To assess the circumstances of recent transmission of tuberculosis (TB) (progression to active disease
Although tuberculosis (TB) remains a major public health threat worldwide (
Molecular epidemiology has been used to identify groups most at risk for recent TB transmission in high-incidence urban and rural areas of the United States (
In spite of the presence of these groups at high risk of acquiring TB, excellent treatment regimens utilizing directly observed therapy (87% vs. 47% nationally) and four-drug initial therapy (89% vs. 77% nationally) resulted in a 15-year decline in disease incidence (
As part of the CDC-supported National Tuberculosis Genotyping and Surveillance Network, we used DNA fingerprinting of
For all culture-positive patients with available DNA fingerprints, we obtained routinely reported demographic and risk factor information (HIV infection, homelessness, incarceration, alcohol abuse and illegal drug use, long-term care residence, and foreign birth) from the state case registry. These data were used to compare patients by estimated time of TB acquisition.
After obtaining genotype results, we abstracted medical records of the clustered patients to determine whether epidemiologic links existed with other patients in the same cluster. We obtained medical histories and information on workplaces, schools, social settings, known or suspected TB exposures, tuberculin skin test results, and contact investigation records. Locatable clustered patients who had no documented links were interviewed to determine whether an existing relationship had eluded the local health department staff who conducted the contact investigations. We assigned epidemiologic links to patients who were named by another TB patient or were in the same place at the same time as another TB patient, even when they did not name each other. When the date and location of specimen collection and laboratory processing suggested that a clustered patient’s specimen was falsely positive, a pulmonologist reviewed medical records and chest radiographs to determine whether clinical TB was likely (
Patients with “recent TB” were defined as those who had become infected within 2 years of disease diagnosis by an identified source patient with a matching fingerprint and whose transmission setting was known. Symptom onset had to occur at least 1 month after the onset date of the source’s symptoms. The date was obtained from the patient’s report or conservatively estimated to be 14 days before the date the first positive specimen was collected or the date that treatment was begun, whichever came first. Patients with “probable recent TB” were defined as all clustered patients who had no known transmission from source patients or evidence of past infection, e.g., no history of previous disease or documented positive results of a tuberculin skin test.
The category of “reactivated TB” from latent TB infection was assigned to clustered patients with documented past infection or disease and no identified source case, and to all patients with unique
Traditional settings for transmission were defined as those settings routinely investigated during contact investigations, e.g., households and transmission between close friends and relatives in any location. All other settings where transmission occurred were considered nontraditional.
Using only clustered patients as a convenience sample, we compared the times from reported symptom onset to treatment initiation between transmitters (persons who were the source of infection for a patient with recent TB) and nontransmitters (persons who were never identified as a source for another patient). The possibility of transmission was evaluated through July 2002, 19 months after the last patient in the study was reported.
Patients with
Chi-square tests were conducted for all categorical analyses; Fisher exact test was used when expected cell values were <5. Student
Of 1,554 TB patients reported from 1996 through 2000, a total of 1,198 (77%) had positive cultures. The cluster investigations revealed that specimens from 11 patients were false positive, and these were deleted from our state TB registry. Five patients with
Of the 1,172 patient isolates, 436 (37%) were grouped in 111 clusters (median patients per cluster 2; mean 3; range 2–19). Eighty-eight (79%) clusters included persons who resided in one or two adjacent jurisdictions within the state. Overall, 155 (36%) clustered patients were epidemiologically linked to another patient in the cluster; among 336 with high-copy IS
The time of TB acquisition could not be determined for 42 patients who were the first symptomatic patients in their respective cluster and had no known source patient, and 145 patients who had low-copy IS
| DNA cluster status of patients’ isolates | No. patients with recent TB | No. patients with probable recent TB | No. patients with reactivated TB | No. patients with unknown time of TB acquisition | Totals |
|---|---|---|---|---|---|
| Clustered strains with >6 IS | 89 | 82 | 56b | 42c | 269 |
| Clustered strains with | 22 | 0 | 0 | 145 | 167 |
| Nonclustered strains | 4d | 0 | 732 | 0 | 736 |
| Total | 115 | 82 | 788 | 187 | 1,172 |
aTB, tuberculosis. bHistory of previous positive tuberculin skin test or extensive past exposure to a patient. cFirst patient in a cluster by estimated date of symptom onset and no identified source patient. dKnown link to another patient outside the study area or timeframe whose isolate had the same DNA fingerprint.
