| Literature DB >> 23725337 |
Fang-Qiu Li1, Chun-Fang Ma, Li-Ning Shi, Jing-Fen Lu, Ying Wang, Mei Huang, Qian-Qian Kong.
Abstract
BACKGROUND: The yeast Candida is one of the most frequent pathogens isolated from bloodstream infections and is associated with significant morbidity and mortality. Problems with clinical and microbiological diagnosis of invasive candidiasis (IC) have prompted the development of non-culture-based laboratory methods. Previous reports suggest that serological detection of antibodies might be useful for diagnosing systemic candidiasis.Entities:
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Year: 2013 PMID: 23725337 PMCID: PMC3673856 DOI: 10.1186/1471-2334-13-253
Source DB: PubMed Journal: BMC Infect Dis ISSN: 1471-2334 Impact factor: 3.090
Base-line characteristics of the 475 subjects and results of serum testing
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|---|---|---|---|---|---|
| | | ||||
| Demographic factors | | | | | |
| Sex | | | | | |
| Male | 63 (73.0, 82.5)f | 41 (7.3; 7.3) | 52 (3.8,19.2) | 33 (6.1; 0) | 117 (2.6; 5.1) |
| Female | 38 (71.1, 94.7) | 9 (22.2; 22.2) | 32 (6.3; 9.4) | 7 (14.3; 14.3) | 83 (1.2; 2.4) |
| Age (years, mean ± SD) | 52.3 ± 19.6 | 76.12 ± 14.89 | 51.9 ± 14.2 | 57.6 ± 15.8 | 59.1 ± 12.4 |
| ≤65 years | 71 (69.0, 87.3)g | 9 (22.2; 44.4) | 48 (6.3; 14.6) | 28 (3.6; 0) | 108 (1.9; 4.6) |
| >65 years | 30 (80.0, 86.7) | 41 (7.3; 2.4) | 36 (2.8; 16.7) | 12 (16.7; 8.3) | 92 (2.2; 3.3) |
| Primary condition | | | | | |
| Hematological malignancy | 10 (60.0; 80.0) | 3 (33.3; 33.3) | 6 (33.3; 33.3) | 1 (0; 0) | 0 |
| Leukemia | 5 (40.0; 80.0) | 1 (0; 0) | 3 (33.3; 33.3) | | |
| Lymphoma | 3 (100.0; 66.7) | 1 (100.0; 100.0) | 2 (50.0; 50.0) | | |
| Myelodysplasia | 1 (0; 100.0) | 1 (0; 0) | 1 (0; 0) | | |
| Multiple myeloma | 1 (100.0; 100.0) | 0 (0; 0) | 0 (0; 0) | 1 (0; 0) | |
| Solid tumor | 11 (45.5; 81.8) | 7 (14.3; 28.6) | 10 (0; 30.0) | 0 | 0 |
| Bronchopulmonary neoplasm | 2 (50.0; 50.0) | 1 (0; 0) | 4 (0; 50.0) | | |
| Pancreas/colon adenocarcinoma | 7 (71.4; 85.7) | 6 (16.7; 33.3) | 5 (0; 20) | | |
| Bladder neoplasm | 2 (50.0; 100.0) | 0 (0; 0) | 1 (0; 0) | | |
| Nonmalignant diseases | 80 (77.5; 88.8) | 40 (7.5; 5.0) | 68 (2.9; 11.8) | 39 (7.7; 2.6) | 0 |
| Respiratory dysfunctionb | 5 (80.0; 60.0) | 18 (11.1; 5.6) | 3 (33.3; 33.3) | 21 (4.8; 4.8) | |
| Gastrointestinal pathologyc | 65 (75.4; 92.3) | 4 (25.0; 25.0) | 60 (1.7; 11.7) | 2 (100.0; 0) | |
| Othersd | 10 (90.0; 80.0) | 18 (0; 0) | 5 (0; 0) | 16 (0; 0) | |
| Risk factors | | | | | |
| Iatrogenic predisposing factors | | | | | |
| Broad spectrum antibiotics | 68 (76.5; 86.8)h | 44 (4.5; 2.3) | 64 (4.7; 9.4) | 20 (5.0; 5.0) | 0 |
| Glucocorticoids therapy | 57 (87.7; 91.2) | 40 (2.5; 2.5) | 46 (2.2; 2.2) | 0 (0; 0) | 0 |
| Central venous catheters | 36 (72.2; 88.9) | 28 (0; 0) | 27 (0; 0) | 9 (0; 0) | 0 |
| Parenteral nutrition | 56 (82.1; 92.9) | 15 (0; 0) | 49 (0; 0) | 3 (66.7; 0) | 0 |
| Other risk factors | | | | | |
| Intensive care unit stay | 26 (80.8; 92.3)i | 12 (8.3; 16.7) | 18 (5.6; 11.1) | 12 (16.7; 0) | 0 |
| Neutropeniae | 11 (36.4; 45.5) | 2 (0; 50.0) | 3 (0; 33.3) | 0 (0; 0) | 0 |
| Acute renal failure | 2 (50.0; 50.0) | 2 (50.0; 0) | 1 (100.0; 0) | 0 (0; 0) | 0 |
| Outcome of hospital stay | | | | | |
| Death | 36 (63.9; 88.9)j | 8 (37.5; 50.0) | 10 (20.0; 50.0) | 12 (8.3; 8.3)1,1 | nk |
| Discharge | 65 (76.9; 86.2) | 42 (4.8; 2.4) | 74 (2.7; 10.8) | 28 (7.1; 0) | nk |
a Patients with proven and probable IA.
bIncludes the following diseases: pneumonia, chronic obstructive pulmonary disease, and acute respiratory distress syndrome.
c Includes the following diseases: cholecystitis, angiocholitis, pancreatitis, peritonitis, and hepatitis.
d Includes the following diseases: multiple trauma, acute renal insufficiency, and diabetes mellitus.
e Neutropenia was defined as an absolute neutrophil count below 500 cells/mm3.
f,g,h,I,j No significant difference was found in patients with candidemia associated with age, sex, predisposing factors for IC and clinical outcomes (P > 0.05).
k Not applicable.
