physical contact. Close
contact does not include activities such as walking near a person
or sitting across a waiting room or office for a brief period.
(e) Assays to diagnose SARS-CoV infection include enzyme linked
immunosorbent assay, indirect fluorescent-antibody assay, and
RT-PCR assays of appropriately collected clinical specimens.
Absence of SARS-CoV antibody from serum obtained <28 days
after illness onset, (f) a negative PCR test, or a negative
viral culture does not exclude SARS CoV infection and is not
considered a definitive laboratory result. In these instances,
a convalescent phase serum sample obtained >28 days after
illness is needed to determine infection with SARS-CoV. (f)
All SARS diagnostic assays are under evaluation.
(f) Does not apply to serum samples collected before July 11,
2003. Testing results from serum samples collected before July
11, 2003 and between 22 and 28 days after symptom onset are
acceptable and will not require collection of additional sample
>28 days after symptom onset.
(g) Factors that may be considered in assigning alternate
diagnoses include strength of epidemiologic exposure criteria
for SARS, specificity of diagnostic test, and compatibility
of clinical presentation and course of illness for alternative
diagnosis.
Table 3. Travel criteria for persons with suspect or probable
SARS, United States (a)
First date of illness Last date of illness
onset for inclusion as onset for inclusion as
Area reported case (b) reported case (c)
China (Mainland) November 1, 2002 July 13, 2003
Hong Kong February 1, 2003 July 11, 2003
Hanoi, Vietnam February 1, 2003 May 25, 2003
Singapore February 1, 2003 June 14, 2003
Toronto, Canada April 1, 2003 July 18, 2003
Taiwan May 1, 2003 July 25, 2003
Beijing, China November 1, 2002 July 21, 2003
(a) SARS, severe acute respiratory syndrome.
(b) The World Health Organization has specified that the
surveillance period for China should begin on November 1;
the first recognized cases in Hong Kong, Singapore, and Hanoi
(Vietnam) had onset in February 2003. The date for Toronto
is linked to laboratory-confirmed case of SARS in a U.S.
resident who had traveled to Toronto; the date for Taiwan
is linked to the Centers for Disease Control and Prevention
(CDC) travel recommendations.
(c) The last date for illness onset is 10 days (i.e., one
incubation period) alter removal of a CDC travel alert. The
case-patient's travel should have occurred on or before the
last date the travel alert was in place.
Table 4. Characteristics of SARS case-patients, U.S.
SARS surveillance, March 17-July 18, 2003 (a)
SARS-CoV
Overall positive
Probable, % Suspect, % Probable, %
Characteristic (n = 72) (n = 326) (n = 8)
Age (years)
0-4 15 14 0
5-9 4 4 0
10-17 3 2 0
18-64 58 73 100
[greater than or
equal to] 65 20 7 0
Sex
Female 44 47 50
Male 56 53 50
Race
White 47 58 37
Black 1 2 0
Asian 40 33 63
Other 2 0 0
Unknown 10 7 0
Exposure
Travel 83 81 88
Close contact 14 16 12
Health care worker 0 1 0
Unknown 3 2 0
Hospitalized
Yes 61 25 88
No 39 75 12
Unknown 0 1 0
Mechanically ventilated
Yes 3 1 12
No 89 93 88
Unknown 8 6 0
SARS-CoV negative
Probable, % Suspect, %
Characteristic (n = 39) (n = 167)
Age (years)
0-4 15 10
5-9 3 5
10-17 5 2
18-64 54 76
[greater than or
equal to] 65 23 7
Sex
Female 41 50
Male 59 50
Race
White 54 62
Black 0 2
Asian 36 28
Other 2 0
Unknown 8 8
Exposure
Travel 87 82
Close contact 13 17
Health care worker 0 0
Unknown 0 1
Hospitalized
Yes 59 26
No 41 73
Unknown 0 1
Mechanically ventilated
Yes 0 1
No 97 95
Unknown 3 4
SARS-CoV undetermined
Probable, % Suspect, %
Characteristic (n = 25) (n = 159)
Age (years)
0-4 20 19
5-9 8 4
10-17 0 0
18-64 52 70
[greater than or
equal to] 65 20 7
Sex
Female 48 45
Male 52 55
Race
White 40 53
Black 4 1
Asian 40 38
Other 0 2
Unknown 16 6
Exposure
Travel 84 81
Close contact 8 14
Health care worker 0 I
Unknown 8 4
Hospitalized
Yes 56 23
No 44 75
Unknown 11 2
Mechanically ventilated
Yes 4 1
No 80 91
Unknown 16 8
(a) SARS-CoV, severe acute respiratory syndrome-associated
coronavirus.
(b) This case-patient also traveled to Hone Kong and stayed
at Hotel M; however, onset of illness was 13 days after
returning to the United States.
