Literature DB >> 33462749

Antibiotic Therapy of 3 Days May Be Sufficient After Biliary Drainage for Acute Cholangitis: A Systematic Review.

Sylke Haal^1,2, Mattheus C B Wielenga³, Paul Fockens³, Charlotte A Leseman³, Cyriel Y Ponsioen³, Ellert J van Soest⁴, Roy L J van Wanrooij⁵, Elske Sieswerda⁶, Rogier P Voermans³.

Abstract

BACKGROUND: The optimal antibiotic therapy duration for cholangitis is unclear. Guideline recommendations vary between 4 and 14 days after biliary drainage. Clinical observations and some evidence however suggest that shorter antibiotic therapy may be sufficient.
OBJECTIVE: To compare the effectiveness and safety of short-course therapy of ≤ 3 days with long-course therapy of ≥ 4 days after biliary drainage in cholangitis patients.
METHODS: We searched the databases PubMed, EMBASE, Cochrane Library, and trial registers for literature up to August 5, 2020. RCTs and observational studies including case series reporting on antibiotic therapy duration for acute cholangitis were eligible for inclusion. Two reviewers independently evaluated study eligibility, extracted data, assessed risk of bias and quality of evidence. A meta-analysis was planned if the included studies were comparable with regard to important study characteristics. Primary outcomes included recurrent cholangitis, subsequent other infection, and mortality.
RESULTS: We included eight studies with 938 cholangitis patients. Four observational studies enrolled patients treated for ≤ 3 days. Recurrent cholangitis occurred in 0-26.8% of patients treated with short-course therapy, which did not differ from long-course therapy (range 0-21.1%). Subsequent other infection and mortality rates were also comparable. Quality of available evidence was very low.
CONCLUSION: There is no high-quality evidence available to draw a strong conclusion, but heterogeneous observational studies suggest that antibiotic therapy of ≤ 3 days is sufficient in cholangitis patients with common bile duct stones.

Entities: Chemical

Keywords: Acute cholangitis; Antibiotic therapy duration; Antimicrobial stewardship; Biliary drainage; Systematic review

Mesh：

Substances：
Anti-Bacterial Agents

Year: 2021 PMID： 33462749 PMCID： PMC8589797 DOI： 10.1007/s10620-020-06820-3

Source DB: PubMed Journal: Dig Dis Sci ISSN： 0163-2116 Impact factor: 3.199

Introduction

Acute cholangitis is a life-threatening infection which is managed with adequate source control (biliary drainage) and antibiotic therapy (ABT) [1, 2]. The optimal ABT duration for cholangitis is unclear. The Tokyo Guidelines (TG) 2018 recommend 4 to 7 days of ABT for cholangitis after biliary drainage [3]. If a bacteremia with gram-positive cocci is present, this guideline recommends a minimum duration of 14 days. The Dutch national sepsis guideline recommends a maximum of 3 days of ABT for cholangitis after biliary drainage [4]. Similarly, the optimal ABT duration for complicated intra-abdominal infections has been debated. A RCT and two post-hoc analyses showed that 4 days of ABT resulted in similar outcomes when compared with longer duration in patients with complicated intra-abdominal infections (of which 10.8% suffered from biliary tree infection) [5-7]. As a result, the revised Surgical Infection Society guidelines recommend to limit ABT to 4 days after source control [8], and the World Society of Emergency Surgery guidelines suggest a short course of 3–5 days for complicated intra-abdominal infections [9]. In contrast, the Surviving Sepsis Campaign guidelines are more conservative and recommend ABT for 7–10 days for most serious infections and sepsis [10]. Clinicians hesitate to shorten ABT because consensus and harmonized guidelines are lacking for cholangitis, which leads to a wide variety of ABT duration based on personal preference instead of evidence [11]. Additionally, we assume they fear recurrent infections or insufficient treatment of cholangitis complicated by bacteremia. But recurrent infections are often due to inadequate biliary drainage and may not be preventable with longer ABT [5]. While prolonged ABT does increase the risk of side-effects, mortality and antimicrobial resistance, and causes an extra financial burden on the healthcare system [12-16]. So far, one systematic review on this topic has been published by Tinusz et al.[17] In their review, four studies were included with a total of 205 cholangitis patients, and short-course ABT was defined as a shorter ABT duration than suggested by the available guidelines, which resulted in a diversified short-course therapy (SCT) group ranging from 3 to 14 days. In our opinion, it was necessary to reexamine the effectiveness and safety of a real short-course ABT (SCT of ≤ 3 days) versus long-course therapy (LCT) of ≥ 4 days after biliary drainage in cholangitis patients, and considering that new studies have emerged.

Methods

We registered the protocol of this systematic review on PROSPERO (CRD42020175393). We reported according to the Preferred Reporting Items for Systematic Reviews and Meta-analysis (PRISMA) Statement [18].

Eligibility Criteria

We considered RCTs and observational studies including case series eligible for inclusion. Case reports (less than five cases), conference abstracts, and reviews were excluded. Studies written in English were eligible if they reported on patients with acute cholangitis who received biliary drainage, in which duration of ABT was reported, and with a follow-up of at least 30 days. Primary outcomes—as defined by the authors of individual studies—were recurrent cholangitis, subsequent other intra-abdominal or extra-abdominal infection, and mortality. Secondary outcomes included ABT duration, total length of hospital stay, adequacy of empirical therapy (empirical ABT covered the causative organisms found in a blood culture), subsequent infection with highly resistant micro-organisms (HRMO), and Clostridioides difficile infection.

Information Sources and Search Strategy

A clinical librarian searched the electronic databases PubMed, EMBASE, and Cochrane Library up to 5 August 2020, using a combination of text words and controlled vocabulary. Two reviewers (S.H. and M.W.) checked the trial registers ClinicalTrials.gov, ISRCTN registry, EU Clinical Trials Register and WHO ICTRP for ongoing/unpublished trials and scanned reference lists of included studies. The search strategies are shown in Appendix 1 in Supplementary Materials.

