| Literature DB >> 28056845 |
Yusuke Koizumi1,2, Kaoru Shimizu3, Masayo Shigeta3, Takafumi Okuno4, Hitoshi Minamiguchi4, Katsuyuki Kito4, Keiko Hodohara4, Yuka Yamagishi5, Akira Andoh4, Yoshihide Fujiyama4, Hiroshige Mikamo5.
Abstract
BACKGROUND: Febrile neutropenia (FN) is a common infectious complication in chemotherapy. The mortality of FN is higher in hematologic malignancy patients, and early diagnostic marker is needed. Presepsin is a prompt and specific marker for bacterial sepsis, but its efficacy in severe febrile neutropenia (FN) is not well confirmed. We tried to clarify whether it is a useful maker for early diagnosis of FN in patients during massive chemotherapy.Entities:
Keywords: Bacteremia; CD14; Chemotherapy; Febrile neutropenia; Presepsin(soluble CD14-ST)
Mesh:
Substances:
Year: 2017 PMID: 28056845 PMCID: PMC5217328 DOI: 10.1186/s12879-016-2116-8
Source DB: PubMed Journal: BMC Infect Dis ISSN: 1471-2334 Impact factor: 3.090
Patient characteristics
| Comorbidities | Acute myeloid leukemia | 3 |
| multiple myeloma | 2 | |
| malignant lymphoma | 2 | |
| acute lymphoid leukemia | 1 | |
| myelodysplastic syndrome | 1 | |
| aplastic anemia | 1 | |
| chemotheapy | induction therapy | 6 |
| conditioning regimen hematopoietic stem cell transplantation | 3 | |
| consolidation therapy | 1 | |
| Nadir WBC count during the chemotherapy | 0–100/μL | 9 |
| 101–500/μL | 1 | |
| 501- /μL | 0 | |
| focus of infectiona | primary bacteremia | 9 |
| severe pneumonia | 1 | |
| skin & soft tissue infection | 1 | |
| pathogens identified in blood cultures | ||
| Gram negatives | 6 | |
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| 3 | |
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| 1 | |
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| 1 | |
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| 1 | |
| Gram positives | 5 | |
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| 1 | |
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| 1 | |
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| 1 | |
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| 1 | |
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| 1 | |
| days of the infection onsetb | 11.9 [3–18] | |
| average number of the samples examined for presepsin | 6.5 [4–9] | |
afocus denotes the entry site of bacteremia
bday 1 is defined as the day when chemotherapy regimen starts
Fig. 1Plasma presepsin level change over time and comorbidities. Changes in plasma presepsin level over time in lymphoid malignancy cases (a) and myeloid malignancy cases (b) are shown. Horizontal axis shows the day of chemotherapy. The average of plasma presepsin level was lower in myeloid malignancies. Note that most of the presepsin values are above 100 pg/mL, suggesting that it maintains certain levels even in severe neutropenic state
Fig. 2Plasma presepsin levels and other parameters measured at the same time point. a Plasma presepsin levels white blood cell count. White blood cell count and plasma presepsin levels were plotted. Plasma presepsin levels were not significantly associated to the absolute white blood cell count(r = −0.19, p = 0.19). Plasma presepsin level was not associated with neutrophil count, or monocyte count, either (data not shown). b Plasma presepsin levels and C-reactive protein (CRP) levels. CRP levels and plasma presepsin levels were plotted. Plasma presepsin levels were strongly associated to the CRP levels. (r = 0.61, p < 0.01)
Plasma onset presepsin levels and increase rates in 11 febrile neutropenia cases with identified pathogens (FN group) and 4 afebrile neutropenia cases (AFN group)
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| Case | Commobidity | Pathogen identified in blood culture | Baseline level | Onset level | Previous level | blood examination intervala | Increase rate | Onset /Baseline ratio | Blood cell counts at onset day (/μL) | Remarks | |
| (pg/mL) | (pg/mL) | (pg/mL) | (day) | WBC | neutrophils | ||||||
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| AML |
| 280 | 760 | 329 | 4 | 33% | 2.71 | 300 | 3 | pneumonia(ARDS) ▪ ICU stay |
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| AML |
| 206 | 562 | 296 | 3 | 30% | 2.73 | 200 | 0 | bacteremia |
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| ALL |
| 187 | 558 | 279 | 2 | 50% | 2.98 | 200 | 0 | bacteremia |
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| MDS |
| 169 | 341 | 186 | 2 | 42% | 2.02 | 200 | 0 | bacteremia |
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| ML |
| 330 | 1810 | 330 | 4 | 112% | 5.48 | 100 | 0 | bacteremia |
| bacteremia | |||||||||||
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| MM |
| 201 | 884 | 201 | 10 | 33% | 4.4 | <100 | 0 | bacteremia + diverticulitis |
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| 229 ± 62.4 | 819 ± 520 | 50% | 3.39 ± 1.29 | |||||||
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| ML |
| 320 | 644 | 361 | 2 | 39% | 2.01 | <100 | 0 | bacteremia + HPS |
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| MM |
| 116 | 503 | 234 | 2 | 57% | 4.34 | <100 | 0 | bacteremia + CRBSI |
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| MDS |
| 169 | 460 | 151 | 4 | 51% | 2.72 | <100 | 0 | bacteremia |
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| AA |
| 106 | 275 | 106 | 4 | 40% | 2.59 | 300 | 250 | bacteremia + CRBSI |
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| AML |
| 333 | 217 | 211 | 2 | 1% | 0.65 | <100 | 0 | bacteremia + meningitis |
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| 209 ± 110.2 | 420 ± 174 | 38% | 2.46 ± 1.33 | |||||||
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| 220 ± 83.1 | 638 ± 437 | 44% | 2.97 ± 1.33 | |||||||
| AFN group | |||||||||||
| Case | Commobidity | Pathogen identified in blood culture | Baseline level | Onset levelb | Previous level | Blood examination intervala | Increase rate | Onset /Baseline ratio | Blood cell counts at onset day (/μL) | Remarks | |
| (pg/mL) | (pg/mL) | (pg/mL) | (day) | WBC | neutrophils | ||||||
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| AML | 174 | 223 | 172 | 2 | 15% | 1.28 | 400 | 48 | ||
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| AML | 138 | 298 | 137 | 2 | 59% | 2.16 | 100 | 0 | ||
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| MM | 49 | 188 | 89 | 5 | 22% | 3.84 | 100 | 0 | ||
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| ML | 120 | 247 | 136 | 7 | 12% | 2.06 | 100 | 0 | ||
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| 120 ± 52.5 | 239 ± 46.2 | 27% | 2.33 ± 1.08 | |||||||
Abbreviations: ARDS acute respiratory distress syndrome, CRBSI catheter related blood stream infection, HPS hemophagocytic syndrome, WBC white blood cell
ablood examination interval denotes the interval between peak level and previous level (day)
bin the AFN group, onset level denotes the highest value within one chemotherapy course
Fig. 3Plasma presepsin levels in representative cases. a Case 3; 48 year old male with B-ALL, undergoing “JALSG Ph(−) B-ALL 213 consolidation” chemotherapy. He experienced K.pneumoniae bacteremia on day 10. WBC count was 200/mL and plasma presepsin level was already elevated one day prior FN onset. CRP was not elevated at this time. b Case 4; 68 year old female with MDS and Sweet disease, undergoing induction chemotherapy (MEC-GO). Plasma presepsin level was not elevated in spite of marked leukocytosis (day1) or non-infectious fever caused by erythema nodosa (day24). It was elevated at the onset of S.hominis bacteremia (day8), and at K.pneumoniae bacteremia (day15)