Table 5. Results of diagnostic testing for other infectious
respiratory pathogens, U.S. SARS surveillance, March-July,
2003 (a),(b),(c)
SARS-CoV Mycoplasma Streptococcus Chlamydia
status pneumoniae pneumoniae pneumoniae (d)
Positive
Chest imaging 0/2 0/1 0/2
results (f) positive (0%) (0%) (0%)
Negative
Chest imaging 3/24 0/16 0/24
results positive (13%) (0%) (0%)
Chest imaging 11/99 5/71 2/95
results negative (11%) (7%) (2%)
Undetermined
Chest imaging 3/14 1/1 0/15
results positive (21%) (100%) (0%)
Chest imaging 5/61 0/1 0/61
results negative (8%) (0%) (0%)
Totals 22/200 6/90 2/197
(11%) (7%) (1%)
Para-
SARS-CoV Legionella Influenza influenza
status pneumophila HMPV A or B 1, 2, or 3
Positive
Chest imaging 0/2 0/1 1/1 0/1
results (f) positive (0%) (0%) (0%) (100%)
Negative
Chest imaging 0/24 2/22 0/21 1/22
results positive (0%) (9%) (0%) (5%)
Chest imaging 0/96 8/90 16/84 5/90
results negative (0%) (9%) (19%) (6%)
Undetermined
Chest imaging 0/14 1/13 1/13 2/13
results positive (0%) (8%) (8%) (15%)
Chest imaging 0/60 1/47 7/47 4/47
results negative (0%) (2%) (15%) (9%)
Totals 0/196 12/172 25/166 12/172
(0%) (7%) (15%) (7%)
SARS-CoV
status RSV Adenovirus Picornavirus (e)
Positive
Chest imaging 0/1 0/1 --
results (f) positive (0%) (0%)
Negative
Chest imaging 0/22 0/22 3/10
results positive (100%) (0%) (3%)
Chest imaging 2/90 5/90 12/45
results negative (2%) (6%) (27%)
Undetermined
Chest imaging 0/13 1/13 4/13
results positive (0%) (8%) (31%)
Chest imaging 1/47 3/47 10/46
results negative (2%) (6%) (22%)
Totals 3/172 9/172 29/114
(2%) (5%) (25%)
(a) SARS, severe acute respiratory syndrome; CoV-coronavirus; HMPV,
human metapneumovirus; RSV, respiratory syncytial virus; PCR,
polymerase chain reaction.
(b) Denominators for results of tests vary us specimens of appropriate
type and of adequate amount necessary for PCR and serologic testing
were obtained only for a subset of case-patients. Positive results
shown are those persons for whom evidence of acute infection was
demonstrated by serologic and/or PCR testing on the specimens
available for testing.
(c) Only one of the two SARS-CoV-positive case-patients had evidence
of infection with another agent (influenza B). For 22 suspect and
probable cases, more than one agent was identified. Combinations
included: HMPV, Influenza B (FluB) + S. pneumoniae (N = 1); Mycoplasma,
picornavirus + S. pneumoniae (N = 1); Mycoplasma + FluA (N = 5); HMPV
+ parainfluenza virus (HPIV) (N = 1); C. pneumoniae, adenovirus + FluB
(N = 1); Mycoplasma + picornavirus (N = 3); adenovirus + picornavirus
(N = 1); Mycoplasma + HPIV (N = 1); HPIV + picornavirus (N = 1);
HMPV + picornavirus (N = 1); Mycoplasma + picornavirus (N = 1);
S pneumoniae + picornavirus (N = 1); S. pneumoniae + HMPV (N = 1).
(d) All specimens tested for serologic or PCR evidence of C.
pneumoniae were also tested for evidence of C. psittaci; no acute
C. psittaci infections were diagnosed.
(c) Inclusive of rhinovirus and enterovirus.
(d) Plain film x-ray, computed tomographic scan, etc.