Study Selection, Data Extraction and Quality Assessment

Two reviewers (S.H. and M.W.) independently evaluated study eligibility, extracted data, assessed risk of bias and quality of evidence. Disagreements were solved by consensus. Authors of ongoing trials were contacted and asked for the availability of data. We extracted the following data: publication details, study design, eligibility criteria, patient characteristics, sample size, details of the intervention, outcome measures and follow-up duration. We used the Cochrane risk of bias tool version 2, the ROBINS-I tool and the Newcastle–Ottawa scale (NOS) for assessment of risk of bias (at outcome level) in randomized studies, observational intervention studies, and the observational single-arm study, respectively.[19-21] A score of 8–9 stars in the NOS was considered as low risk of bias, 6–7 stars as moderate, and 0–5 stars as high. We rated the quality of evidence using the Grading of Recommendations Assessment, Development and Evaluation (GRADE) approach.

Statistical Analysis

We aimed to compare SCT with LCT, with SCT defined as ≤ 3 days and LCT as ≥ 4 days. In case these data could not be extracted, we planned to compare SCT and LCT as defined by the authors of individual studies. We planned to summarize the data descriptively. We also planned to provide summary measures (risk ratios for dichotomous outcomes and mean differences for continuous outcomes) and to perform a meta-analysis if the included studies were comparable with regard to important study characteristics.

Results

Study Selection

The electronic database search yielded 2439 records, and 8 records were identified from trial registers. After removal of duplicates, 1766 records were screened for relevance. Three eligible ongoing studies were identified of which the data was not yet available [22-24]. We retrieved 41 full-text articles, of which eight met all inclusion criteria (Fig. 1) [11, 25–31].

Fig. 1

PRISMA flowchart showing study selection

Study Characteristics

The study characteristics of the included studies are shown in Table 1. Two RCTs were included, one prospective single-arm study, and five retrospective studies with a total of 938 patients. In five out of eight studies, acute cholangitis was defined according to the diagnostic criteria of the TG. More than 80% of patients suffered from cholangitis due to common bile duct stones (CBDS). Patients with different etiologies were enrolled in 5 out of 8 studies [25, 26, 28–30]. Haal et al. and Satake et al. compared SCT (≤ 3 days) with LCT (≥ 4 days) [11, 31]. In the single-arm study of Kogure et al. ABT was stopped after temperature was < 37 °C for 24 h.[26] Van Lent et al. compared SCT (≤ 3 days) with medium-course therapy (MCT; 4/5 days) and LCT (> 5 days) [30]. The short ABT-regimens in the remaining studies were longer than 3 days and were considered LCT in this review. The short ABT group of Doi et al. was treated for ≤ 7 days [25], and of Netinatsunton et al. until temperature was below 38 °C for 72 h.[27] Park et al. assigned patients to early oral antibiotic switch or to conventional intravenous (IV) regime, but all patients received ABT for 14 days [28]. Uno et al. compared patients treated before May 2013 (ABT: 14 days) and after May 2013 (ABT < 14 days) [29]. All patients received empirical ABT intravenously. Some patients switched to oral ABT after initial recovery. Types of ABT prescribed were penicillins, a combination of a penicillin with a aminoglycoside or fluoroquinolone, cephalosporins, a combination of a cephalosporin with a aminoglycoside or metronidazole, a fluoroquinolone or a carbapenem. The ERCP was performed as soon as possible in the study of Kogure et al.[26] In the other studies, the time between admission and the ERCP ranged from within 24 h, [11, 25, 27–29] to a maximum of 4.5 days [30, 31]. The timing of the drainage differed significantly between the study groups in the studies of Haal et al., Satake et al., and Doi et al. [11, 25, 31]. Follow-up duration ranged between 4 weeks and 6 months.