Of the 985 patients with a known time of infection and subsequent disease, 115 (12%) had recent TB and an additional 82 (8%) had probable recent TB. Fourteen (17%) of these 82 had documented previous negative skin tests. Our extensive case review showed no sources for 56 clustered patients who had documented histories of past infection or disease. We presumed that these 56 patients plus the 732 patients with unique
Patients with recent TB were significantly more likely than patients with probable recent TB to be young and U.S. born, but the proportions of patients with urban residence, HIV infection, illegal drug use, and homelessness were similar for both groups (
| No. patients with recent TB (%)
(N=115) | No. patients with probable
recent TB (%)
(n=82) | No. patients with reactivated TB (%)
(n=788) | p value | p value | |
|---|---|---|---|---|---|
| Characteristic | Group A | Group B | Group C | A vs. B | A vs. C |
| Residence | |||||
| Baltimore City | 57 (50.0) | 38 (46.3) | 157 (19.9) | 0.66 | <0.001 |
| Other state jurisdictions | 58 (50.0) | 44 (53.7) | 631 (80.1) | ||
| Age group (yrs) | |||||
| 0–14a | 6 (5.2) | 3 (3.7) | 5 (0.6) | <0.001 | <0.001 |
| 15–24 | 21 (18.3) | 7 (8.5) | 86 (10.9) | ||
| 25–44 | 46 (40.0) | 27 (32.9) | 275 (34.9) | ||
| 45–64 | 33 (28.7) | 20 (24.3) | 178 (22.6) | ||
| 9 (7.8) | 25 (30.4) | 244 (31.0) | |||
| Race/ethnicity | |||||
| White, non-Hispanic | 20 (17.4) | 17 (20.7) | 162 (20.6) | 0.03 | <0.001 |
| Black, non-Hispanic | 89 (77.4) | 51 (62.2) | 341 (43.3) | ||
| Hispanic | 1 (0.9) | 5 (6.1) | 84 (10.7) | ||
| Asian | 5 (4.3) | 9 (11.0) | 200 (25.4) | ||
| Native American | 0 | 0 | 1 (0.1) | ||
| Country of birth | |||||
| United States | 105 (91.3) | 66 (80.5) | 360 (45.7) | 0.03 | <0.001 |
| Other | 10 (8.7) | 16 (19.5) | 428 (54.3) | ||
| Long-term care resident | |||||
| Yes | 7 (6.1) | 5 (3.3) | 25 (3.2) | 1.00 | 0.11 |
| No | 108 (93.9) | 77 (96.7) | 763 (96.8) | ||
| Homeless | |||||
| Yes | 18 (15.7) | 8 (9.8) | 23 (2.9) | 0.22 | <0.001 |
| No | 97 (84.3) | 74 (90.2) | 765 (97.1) | ||
| Prison resident | |||||
| Yes | 13 (11.3) | 10 (13.1) | 21 (2.7) | 0.85 | <0.001 |
| No | 102 (88.7) | 72 (86.9) | 767 (97.3) | ||
| Uses illegal drugs or abuses alcohol | |||||
| Yes | 53 (46.0) | 30 (36.6) | 76 (9.6) | 0.18 | <0.001 |
| No | 62 (54.0) | 58 (63.4) | 712 (90.4) | ||
| HIV-infected | |||||
| Yes | 28 (24.3) | 19 (23.2) | 75 (9.5) | 0.85 | <0.001 |
| No | 87 (75.7) | 63 (76.8) | 713 (90.5) | ||
| aIncludes one child < 6 years old without a known source patient; the case was classified as recent based on age. | |||||
Of the 115 patients with recent TB, 114 had 69 sources with available risk information. The mean number of secondary patients per source was 1.6 (median 1; range 1–12). Six (5%) of the 114 secondary patients acquired a resistant
Source cases and settings of transmission were identified for all instances of recent transmission except one, a 3-year-old child (n=114). Fifty-six (49%) patients with recent TB acquired their infection and disease in nontraditional settings (
| Settings | Total patients with known settings (%) | Setting identified by routine contact investigation (%) | Setting identified by DNA cluster investigation (%) |
|---|---|---|---|