IgG antibodies and microbiological surveillance of patients with candidemia and colonization
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|---|---|---|---|---|---|---|---|---|
| 25 | 21 (84.0) | 37 | 1 (2.7) | 25 | 23 (92.0) | 37 | 2 (5.4) | |
| 20 | 9 (45.0) | 7 | 1 (14.3) | 20 | 16 (80.0) | 7 | 2 (28.6) | |
| 21 | 18 (85.7) | 1 | 0 (0) | 21 | 19 (90.5) | 1 | 0 (0) | |
| 10 | 7 (70.0) | 3 | 2 (66.7) | 10 | 8 (80.0) | 3 | 1 (33.3) | |
| 5 | 3 (60.0) | — | — | 5 | 5 (100.0) | — | — | |
| 20 | 15 (75.0) | 2 | 1 (50.0) | 20 | 17 (85.0) | 2 | 0 (0) | |
| Total | 101 | 73 (72.3)a | 50 | 5 (10.0) | 101 | 88 (87.1)b | 50 | 5 (10.0) |
2a =51.94, P < 0.01; 2b =84.1, P < 0.01, when compared with the control (patients with candida colonization).
Figure 1SDS-PAGE of recombinant enolase (Eno) and fructose-bisphosphate aldolase (Fba1). A. Lanes: 1, pET28a-Eno in E. coli BL21; 2, pET28a-Eno in E. coli BL21, induced by IPTG; 3, purified recombinant Eno. B. Lanes: 1, pET28a-Fba1 in E. coli BL21; 2, pET28a-Fba1 in E. coli BL21, induced by IPTG; 3, purified recombinant Fba1. Molecular markers (in kDa) of standard proteins are to the left.
Figure 2Antibody levels in study patients (A: anti-Eno and B: anti-Fba1). Patients with candidemia, Candida colonization, bacteremia, invasive aspergillosis and healthy controls were evaluated for the presence of anti-Eno and anti-Fba1 antibodies. The levels of anti-Eno and anti-Fba1 in patients with candidemia were higher than control groups. Boxes indicate interquartile ranges (25–75th percentiles). Horizontal bars in bold indicate the median value in each group. Whiskers extend to 1.5 times the interquartile range. *P < 0.001, for the comparison with the patients with candidemia; **P < 0.001, for the comparison with the patients with candidemia.
Figure 3Anti-Eno and anti-Fba1 antibody titers in patients with candidemia and control groups. A, anti-Eno titers; B, anti-Fba1 titers. In 73 anti-Eno positive patients, 32 at a titer of 1:500, 41 at titers ≥1:1000. In 88 anti-Fba1 positive patients, 81 were tested titers, 33 at a titer of 1:500, 48 at titer ≥1:1000. In 15 anti-Eno positive control individuals, only one at a titer of 1:1000. In 26 anti-Fba1 positive control individuals, 3 at a titer of 1:1000. None control individuals at titer >1:1000.
Diagnostic value of anti-Eno and anti-Fba1 on the test cohort
| True negative | 354 | 347 | 339 |
| False positive | 20 | 27 | 35 |
| True positive | 73 | 88 | 91 |
| False negative | 28 | 13 | 10 |
| Sensitivity (%) | 72.3 | 87.1 | 90.1 |
| Specificity (%) | 94.7 | 92.8 | 90.6 |
| Negative predictive value (%) | 93.0 | 96.4 | 97.1 |
| Positive predictive value (%) | 78.5 | 76.5 | 72.2 |
The number of patients is presented in the upper part of the table. Sensitivity, specificity, and positive and negative predictive values are estimated in percentage calculated from patient responses. In the combined detection of anti-Eno and anti-Fba1, sera with single or both assay positive results were regarded as positive.
Positive rate and timing of anti-Eno and anti-Fba1 antibodies in non-neutropenic and neutropenic patients with candidemia [(%)]
| Non-neutropenia (90) | 38 (42.2) | 31 (34.4) | 69 (76.7) | 46 (51.1) | 37 (41.1) | 83 (92.2) |
| Neutropenia# (11) | 3 (27.3) | 1 (9.1) | 4 (36.4)a | 4 (36.4) | 1 (9.1) | 5 (45.5)b |
| Total (101) | 41 (40.6) | 32 (31.7) | 73 (72.3) | 50 (49.5) | 38 (37.6) | 88 (87.1) |
*Ab: antibody, ** BC: blood culture.
#Neutropenia was defined as an absolute neutrophil count below 500 cells/mm3.
aP = 0.005, for the comparison with the Non-neutropenia group.
bP < 0.001, for the comparison with the Non-neutropenia group.