Table 1

Characteristics of the included studies

First author	Year	Country	Study design	Study population	Intervention		Outcomes
Studies with SCT of ≤ 3 days
Haal [11]	2020	Netherlands	Retrospective multicenter study FU: 3 months	N = 296 Inclusion: acute cholangitis^a due to CBD stones with successful biliary drainage by ERCP; age > 18 years Exclusion: any other etiology of cholangitis; concomitant cholecystitis; death within 3 days after ERCP	SCT: ABT for ≤ 3 days N = 137 LCT: ABT for ≥ 4 days N = 159		Primary: occurrence of a local infectious complication Secondary: occurrence of C. difficile infection, total length of hospital stay, all-cause mortality
Kogure [26]	2011	Japan	Prospective single-center, single-arm study FU: 4 weeks	N = 18 Inclusion: moderate or severe acute cholangitis^b Exclusion: age < 20 years; most severe cholangitis requiring catecholamine administration, mechanical ventilation, or hemodialysis; acute pancreatitis; active concomitant infections; inadequate drainage; antibiotic use in the 4 weeks preceding the observation period	SCT: ABT was stopped after temp was < 37 °C for 24 h N = 18		Primary: recurrence of acute cholangitis within 3 days after withdrawal of antibiotics Secondary: period between initiation of therapy and normalization of WBC count and CRP, complications related to cholangitis, rate of re-administration of antibiotics within 4 weeks
Satake [31]	2020	Japan	Retrospective single-center study FU: 3 months	N = 96 Inclusion: acute cholangitis^a due to CBD stones with successful biliary drainage by ERCP Exclusion: severe cholangitis, inadequate drainage, stent occlusion, sclerosing cholangitis, concomitant infections	SCT: ABT for ≤ 3 days N = 22 LCT: ABT for ≥ 4 days N = 74		Primary: 30-day mortality, 3-month recurrence rate Secondary: length of hospital stay, acute bacteremic cholangitis rates
Van Lent [30]	2002	Netherlands	Retrospective single-center study FU: 6 months	N = 80 Inclusion: acute cholangitis^c with successful biliary drainage by ERCP Exclusion: primary sclerosing cholangitis; inflammatory bowel disease; bile duct atresia; liver transplantation; maintenance antibiotic therapy	SCT: ABT for ≤ 3 days N = 41 MCT: ABT for 4/5 days N = 19 LCT: ABT for > 5 days N = 20		Infectious complications and other episodes requiring antibiotic treatment, recurrent cholangitis, surgical procedures, death
Studies without SCT of ≤ 3 days
Doi [25]	2018	Japan	Retrospective single-center study FU: 3 months	N = 263 Inclusion: acute bacteremic cholangitis^d with successful biliary drainage by procedures such as ERCP Exclusion: age < 16 years	1: ABT for ≤ 7 days N = 86 2: ABT for ≥ 8 days N = 177	Primary: 30-day mortality Secondary: recurrence, recrudescence; new bacteremia or liver abscess, other complications that occurred as a consequence of cholangitis within 3 months
Netinatsunton [27]	2019	Thailand	Single-center, randomized controlled trial FU: 8 weeks	N = 34 Inclusion: acute cholangitis^c due to CBD stones with successful biliary drainage by ERCP Exclusion: severe cholangitis based on Reynold’s Pentad; other causes of cholangitis; concomitant cholecystitis; severe co-morbidity; active concomitant infection	1: ABT was stopped after temp was < 38 °C for 72 h N = 18 2: ABT for 14 days N = 16	Primary: recurrence of cholangitis after discontinuation of antibiotics Secondary: clinical and laboratory parameters, outcome of patients with and without bacteremia, hospital stay, complications
Park [28]	2014	Korea	Multicenter, randomized controlled trial FU: 30 days	N = 59 Inclusion: acute cholangitis^b and bacteremia with successful biliary decompression; age > 20 and < 85 years Exclusion: immunocompromised; severe infection requiring ventilation or inotropes/vasopressors administration; biliary drainage in the previous 2 weeks; other severe infection; complications associated with bacteremia at diagnosis; need for surgery; withdrawal	1: Early oral switch: IV for 6 days + oral for 8 days N = 29 2: Conventional IV: IV for > 10 days + oral for 4 days N = 30	Primary: eradication of bacteria in the bloodstream 30 days after diagnosis of bacteremia Secondary: recurrence of acute cholangitis, 30-day mortality
Uno [29]	2017	Japan	Retrospective single-center study FU: 3 months	N = 92 Inclusion: acute cholangitis^c and positive blood culture Exclusion: malignant biliary obstruction; bacteremia caused by gram-positive cocci; complication of cholecystitis or hepatic abscess; non-receipt of drainage	1: ABT for < 14 days After May 2013 (updated TG) N = 52 2: ABT for 14 days Before May 2013 N = 40	Primary: 30-day mortality, recurrence rate within 3 months of onset Secondary: treatment duration, length of hospital stay

ABT antibiotic therapy, CBD common bile duct, CRP C-reactive protein, FU follow-up, IV intravenous, LCT long-course therapy, MCT medium-course therapy, SCT short-course therapy, TG Tokyo guidelines, WBC white blood cell

aDiagnostic criteria of TG18

bDiagnostic criteria of TG07

cAcute cholangitis was defined as an illness characterized by fever (> 38 °C) and bile duct obstruction, as evidenced by increased bilirubin levels or dilated bile ducts by ultrasound

dAcute bacteraemic cholangitis was defined by clinical diagnosis of treating physicians with positive blood cultures

eDiagnostic criteria of TG13

Characteristics of the included studies Retrospective multicenter study FU: 3 months N = 296 Inclusion: acute cholangitisa due to CBD stones with successful biliary drainage by ERCP; age > 18 years Exclusion: any other etiology of cholangitis; concomitant cholecystitis; death within 3 days after ERCP SCT: ABT for ≤ 3 days N = 137 LCT: ABT for ≥ 4 days N = 159 Primary: occurrence of a local infectious complication Secondary: occurrence of C. difficile infection, total length of hospital stay, all-cause mortality Prospective single-center, single-arm study FU: 4 weeks N = 18 Inclusion: moderate or severe acute cholangitisb Exclusion: age < 20 years; most severe cholangitis requiring catecholamine administration, mechanical ventilation, or hemodialysis; acute pancreatitis; active concomitant infections; inadequate drainage; antibiotic use in the 4 weeks preceding the observation period SCT: ABT was stopped after temp was < 37 °C for 24 h N = 18 Primary: recurrence of acute cholangitis within 3 days after withdrawal of antibiotics Secondary: period between initiation of therapy and normalization of WBC count and CRP, complications related to cholangitis, rate of re-administration of antibiotics within 4 weeks Retrospective single-center study FU: 3 months N = 96 Inclusion: acute cholangitisa due to CBD stones with successful biliary drainage by ERCP Exclusion: severe cholangitis, inadequate drainage, stent occlusion, sclerosing cholangitis, concomitant infections SCT: ABT for ≤ 3 days N = 22 LCT: ABT for ≥ 4 days N = 74 Primary: 30-day mortality, 3-month recurrence rate Secondary: length of hospital stay, acute bacteremic cholangitis rates Retrospective single-center study FU: 6 months N = 80 Inclusion: acute cholangitisc with successful biliary drainage by ERCP Exclusion: primary sclerosing cholangitis; inflammatory bowel disease; bile duct atresia; liver transplantation; maintenance antibiotic therapy SCT: ABT for ≤ 3 days N = 41 MCT: ABT for 4/5 days N = 19 LCT: ABT for > 5 days N = 20 Retrospective single-center study FU: 3 months N = 263 Inclusion: acute bacteremic cholangitisd with successful biliary drainage by procedures such as ERCP Exclusion: age < 16 years 1: ABT for ≤ 7 days N = 86 2: ABT for ≥ 8 days N = 177 Primary: 30-day mortality Secondary: recurrence, recrudescence; new bacteremia or liver abscess, other complications that occurred as a consequence of cholangitis within 3 months Single-center, randomized controlled trial FU: 8 weeks N = 34 Inclusion: acute cholangitisc due to CBD stones with successful biliary drainage by ERCP Exclusion: severe cholangitis based on Reynold’s Pentad; other causes of cholangitis; concomitant cholecystitis; severe co-morbidity; active concomitant infection 1: ABT was stopped after temp was < 38 °C for 72 h N = 18 2: ABT for 14 days N = 16 Primary: recurrence of cholangitis after discontinuation of antibiotics Secondary: clinical and laboratory parameters, outcome of patients with and without bacteremia, hospital stay, complications Multicenter, randomized controlled trial FU: 30 days N = 59 Inclusion: acute cholangitisb and bacteremia with successful biliary decompression; age > 20 and < 85 years Exclusion: immunocompromised; severe infection requiring ventilation or inotropes/vasopressors administration; biliary drainage in the previous 2 weeks; other severe infection; complications associated with bacteremia at diagnosis; need for surgery; withdrawal 1: Early oral switch: IV for 6 days + oral for 8 days N = 29 2: Conventional IV: IV for > 10 days + oral for 4 days N = 30 Primary: eradication of bacteria in the bloodstream 30 days after diagnosis of bacteremia Secondary: recurrence of acute cholangitis, 30-day mortality Retrospective single-center study FU: 3 months N = 92 Inclusion: acute cholangitisc and positive blood culture Exclusion: malignant biliary obstruction; bacteremia caused by gram-positive cocci; complication of cholecystitis or hepatic abscess; non-receipt of drainage 1: ABT for < 14 days After May 2013 (updated TG) N = 52 2: ABT for 14 days Before May 2013 N = 40 Primary: 30-day mortality, recurrence rate within 3 months of onset Secondary: treatment duration, length of hospital stay ABT antibiotic therapy, CBD common bile duct, CRP C-reactive protein, FU follow-up, IV intravenous, LCT long-course therapy, MCT medium-course therapy, SCT short-course therapy, TG Tokyo guidelines, WBC white blood cell aDiagnostic criteria of TG18 bDiagnostic criteria of TG07 cAcute cholangitis was defined as an illness characterized by fever (> 38 °C) and bile duct obstruction, as evidenced by increased bilirubin levels or dilated bile ducts by ultrasound dAcute bacteraemic cholangitis was defined by clinical diagnosis of treating physicians with positive blood cultures eDiagnostic criteria of TG13