Acknowledgments We thank the state and local health departments and healthcare providers in the medical community whose efforts were the foundation for domestic SARS surveillance and reporting. We are grateful especially for the contributions made by the Council of State and Territorial Epidemiologists, the Association of Public Health Laboratories The Association of Public Health Laboratories (APHL) works to safeguard the public's health by strengthening government laboratories with a public health mandate in the United States and across the world. , the National Association of County and City Health Officials, the Association of State and Territorial Health Officials, Epidemic Intelligence Service The Epidemic Intelligence Service is a program of the United States' Centers for Disease Control and Prevention. Established in 1951 due to biological warfare concerns arising from the Korean War, it has become a hands-on two-year postgraduate training program in epidemiology, with Officers, Public Health Prevention Service Fellows, the CDC Emergency Operations Center The Emergency Operations Center, or EOC, is a central command and control facility responsible for carrying out the principles of emergency preparedness and emergency management, or disaster management functions at a strategic level in an emergency situation, and ensuring (EOC EOC Emergency Operations Center EOC Equal Opportunities Commission (UK) EOC Educational Opportunity Center EOC End Of Course EOC Epithelial Ovarian Cancer EOC Environment of Care (JCAHO) ), and Sherrie Bruce and Joseph Posid, who served as liaisons to the EOC. The following groups were instrumental in the surveillance effort: U.S. Domestic SARS Surveillance Team-Allen, D., Alexander, S., Amann, J., Anderson, S., Andre, M., Asamoa, K., Asrat, L., Auro, R., Avashia, S., Baker, N., Ballesteros, M., Banerjee, A., Bang, K.M., Barson, J., Basso, M., Beatty, M., Beltrami, E., Bensyl, D., Bhatti, L., Bialek, S., Borkowf, C., Boyer, S., Buchacz, K., Budnitz, D., Carter, K., Carter, M., Causer, L., Chamany, S., Chang, S., Chiller chill·er n. 1. One that chills. 2. A frightening story, especially one involving violence, evil, or the supernatural; a thriller. chiller Noun 1. , T., Chowdhary, J., Clark, T., Contractor, D., Coronado, F., Creek, T., Curtis, R., Dale, H., DeBerry, M., Dent, A., Doe, J., Dott, M., Dohle, S., Dong, M., Dunn, J., Espinoza, L., Fairley, T., Fehr, J., Felton, C., Filler, S., Finelli, L., Flannery, B., Fleischauer, A., Fox, L., Franklin, W., Fry, A., Funk, R., Gaffney, M., Gammino, V., Gay, T., Giroux, J., Gorina, Y., Gorwitz, R., Gottlieb, S., Griffith, K., Haddad, M., Hadden, W., Hammett, T., Heinen, M., Herrick, M., Hilsbos, K., Hooper, K., Horton, D.K., Houston, D., Hsu, V., Hutwagner, L., Ing, D., Jefferds, M., Jensen, K., Johnston, B., Jones, C., Jones, J., Jones, S., Kalluri, R, Kassim, S., Kaydos-Daneils, S., N., Kellerman, S., Khromova, A., Kile, J., Kirkland, E., Kretsinger, K., Kucik, J., Kyaw, M., LaMonte, A., Lash, B., Lobato, M., Loo, V., Luber, G., Lynch, M., MacKey, T., Malakmadze, N., Marano, N., McConnell, M., McCoy, S., McGowan, A., McLendon, T., Middleton, D., Miller, J., Miranda, A., Montgomery, J., Montagliani, H., Moore, K., Morano, J., Muralles, A., Nakib, S., Nadol, P., Nelson, L., Newman, L., Noggle, B., Norman, N., Park, B., Park, S., Peck, A., Perez, N., Pollack pollack: see cod. pollack or pollock Either of two commercially important North Atlantic species of food fish in the cod family (Gadidae). , L..A., Powell, T., Radke, M., Reefhuis, J., Rogers, M., Roy, S., Rumph-Person, D., Sahakian, N., Samandari, T., Sanchez, C., Sandhu, H., Shah, J., Shepard, C., Shetty, S., Smith, N., Sobel, J., Srikantiah, P., Stock, A., L., Stockton, M., Suen, J., Surdo, A., Tan, R., Teshale, E., Thomas, P., Tierney, B., Tun TUN, measure. A vessel of wine or oil, containing four hogsheads. , W., Turcios, R., Valdez, M., Varma, J., Victor, M., Vogt, T., Vong, S., Walker, F., Weintraub, E., Welsh, J., Williams, J., Williams, L., White, C., Whitehurst, J., Whiteman, M., Winston, L., Wong, D., Wright, J., Yeung, L., Zaudere, L., Zeitz-Ruckart, P., and Zhou, W.; SARS Laboratory Team--Balish, A., Beach, M., Carlone, G., Cox, N., Emery emery: see corundum. emery Granular rock consisting of a mixture of the mineral corundum (aluminum oxide, Al2O3) and iron oxides such as magnetite (Fe3O4) or hematite (Fe2O3). , S., Fields, B., Freeman, C., Glass, N., Goldsmith, N., Hall, Holder, P., H., Liu, G., Lu, X., Mabry, J., Messmer, T., Monroe, M., Nicholson, J., Robertson, B.J, Schwartz, S., Steiner, S., Stevens, V., Stinson, A., Warnock, D., Wilkins, P., and Wilson, M.; SARS Domestic Information Technology Team--Agyeman, K., Grissom, S., Karanam, P., Kass-Hout, T., Mason, N., Miller, C., Murphy, R., Nay, J., and Reed, D. 