Systematic Review
Copyright ©The Author(s) 2019.
World J Hepatol. Jul 27, 2019; 11(7): 596-606
Published online Jul 27, 2019. doi: 10.4254/wjh.v11.i7.596
Table 1 Management, prognosis and mortality in cirrhotic patients with spontaneous fungal peritonitis
StudyCountry, settingStudy designStudy populationManagement
Mortality
n (%)n (%)
Hwang et al[10], 2014South Korea, University HospitalRetrospective, Cross-sectionaln = 416 patients3rd generation cephalosporin (n = 15)In-hospital: -
SBP (n = 401)Antifungal: n = 5 (33.3%)1-mo: 11/15 (73.3%)
SFP (n = 4)Amphotericin B: n = 26-mo: 3/15 (20%)
Polymicrobial SFP (n = 11)Liposomal Amphotericin B: n = 1
Fluconazole: n = 2
Hassan et al[9], 2014Egypt, University HospitalProspective cohort studyn = 46 patientsNot describedIn-hospital: 1/3 (33.33%)
Control patients with no infection (n = 18)
SFP (n = 4; only 3 patients described with ascitic fluid polymorphs > 250 cells/mm3)
Karvellas et al[11], 2015(CATSS Database) from 28 medical centers in United States, Canada, Saudi ArabiaRetrospective cohort studyn = 126 patientsAnti-fungal: n = 9 (81.8%)In-hospital: 11/11 (100%)
SBP (n = 126)
SFP and SBP (n = 11)
Bremmer et al[1], 20151University of Pittsburgh, United StatesRetrospective, cross-sectional studyn = 25Antifungal: n = 15 (60%)In hospital: 15/25 (60%)
SFP (n = 25)One mo: 14/25 (56%)
Lahmer, et al[2], 2016University Hospital, GermanyRetrospective, cross-sectional studyn = 208 SFP (n = 20)Antibiotic pretreatment: SFP n = 17 Antifungal: n = 6 (30% of SFP)In-hospital: 18/20 (90%)
SBP (n = 28)
Gravito-Soares et al[6], 2017University of Coimbra, Coimbra, PortugalRetrospective, case–control studyn = 231Cefotaxime n = 2311 -mo: 4/8
SFP (n = 3)Antifungal: n = 5/8 (62.5%)(50%)
Polymicrobial SFP (n = 5)Fluconazole: n = 3
SBP (n = 119)Caspofungin: n = 1
Amphotericin B: n = 1
1The study was described as a retrospective cohort study design but in the absence of a comparative non-exposure/control group we decided it more appropriately fitted the description of a cross—sectional study. SBP: Spontaneous bacterial peritonitis; SFP: Spontaneous fungal peritonitis.
Table 2 Quality assessment of included observational cohort and cross-sectional studies according to NHBLI Quality Assessment Tool
Hwang et al[10], 2014Hassan et al[9], 2014Karvellas et al[11], 2015Bremmer et al[1], 2015Lahmer et al[2], 2016
1 Was the research question or objective in this paper clearly stated?YesYesYesYesYes
2 Was the study population clearly specified and defined?YesYesYesYesYes
3 Was the participation rate of eligible persons at least 50%?YesYesYesYesYes
4 Were all the subjects selected or recruited from the same or similar populations (including the same time period)? Were inclusion and exclusion criteria for being in the study prespecified and applied uniformly to all participants?YesYesYesYesYes
5 Was a sample size justification, power description, or variance and effect estimates provided?NoNoNoNoNo
6 For the analyses in this paper, were the exposure(s) of interest measured prior to the outcome(s) being measured?YesYesYesYesYes
7 Was the timeframe sufficient so that one could reasonably expect to see an association between exposure and outcome if it existed?YesYesYesYesYes
8 For exposures that can vary in amount or level, did the study examine different levels of the exposure as related to the outcome (e.g., categories of exposure, or exposure measured as continuous variable)?NANAYesNANA
9 Were the exposure measures (independent variables) clearly defined, valid, reliable, and implemented consistently across all study participants?YesYesYesYesYes
10 Was the exposure(s) assessed more than once over time?NoNoNoNoNo
11 Were the outcome measures (dependent variables) clearly defined, valid, reliable, and implemented consistently across all study participants?YesYesYesYesYes
12 Were the outcome assessors blinded to the exposure status of participants?NoNoNoNoNo
13 Was loss to follow-up after baseline 20% or less?YesYesYesYesYes
14 Were key potential confounding variables measured and adjusted statistically for their impact on the relationship between exposure(s) and outcome(s)?NoYesYesYesYes
RatingGoodGoodGoodGoodGood
Table 3 Quality assessment of included case-control studies according to NHBLI Quality Assessment Tool
Gravito-Soares et al[6], 2017
1 Was the research question or objective in this paper clearly stated?Yes
2 Was the study population clearly specified and defined?Yes
3 Did the authors include a sample size justification?No
4 Were controls selected or recruited from the same or similar population that gave rise to the cases (including the same timeframe)?Yes
5 Were the definitions, inclusion and exclusion criteria, algorithms or processes used to identify or select cases and controls valid, reliable, and implemented consistently across all study participants?No
6 Were the cases clearly defined and differentiated from controls?Yes
7 If less than 100 percent of eligible cases and/or controls were selected for the study, were the cases and/or controls randomly selected from those eligible?NA
8 Was there use of concurrent controls?No
9 Were the investigators able to confirm that the exposure/risk occurred prior to the development of the condition or event that defined a participant as a case?Yes
10 Were the measures of exposure/risk clearly defined, valid, reliable, and implemented consistently (including the same time period) across all study participants?Yes
11 Were the assessors of exposure/risk blinded to the case or control status of participants?No
12 Were key potential confounding variables measured and adjusted statistically in the analyses? If matching was used, did the investigators account for matching during study analysis?Yes
RatingFair