| Traditional Household Close relative Close friend Nontraditional Hospital (23,28) Other workplace (24) Social club (25) Homeless shelter Bar Prison/jail (26) Store (27) Church Nursing home School Ship Mortuary (29) Total | 28 (24.6) 13 (11.4) 17 (14.9) 10 (8.8) 6 (5.3) 11 (9.6) 5 (4.4) 10 (8.8) 5 (4.4) 2 (1.8) 2 (1.8) 1 (0.9) 1 (0.9) 1 (0.9) 114 (100.0) | 25 (34.7) 13 (18.1) 11 (22.2) 5 (6.9) 6 (8.3) 7 (9.7) 0 1 (1.4) 3 (4.2) 0 0 0 0 1 (1.8) 0 (1.4) 72 (100.0) | 3 (7.1) 0 6 (14.3) 5 (11.9) 0 4 (9.5) 5 (11.9) 9 (21.4) 2 (4.8) 2 (4.8) 2 (4.8) 2 4.8) 1 (2.4) 0 (2.4) 42 (100.0) |
The importance of nontraditional settings among persons at high risk was influenced in part by large outbreaks (three or more secondary patients) (
TB acquisition in nontraditional settings was associated with age >14 years (p=0.033, when differences between older and younger patients were compared), U.S. birth (p=0.012, compared to foreign birth), and illegal drug use (p<0.001, comparing differences between users and nonusers). At least 5 of 15 patients who acquired TB in public settings, i.e., churches, hospitals, a school, and a store, had only brief or distant (casual) exposure to a highly infectious person (
TB transmission occurred in households for all 10 foreign-born persons with recent TB, and the sources for all but one foreign-born patient were found by contact investigations (
| Characteristic | Total recent TB patients (n=114) (%) | Source patient identified by routine contact investigation (n=72) (%) | Source patient identified by cluster investigation (n=42) (%) | p value |
|---|---|---|---|---|
| Residence | ||||
| Baltimore city | 56 (49.0) | 33 (45.8) | 23 (54.8) | 0.38 |
| Other state jurisdictions | 58 (51.0) | 39 (54.2) | 19 (45.2) | |
| Country of birth | ||||
| United States | 104 (91.3) | 63 (87.5) | 41 (97.6) | 0.07 |
| Other | 10 (8.7) | 9 (12.5) | 1 (2.4) | |
| Long-term care resident | ||||
| Yes | 7 (6.1) | 3 (4.2) | 4 (9.5) | 0.25 |
| No | 107 (93.9) | 69 (95.8) | 38 (90.5) | |
| Homeless | ||||
| Yes | 18 (15.8) | 6 (8.3) | 12 (28.6) | 0.004 |
| No | 96 (84.2) | 66 (91.7) | 30 (71.4) | |
| Prison resident | ||||
| Yes | 13 (11.4) | 8 (11.1) | 5 (11.9) | 0.86 |
| No | 101 (88.6) | 64 (88.9) | 37 (88.1) | |
| Abuses alcohol | ||||
| Yes | 40 (35.0) | 19 (26.4) | 21 (50.0) | 0.01 |
| No | 74 (65.0) | 53 (73.6) | 21 (50.0) | |
| Uses injection drugs | ||||
| Yes | 17 (14.9) | 11 (15.3) | 6 (14.3) | 0.89 |
| No | 97 (85.1) | 61 (84.7) | 36 (85.7) | |
| Uses noninjection drugs | ||||
| Yes | 35 (30.7) | 23 (31.9) | 12 (28.6) | 0.71 |
| No | 79 (69.3) | 49 (68.1) | 30 (71.4) | |
| HIV-infected | ||||
| Yes | 28 (24.6) | 16 (22.2) | 12 (28.6) | 0.45 |
| No | 86 (75.4) | 56 (77.8) | 30 (71.4) |
The estimated time of symptom onset was available for 69 transmitters and 99 nontransmitters. TB transmitters were significantly more likely than nontransmitters to have pulmonary disease (68/69 vs. 73/99; p<0.001). Among patients with pulmonary disease, transmitters were more likely than nontransmitters to have lung cavitation (40/68 vs. 14/73; p<0.001) and sputum smears positive for acid-fast bacilli (64/68 vs. 59/73; p=0.034). Among transmitters, the mean time from symptom onset to treatment initiation was 16.8 weeks compared with 8.5 weeks among nontransmitters (median 11 vs. 6 weeks, respectively; p=0.008). Transmitters also were more likely than nontransmitters to have at least one risk factor for TB, e.g., homelessness, HIV infection, alcohol abuse, or illegal drug use, residence in a long-term care facility, incarceration, foreign birth (60/69 vs. 38/99, respectively; p<0.001).