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Lee HKK HKK Hokitika, New Zealand - Hokitika (Airport Code) HKK Hava Kuvvetleri Komutanligi , Tso EYK EYK Expand Your Knowledge , Tsang OTW OTW Otherwise OTW Off The Wall OTW On the Way OTW On the Whole OTW Of The World (online TV network) OTW On The Web OTW Out the Window (display/graphics) OTW On The Water Choi KW, Lai TST TST 1 Toxic shock toxin 2 Treadmill stress test, see there . Asymptomatic severe acute respiratory syndrome-associated coronavirus infection. Emerg Infect Dis [serial online] 2003 Nov. Available from: URL: http://www.cdc.gov/ncidod/EID/vol9no11/03-0401.htm (29.) Hacker JK, Mark J, Erdman D, Fischer M, Espinosa A, Yagi S ya·gi n. pl. ya·gis A directional radio and television antenna consisting of a horizontal conductor with several insulated dipoles parallel to and in the plane of the conductor. , et al. Utility of sensitive molecular testing to evaluate suspect SARS cases in California (abstract V-796). Proceedings of the 43rd Interscience Conference on Antimicrobial Agents and Chemotherapy; 2003 Sept 14-17; Chicago. Washington: ASM Press; 2003. (30.) Mederski B, Zahariadis G, Latchford M, Ryall P and Hutchinson C. Occurrence of respiratory co-infections in persons suspected of having SARS. Abstract K-1315d. Proceedings of the 43rd Interscience Conference on Antimicrobial Agents and Chemotherapy; 2003 Sept 14-17; Chicago. Washington: ASM Press; 2003. (31.) Revision of CSTE case definition for severe acute respiratory syndrome (SARS) [monograph on the Internet]. Atlanta: Council of State and Territorial Epidemiologists; 2003 [cited 2003 Nov 19]. Available from: URL: http://www.cste.org/PS/2003pdfs/2003finalpdf/ CSTESARScasedefrevision2003-10-30.pdf (32.) Public health guidance for community-level preparedness and response to severe acute respiratory syndrome (SARS) [monograph on the Internet]. Atlanta: Centers for Disease Control and Prevention; 2003 [cited 2003 Oct 27]. Available from: URL: http://www.cdc.gov/ncidod/sars/sarsprepplan.htm Dr. Schrag is an epidemiologist in the Respiratory Diseases Branch, Division of Bacterial and Mycotic mycotic /my·cot·ic/ (mi-kot´ik) 1. pertaining to mycosis. 2. caused by a fungus. my·cot·ic adj. 1. Relating to mycosis. 2. Diseases, in the National Center for Infectious Diseases infectious diseases: see communicable diseases. , Centers for Disease Control and Prevention. For the national emergency response to SARS, Dr. Schrag participated as a coleader of the Domestic Epidemiology and Surveillance Team of CDC's Emergency Operations Center. Address for correspondence: Stephanie J. Schrag, Division of Bacterial and Mycotic Diseases, Respiratory Diseases Branch, National Center for Infectious Diseases, Centers for Disease Control and Prevention, 1600 Clifton Road Clifton Road is main street in Clifton neighborhood of Saddar Town in Karachi, Sindh, Pakistan. Its name dates from the British Colonial rule, and its market is posh areas of Karachi. N.E., Mailstop C23, Atlanta, GA 30333, USA; fax 404-6390-3970; email: zha6@cdc.gov The opinions expressed by authors contributing to this journal do not necessarily reflect the opinions of the Centers for Disease Control and Prevention or the institutions with which the authors are affiliated. Stephanie J. Schrag, * John T. Brooks, * Chris Van Beneden, * Umesh D. Parashar, * Patricia M. Griffin, * Larry J. Anderson, * William J. Bellini, * Robert F. Benson, * Dean D. Erdman, * Alexander Klimov, * Thomas G. Ksiazek, * Teresa C.T. Peret, * Deborah F. Talkington, * W. Lanier Thacker, * Maria L. Tondella, * Jacquelyn S. Sampson, * Allen W. Hightower, * Dale F. Nordenberg, * Brian D. Plikaytis, * Ali S. Khan, * Nancy E. Rosenstein, * Tracee A. Treadwell, * Cynthia G. Whitney, * Anthony E. Fiore, * Tonji M. Durant, * Joseph F. Perz, * Annemarie Wasley, * Daniel Feikin, * Joy L. Herndon, * William A. Bower, * Barbara W. Kilbourn,* Deborah A. Levy, * Victor G. Coronado, * Joanna Buffington, * Clare A. Dykewicz, * Rima F. Khabbaz, * and Mary E. Chamberland * * Centers for Disease Control and Prevention, Atlanta, Georgia, USA |
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