Risk of Bias in Included Studies

Table 2a–c shows the results of the risk of bias assessments. All studies had methodological limitations. The two RCTs were at low risk of bias in three out of five domains, while two out of five domains raised some concerns [27, 28]. We considered the observational intervention study of Doi et al. to be at moderate risk of bias [25], and the four other observational intervention studies to be at serious risk of bias, especially due to a high risk of confounding [11, 29–31]. We judged the prospective single-arm study of Kogure et al. to be at moderate risk of bias [26].

Table 2

Risk of bias in (a) the randomized controlled trials—RoB-2 tool, (b) the observational studies (non-randomized studies of interventions)—ROBINS-I tool, (c) single-arm observational study—Newcastle–Ottawa assessment scale

Study	Randomization process	Deviations from intended interventions	Missing outcome data	Measurement of the outcome	Selection of the reported result	Overall bias
(a)
Netinatsunton [27]	Low risk of bias	Some concerns	Low risk of bias	Some concerns	Low risk of bias	Some concerns
Park [28]	Low risk of bias	Some concerns	Low risk of bias	Low risk of bias	Some concerns	Some concerns

Quality of Evidence

The quality of evidence was very low for all outcomes. Main reasons for down rating the evidence were design limitations of the included studies, indirectness (different study populations, and only a minority of patients treated for ≤ 3 days), and imprecision (only small studies, and few events).

Results of Individual Studies

Tables 3 and 4 show the individual study results regarding primary and secondary outcomes.

Table 3

Primary outcomes

Study	Intervention	Sample size	Recurrent cholangitis (n/N, %)	Subsequent other infection (n/N, %)	Mortality (n/N, %)
Studies with SCT of ≤ 3 days
Haal [11]	SCT: ABT for ≤ 3 days LCT: ABT for ≥ 4 days	N = 137 N = 159	10/137 (7.3%) 18/159 (11.3%)	6/137 (4.3%)^a 7/159 (4.4%)^a	0 4/159 (2.5%)
Kogure [26]	SCT: ABT stopped after T < 37 °C 24 h	N = 18	0	0^b	0
Satake [31]	SCT: ABT for ≤ 3 days LCT: ABT for ≥ 4 days	N = 22 N = 74	2/22 (9.1%) 1/74 (1.4%)	NR	0 2/74 (2.7%)
Van Lent [30]	SCT: ABT for ≤ 3 days MCT: ABT for 4/5 days LCT: ABT for > 5 days	N = 41 N = 19 N = 20	11/41 (26.8%) 4/19 (21.1%) 4/20 (20%)	NR	6/41 (14.6%) 2/19 (10.5%) 1/20 (5%)
Studies without SCT of ≤ 3 days
Doi [25]	1: ABT for ≤ 7 days 2: ABT for ≥ 8 days	N = 86 N = 177	5/77 (6.5%) 6/153 (7.9%)	4/72 (5.6%)^c 12/132 (9.1%)^c	4/85 (4.7%) 10/176 (5.7%)
Netinatsunton [27]	1: ABT stopped after T < 38 °C 72 h 2: ABT for 14 days	N = 18 N = 16	0 1/16 (6.3%)	NR	0 0
Park [28]	1: ABT for 14 days (early oral switch) 2: ABT for 14 days (conventional IV)	N = 29 N = 30	1/29 (3.4%) 0	NR	0 0
Uno [29]	1: ABT for < 14 days (after May 2013) 2: ABT for 14 days (before May 2013)	N = 52 N = 40	0/37 (0%) 4/30 (13.3%)	NR	0/47 (0%) 2/35 (5.7%)

Study

Intervention

Sample size

Recurrent cholangitis (n/N, %)

Subsequent other infection (n/N, %)

Mortality (n/N, %)

Studies with SCT of ≤ 3 days

Haal [11]

SCT: ABT for ≤ 3 days

LCT: ABT for ≥ 4 days

N = 137

N = 159

10/137 (7.3%)

18/159 (11.3%)

6/137 (4.3%)^a

7/159 (4.4%)^a

4/159 (2.5%)

Kogure [26]