Our 5-year molecular epidemiologic study featured a complete sampling of patients’ isolates from the entire state (
The importance of clustered patients who do not have identifiable links has remained unclear (
Patients with reactivated disease were rarely misclassified. Among clustered patients with histories of old infection, disease, or both, our extensive review revealed no source patients. In addition, as of July 2002, we found no instances of exogenous reinfection by a different
Most recent transmission occurred between U.S.-born persons who had at least one common urban risk factor such as HIV infection or illegal drug use. In contrast, transmission between foreign-born persons occurred exclusively in households among persons who had no other risk except their arrival from a high-incidence country of origin or close exposure to their source patient. We found no instances of transmission between U.S.-born and foreign-born persons. These results differed from other studies, which reported that foreign-born patients who acquired TB from U.S.-born sources shared risks such as homelessness, HIV infection, and illegal drug use with those source patients (
In spite of a recommended concentric circle approach for routine contact investigations that includes leisure and social locations (
Perhaps more importantly, almost half of recent TB cases were acquired in nontraditional settings. Many of these patients were from marginalized groups at high risk, who may have been reluctant or unable to provide names of their associates to contact investigators. However, cluster and contact investigations were equally effective in identifying sources for patients with recent TB who were users of illegal drug users, incarcerated, and HIV-infected, and more aggressive contact investigations could probably not substantially improve patient reporting. Instead, our data suggest that the setting and not the risk group eludes routine contact investigators.
In addition, TB genotyping and cluster investigations indicated unsuspected transmission to immunocompetent persons in public locations such as churches, hospitals, and stores. In these instances, the possibility of casual transmission must be considered. Casual transmission was likely in the store outbreak (
The mean time between reported symptom onset and initiation of treatment among transmitters was twice that identified for nontransmitters. Whether treatment delays are due to patients who delay in seeking care or to providers who do not include TB in the differential diagnosis, treatment delays provide ample time for pulmonary TB patients to develop smear-positive disease and cavitation (
Even with excellent treatment indices, one sixth of Maryland’s patients with positive cultures had recent or probable recent disease. The new guidelines for targeted testing and treatment for latent TB infection (
Actions needed to decrease recent tuberculosis transmission in various settings. Decreasing diagnostic delays can potentially eliminate large point source clusters and substantially reduce transmission in both traditional and nontraditional settings. CI, contact investigation.
We thank Sarah Bur, Richard E. Chaisson, and Timothy R. Sterling for their thoughtful reviews of this manuscript, Bianca Oden for her work on the figures, and the Division of Tuberculosis Elimination, Centers for Disease Control and Prevention, for supporting the Maryland statewide molecular epidemiology project (U52-CCU300500).
Dr. Cronin is an epidemiologist with the Division of Tuberculosis Control, Refugee and Migrant Health, Maryland Department of Health and Mental Hygiene, and currently the coprincipal investigator for the Maryland site of the Tuberculosis Epidemiologic Studies Consortium, supported by the Centers for Disease Control and Prevention. Her primary research interest includes epidemiology, particularly molecular epidemiology related to the prevention of tuberculosis and nosocomial infections.