SCT: ABT stopped after T < 37 °C 24 h

N = 18

0^b

Satake [31]

SCT: ABT for ≤ 3 days

LCT: ABT for ≥ 4 days

N = 22

N = 74

2/22 (9.1%)

1/74 (1.4%)

2/74 (2.7%)

Van Lent [30]

SCT: ABT for ≤ 3 days

MCT: ABT for 4/5 days

LCT: ABT for > 5 days

N = 41

N = 19

N = 20

11/41 (26.8%)

4/19 (21.1%)

4/20 (20%)

6/41 (14.6%)

2/19 (10.5%)

1/20 (5%)

Studies without SCT of ≤ 3 days

Doi [25]

1: ABT for ≤ 7 days

2: ABT for ≥ 8 days

N = 86

N = 177

5/77 (6.5%)

6/153 (7.9%)

4/72 (5.6%)^c

12/132 (9.1%)^c

4/85 (4.7%)

10/176 (5.7%)

Netinatsunton [27]

1: ABT stopped after T < 38 °C 72 h

2: ABT for 14 days

N = 18

N = 16

1/16 (6.3%)

Park [28]

1: ABT for 14 days (early oral switch)

2: ABT for 14 days (conventional IV)

N = 29

N = 30

1/29 (3.4%)

Uno [29]

1: ABT for < 14 days (after May 2013)

2: ABT for 14 days (before May 2013)

N = 52

N = 40

0/37 (0%)

4/30 (13.3%)

0/47 (0%)

2/35 (5.7%)

ABT antibiotic therapy, IV intravenous, LCT long-course therapy, MCT medium-course therapy, NR not reported, SCT short-course therapy, T temperature

aLocal infectious complication

bCholangitis-related complications or re-administration of antibiotics

cBacteremia, liver abscess or other complications that occurred as a consequence of cholangitis

Table 4

Secondary outcomes

Study	Intervention	Sample size	ABT duration (in days)	Length of hospital stay (in days)	Adequacy of empirical therapy	Infection with resistant pathogen	C. difficile infection
Studies with SCT of ≤ 3 days
Haal [11]	SCT: ABT for ≤ 3 days	N = 137	Median: 2 (1–3)^1a Median: 4 (3–6)^2a	Median: 6 (4–8)^a	NR	0	0
Haal [11]	LCT: ABT for ≥ 4 days	N = 159	Median: 6 (4–7)^1a Median: 7 (6–10)^2a	Median: 7 (5–9)^a	NR	0	0
Kogure [26]	SCT: ABT stopped after T < 37 °C 24 h	N = 18	Median: 3 (2–7)^2b	NR	NR	NR	NR
Satake [31]	SCT: ABT for ≤ 3 days	N = 22	Median: 1.5 (1–3)^1b Mean: 6.3 (2.4)^2c	Mean: 19.5 (21.6)^c	NR	NR	NR
Satake [31]	LCT: ABT for ≥ 4 days	N = 74	Median: 7 (4–17)^1b Mean: 11.1 (3.8)^2c	Mean: 21.3 (21.1)^c	NR	NR	NR
Van Lent [30]	SCT: ABT for ≤ 3 days MCT: ABT for 4/5 days LCT: ABT for > 5 days	N = 41 N = 19 N = 20	NR	NR	NR	NR	NR
Studies without SCT of ≤ 3 days
Doi [25]	1: ABT for ≤ 7 days 2: ABT for ≥ 8 days	N = 86 N = 177	Median: 6 (2–7)^2b Median: 12 (8–46)^2b	NR	75/78 (96%) 136/157 (87%)	NR	NR
Netinatsunton [27]	1: ABT stopped after T < 38 °C 72 h 2: ABT for 14 days	N = 18 N = 16	Mean: 4.6 (3–9)^2b Fixed: 14²	Mean: 5.8 (2.4)^c Mean: 6.4 (2.3)^c	NR	NR	NR
Park [28]	1: ABT for 14 days (early oral switch) 2: ABT for 14 days (conventional IV)	N = 29 N = 30	Fixed: 14² Fixed: 14²	Mean: 10.8 (3.8)^c Mean: 12.3 (5.7)^c	NR	NR	NR
Uno [29]	1: ABT for < 14 days (after May 2013) 2: ABT for 14 days (before May 2013)	N = 52 N = 40	Median: 10 (7.3–12.8)^2a Median: 14.5 (14–15)^2a	Median: 14 (10–17)^a Median: 17.5 (16–22.5)^a	47/52 (90%) 30/40 (75%)	NR	NR

ABT antibiotic therapy, C Clostridioides, IV intravenous, LCT long-course therapy, MCT medium-course therapy, NR not reported, SCT short-course therapy, T temperature

1ABT duration after ERCP

2Total ABT duration

aInterquartile range

bRange

cStandard deviation

Primary outcomes SCT: ABT for ≤ 3 days LCT: ABT for ≥ 4 days N = 137 N = 159 10/137 (7.3%) 18/159 (11.3%) 6/137 (4.3%)a 7/159 (4.4%)a 0 4/159 (2.5%) SCT: ABT for ≤ 3 days LCT: ABT for ≥ 4 days N = 22 N = 74 2/22 (9.1%) 1/74 (1.4%) 0 2/74 (2.7%) SCT: ABT for ≤ 3 days MCT: ABT for 4/5 days LCT: ABT for > 5 days N = 41 N = 19 N = 20 11/41 (26.8%) 4/19 (21.1%) 4/20 (20%) 6/41 (14.6%) 2/19 (10.5%) 1/20 (5%) 1: ABT for ≤ 7 days 2: ABT for ≥ 8 days N = 86 N = 177 5/77 (6.5%) 6/153 (7.9%) 4/72 (5.6%)c 12/132 (9.1%)c 4/85 (4.7%) 10/176 (5.7%) 1: ABT stopped after T < 38 °C 72 h 2: ABT for 14 days N = 18 N = 16 0 1/16 (6.3%) 0 0 1: ABT for 14 days (early oral switch) 2: ABT for 14 days (conventional IV) N = 29 N = 30 1/29 (3.4%) 0 0 0 1: ABT for < 14 days (after May 2013) 2: ABT for 14 days (before May 2013) N = 52 N = 40 0/37 (0%) 4/30 (13.3%) 0/47 (0%) 2/35 (5.7%) ABT antibiotic therapy, IV intravenous, LCT long-course therapy, MCT medium-course therapy, NR not reported, SCT short-course therapy, T temperature aLocal infectious complication bCholangitis-related complications or re-administration of antibiotics cBacteremia, liver abscess or other complications that occurred as a consequence of cholangitis Secondary outcomes Median: 2 (1–3)1a Median: 4 (3–6)2a Median: 6 (4–7)1a Median: 7 (6–10)2a Median: 1.5 (1–3)1b Mean: 6.3 (2.4)2c Median: 7 (4–17)1b Mean: 11.1 (3.8)2c SCT: ABT for ≤ 3 days MCT: ABT for 4/5 days LCT: ABT for > 5 days N = 41 N = 19 N = 20 1: ABT for ≤ 7 days 2: ABT for ≥ 8 days N = 86 N = 177 Median: 6 (2–7)2b Median: 12 (8–46)2b 75/78 (96%) 136/157 (87%) 1: ABT stopped after T < 38 °C 72 h 2: ABT for 14 days N = 18 N = 16 Mean: 4.6 (3–9)2b Fixed: 142 Mean: 5.8 (2.4)c Mean: 6.4 (2.3)c 1: ABT for 14 days (early oral switch) 2: ABT for 14 days (conventional IV) N = 29 N = 30 Fixed: 142 Fixed: 142 Mean: 10.8 (3.8)c Mean: 12.3 (5.7)c 1: ABT for < 14 days (after May 2013) 2: ABT for 14 days (before May 2013) N = 52 N = 40 Median: 10 (7.3–12.8)2a Median: 14.5 (14–15)2a Median: 14 (10–17)a Median: 17.5 (16–22.5)a 47/52 (90%) 30/40 (75%) ABT antibiotic therapy, C Clostridioides, IV intravenous, LCT long-course therapy, MCT medium-course therapy, NR not reported, SCT short-course therapy, T temperature 1ABT duration after ERCP 2Total ABT duration aInterquartile range bRange cStandard deviation

Recurrent Cholangitis

All studies assessed recurrent cholangitis. Haal et al. reported recurrence rates of 7.3% and 11.3% in the SCT (≤ 3 days) and LCT groups (≥ 4 days), respectively (p = 0.238) [11]. In the study of Kogure et al., none of the 18 patients developed recurrent cholangitis (median ABT: 3 days) [26]. Satake et al. reported rates of 9.1% and 1.4% in the SCT (≤ 3 days) and LCT groups (≥ 4 days), respectively (p = 0.13) [31]. Van Lent et al. reported rates of 26.8%, 21.1% and 20% in the SCT (≤ 3 days), MCT (4/5 days) and LCT groups (> 5 days), respectively (p = 0.80) [30]. Doi et al. reported rates of 6.5% and 7.9% in patients treated for ≤ 7 days and ≥ 8 days (p = 0.69) [25]. In the study of Netinatsunton et al., recurrent cholangitis did not occur in the fever-based group (mean ABT: 4.6 days), compared to one recurrence (6.3%) in the 14-day group (p = 0.485) [27]. Park et al. reported rates of 3.4% in the early oral switch group, and 0% in the conventional IV group (p = 0.50) [28]. Uno et al. reported four recurrences (13.3%) in the group treated for 14 days (median ABT: 14.5 days), and zero in the group treated for < 14 days (median ABT: 10 days; p = 0.036) [29].

Subsequent Other Intra-abdominal or Extra-abdominal Infection

Three studies assessed this outcome [11, 25, 26]. Haal et al. reported six patients (4.3%) with a local infectious complication in the SCT group, compared with seven patients (4.4%) in the LCT group (p = 0.992) [11]. In the study of Kogure et al. none of the patients developed complications related to cholangitis or needed re-administration of ABT [26]. In the study of Doi et al., four patients (5.6%) treated for ≤ 7 days developed bacteremia, liver abscess or other complications related to cholangitis, compared with 12 patients (9.1%) treated for ≥ 8 days (p = 0.43) [25].

Mortality

Six studies assessed mortality [11, 25, 28–31]. The studies of Kogure et al. and Netinatsunton et al. did not report mortality as outcome but we assessed rates of 0%, because all patients visited the outpatient clinic or were contacted by telephone [26, 27]. Haal et al. reported mortality rates of 0% and 2.5% in the SCT and LCT groups, respectively (p = 0.13) [11]. Satake et al. reported rates of 0% and 2.7% in the SCT and LCT groups (p = 1) [31]. Van Lent et al. reported rates of 14.6%, 10.5% and 5% in the SCT, MCT and LCT groups (no p value reported) [30]. In the study of Doi et al., mortality rates were 4.7% and 5.7% in patients treated for ≤ 7 days and ≥ 8 days (p = 0.74) [25]. No deaths were observed in the study of Park et al.[28]. Uno et al. reported two deaths (5.7%), and both patients were treated before May 2013 (p = 0.179) [29].

ABT Duration

Five studies reported total ABT duration which are show in Table 4 [24-29]. In these studies, most patients received biliary drainage within 24 h after admission. Haal et al. and Satake et al. reported both total and ABT duration after biliary drainage [11, 31], while van Lent et al. only after biliary drainage (timing unknown) [30].

Total Length of Hospital Stay

Five studies assessed hospital stay [11, 27–29, 31]. Haal et al. reported a median hospital stay of 6 days for SCT, and 7 days for LCT (p = 0.03) [11]. Satake et al. reported a mean hospital stay of 19.5 days in the SCT, and 21.3 days in the LCT group (p = 0.73) [31]. In the study of Netinatsunton et al., mean hospital stay did not significantly differ (5.8 days vs 6.4 days; p = 0.467) [27]. Park et al. reported a mean hospital stay of 10.8 days in the early oral switch group and 12.3 days in the conventional IV group (p = 0.02) [28]. Uno et al. reported a median hospital stay of 14 days and 17.5 days in the groups treated after and before May 2013 (p < 0.001) [29].

Adequacy of Empirical Therapy

Two studies assessed adequacy of empirical therapy [25, 29]. Doi et al. reported rates of adequate empirical ABT of 96% and 87% in the groups treated for ≤ 7 days and ≥ 8 days (p = 0.02) [25]. Uno et al. reported rates of 90% and 75% in the groups treated after and before May 2013 (no p-value reported) [29].

Subsequent Infection with HRMO and C. difficile Infection

None of the enrolled patients developed these outcomes, only assessed by Haal et al.[11]

Synthesis of Results: SCT ≤ 3 Days Versus LCT ≥ 4 Days

Four observational studies included a total of 211 patients treated for ≤ 3 days [11, 26, 30, 31]. Recurrent cholangitis occurred in 0 to 26.8% of patients treated with SCT of ≤ 3 days, which did not differ from LCT (range 0–21.1%). Subsequent other infection (range 0–4.3% vs 4.4%-9.1%) and mortality (range 0–14.6% vs 0–10.5%) were also comparable. Secondary outcomes were scarcely reported. Haal et al. reported a median hospital stay of 6 days in patients with SCT of ≤ 3 days [11], while Satake et al. reported a mean stay of 19.5 days [31]. A wide range was found in patients treated for ≥ 4 days (5.8–21.3 days) [11, 27–29, 31]. We did not perform a meta-analysis because the included studies were too heterogeneous. The study populations differed significantly in etiology and severity of cholangitis, and number of patients with bacteremia. Moreover, the definition of ABT duration varied from total versus after drainage.

Discussion

The optimal ABT duration for cholangitis after biliary drainage remains arguable, while appropriate ABT use improves patient outcomes and reduces antimicrobial resistance [12-16]. None of the included studies found significant differences in outcomes between SCT and LCT according to their own definition of SCT and LCT. No evidence was available from RCTs on the effectiveness and safety of SCT of ≤ 3 days in cholangitis patients after biliary drainage. Heterogeneous observational studies of low quality suggest that ABT of ≤ 3 days is sufficient in cholangitis patients with CBDS. ABT plays an important role in the initial treatment of acute cholangitis [2]. In the included studies, blood cultures appeared to be standard care while bile cultures were done infrequently. As advised by the TG18, blood and bile cultures should be routinely performed to guide and further optimise ABT [1]. Evidence in patients with complicated intra-abdominal infections support the opinion that ABT can be stopped quickly after source control is established [5-7]. Still, there is a need for well-designed studies which accurately evaluate the effectiveness and safety of SCT ≤ 3 days after biliary drainage in cholangitis patients. We are looking forward to the results of three ongoing studies [22, 24]. The FANTASTIC trial might end with a SCT group of ≤ 3 days—as they randomly assigned patients to a fever-based group: ABT is stopped when temperature is below 37 °C for 24 h or to a guideline-based group: ABT for 4–7 days [22]. The group of Doi et al. compares ABT of ≥ 5 days with ABT of ≥ 7 days in a RCT [24], while the third study (retrospective case–control) compares ABT of < 7 days with ABT > 7 days in patients with cholangitis admitted to the intensive care [22]. Strengths of this review are that we aimed to minimize bias by performing a thorough search, by working with two independent reviewers, and by our decision not to pool the data. On the other hand, our review has limitations. First, the majority of included studies was observational. Second, we were not able to draw a strong conclusion about the effectiveness and safety of SCT of ≤ 3 days, because only 211 patients were treated for ≤ 3 days. Third, the variance in reporting ABT duration (after and total) and different enrolled study populations withheld us providing summary measures and performing a meta-analysis. At the same time, we were not able to perform a subgroup analysis due to the limited number of patients with other etiologies than CBDS. Hence, the generalizability of our results is limited. Only van Lent et al. included a high number of patients (64%) with complex causes of cholangitis, which are more dependent on the technical success of drainage [30]. This might explains the high rates of recurrent cholangitis and mortality in all treatment groups. Besides the technical success of the ERCP, timing of biliary drainage has also impact on the outcome of acute cholangitis, regardless of ABT duration [32, 33]. In three included studies, the timing of biliary drainage differed significantly between the SCT and LCT groups [11, 26, 31]. However, in the study of Doi et al. both groups underwent biliary drainage within 24 h. While in the two other studies, biliary drainage was performed on a later time point in the SCT group. Hence, it unlikely that the effectiveness and safety of SCT were positively affected by the variance in timing of biliary drainage. In conclusion, currently, there is no high-quality evidence available to draw a strong conclusion about the optimal ABT duration for cholangitis after biliary drainage. Prospective studies are awaited to confirm the results of observational studies which suggest that ABT of ≤ 3 days is sufficient in cholangitis patients with CBDS. Below is the link to the electronic supplementary material. Supplementary material (DOCX 14 kb)

28 in total

1. Endoscopic management of common bile duct stones: European Society of Gastrointestinal Endoscopy (ESGE) guideline.

Authors: Gianpiero Manes; Gregorios Paspatis; Lars Aabakken; Andrea Anderloni; Marianna Arvanitakis; Philippe Ah-Soune; Marc Barthet; Dirk Domagk; Jean-Marc Dumonceau; Jean-Francois Gigot; Istvan Hritz; George Karamanolis; Andrea Laghi; Alberto Mariani; Konstantina Paraskeva; Jürgen Pohl; Thierry Ponchon; Fredrik Swahn; Rinze W F Ter Steege; Andrea Tringali; Antonios Vezakis; Earl J Williams; Jeanin E van Hooft
Journal: Endoscopy Date: 2019-04-03 Impact factor: 10.093

2. Trial of short-course antimicrobial therapy for intraabdominal infection.

Authors: Robert G Sawyer; Jeffrey A Claridge; Avery B Nathens; Ori D Rotstein; Therese M Duane; Heather L Evans; Charles H Cook; Patrick J O'Neill; John E Mazuski; Reza Askari; Mark A Wilson; Lena M Napolitano; Nicholas Namias; Preston R Miller; E Patchen Dellinger; Christopher M Watson; Raul Coimbra; Daniel L Dent; Stephen F Lowry; Christine S Cocanour; Michaela A West; Kaysie L Banton; William G Cheadle; Pamela A Lipsett; Christopher A Guidry; Kimberley Popovsky
Journal: N Engl J Med Date: 2015-05-21 Impact factor: 91.245

Review 3. Tokyo Guidelines 2018: initial management of acute biliary infection and flowchart for acute cholangitis.

Authors: Fumihiko Miura; Kohji Okamoto; Tadahiro Takada; Steven M Strasberg; Horacio J Asbun; Henry A Pitt; Harumi Gomi; Joseph S Solomkin; David Schlossberg; Ho-Seong Han; Myung-Hwan Kim; Tsann-Long Hwang; Miin-Fu Chen; Wayne Shih-Wei Huang; Seiki Kiriyama; Takao Itoi; O James Garden; Kui-Hin Liau; Akihiko Horiguchi; Keng-Hao Liu; Cheng-Hsi Su; Dirk J Gouma; Giulio Belli; Christos Dervenis; Palepu Jagannath; Angus C W Chan; Wan Yee Lau; Itaru Endo; Kenji Suzuki; Yoo-Seok Yoon; Eduardo de Santibañes; Mariano Eduardo Giménez; Eduard Jonas; Harjit Singh; Goro Honda; Koji Asai; Yasuhisa Mori; Keita Wada; Ryota Higuchi; Manabu Watanabe; Toshiki Rikiyama; Naohiro Sata; Nobuyasu Kano; Akiko Umezawa; Shuntaro Mukai; Hiromi Tokumura; Jiro Hata; Kazuto Kozaka; Yukio Iwashita; Taizo Hibi; Masamichi Yokoe; Taizo Kimura; Seigo Kitano; Masafumi Inomata; Koichi Hirata; Yoshinobu Sumiyama; Kazuo Inui; Masakazu Yamamoto
Journal: J Hepatobiliary Pancreat Sci Date: 2018-01-08 Impact factor: 7.027

4. Longer-Duration Antimicrobial Therapy Does Not Prevent Treatment Failure in High-Risk Patients with Complicated Intra-Abdominal Infections.

Authors: Taryn E Hassinger; Christopher A Guidry; Ori D Rotstein; Therese M Duane; Heather L Evans; Charles H Cook; Patrick J O'Neill; John E Mazuski; Reza Askari; Lena M Napolitano; Nicholas Namias; Preston R Miller; E Patchen Dellinger; Raul Coimbra; Christine S Cocanour; Kaysie L Banton; Joseph Cuschieri; Kimberley Popovsky; Robert G Sawyer
Journal: Surg Infect (Larchmt) Date: 2017-06-26 Impact factor: 2.150

5. Fever-based antibiotic therapy for acute cholangitis following successful endoscopic biliary drainage.

Authors: Hirofumi Kogure; Takeshi Tsujino; Keisuke Yamamoto; Suguru Mizuno; Yoko Yashima; Hiroshi Yagioka; Kazumichi Kawakubo; Takashi Sasaki; Yousuke Nakai; Kenji Hirano; Naoki Sasahira; Hiroyuki Isayama; Minoru Tada; Takao Kawabe; Masao Omata; Sohei Harada; Yasuo Ota; Kazuhiko Koike
Journal: J Gastroenterol Date: 2011-08-13 Impact factor: 7.527

6. Duration of antibiotic therapy for cholangitis after successful endoscopic drainage of the biliary tract.

Authors: Anja U G van Lent; Joep F W M Bartelsman; Guido N J Tytgat; Peter Speelman; Jan M Prins
Journal: Gastrointest Endosc Date: 2002-04 Impact factor: 9.427

7. Short-course antimicrobial treatment for acute cholangitis with Gram-negative bacillary bacteremia.

Authors: Shunsuke Uno; Ryota Hase; Masayoshi Kobayashi; Toshiyasu Shiratori; So Nakaji; Nobuto Hirata; Naoto Hosokawa
Journal: Int J Infect Dis Date: 2016-12-24 Impact factor: 3.623

8. Early oral antibiotic switch compared with conventional intravenous antibiotic therapy for acute cholangitis with bacteremia.

Authors: Tae Young Park; Jung Sik Choi; Tae Jun Song; Jae Hyuk Do; Seong-Ho Choi; Hyoung-Chul Oh
Journal: Dig Dis Sci Date: 2014-06-05 Impact factor: 3.199

9. ROBINS-I: a tool for assessing risk of bias in non-randomised studies of interventions.

Authors: Jonathan Ac Sterne; Miguel A Hernán; Barnaby C Reeves; Jelena Savović; Nancy D Berkman; Meera Viswanathan; David Henry; Douglas G Altman; Mohammed T Ansari; Isabelle Boutron; James R Carpenter; An-Wen Chan; Rachel Churchill; Jonathan J Deeks; Asbjørn Hróbjartsson; Jamie Kirkham; Peter Jüni; Yoon K Loke; Theresa D Pigott; Craig R Ramsay; Deborah Regidor; Hannah R Rothstein; Lakhbir Sandhu; Pasqualina L Santaguida; Holger J Schünemann; Beverly Shea; Ian Shrier; Peter Tugwell; Lucy Turner; Jeffrey C Valentine; Hugh Waddington; Elizabeth Waters; George A Wells; Penny F Whiting; Julian Pt Higgins
Journal: BMJ Date: 2016-10-12

10. Shortening antibiotic duration in the treatment of acute cholangitis: rationale and study protocol for an open-label randomized controlled trial.

Authors: Kentaro Iwata; Asako Doi; Yuichiro Oba; Hiroo Matsuo; Kei Ebisawa; Manabu Nagata; Sho Nishimura; Kenichi Yoshimura; Atsuhiro Masuda; Hideyuki Shiomi; Yuzo Kodama
Journal: Trials Date: 2020-01-17 Impact factor: 2.279