CC BY-NC-ND 4.0 · Journal of Digestive Endoscopy 2021; 12(03): 138-150
DOI: 10.1055/s-0041-1739567
Systematic Review

Endoscopy in Pregnancy: A Systematic Review

Partha Pal
1   Medical Gastroenterology, Asian Institute of Gastroenterology, Hyderabad, Telangana, India
,
D. Nageshwar Reddy
1   Medical Gastroenterology, Asian Institute of Gastroenterology, Hyderabad, Telangana, India
,
Manu Tandan
1   Medical Gastroenterology, Asian Institute of Gastroenterology, Hyderabad, Telangana, India
› Author Affiliations
Funding None.
 

Abstract

Background Fetomaternal outcomes are of primary concern for gastrointestinal (GI) endoscopy in pregnancy. We aimed to systematically review the safety and utility of endoscopic procedures in pregnancy.

Methods A systematic literature search was performed using PubMed. All original research articles with sample size > 10 involving endoscopy in pregnancy were included for the review along with case report/series describing novel/rare techniques from 1948 to July 2021.

Results After screening 12,197 references, 216 citations were found and finally 66 references were included. Esophagogastroduodenoscopy had favorable fetal outcome (>95%) based on two large retrospective studies and a review of case reports. Sclerotherapy and band ligation of varices were safe according to case series. A large nationwide cohort study established safety of endotherapy for nonvariceal bleed. Botulinum toxin and pneumatic dilation in achalasia are only supported by case reports. Percutaneous endoscopic gastrostomy can be useful to support nutrition based on case reports. A retrospective case–control and cohort study with systemic review justified flexible sigmoidoscopy if strongly indicated. Low birth weight was more common when sigmoidoscopy was done in inflammatory bowel disease based on a prospective study. Colonoscopy was considered safe in second trimester based on a case–control study whereas it can be performed otherwise only in presence of strong indication like malignancy. Capsule endoscopy is promising and can be useful in acute small bowel bleeding although risk of capsule retention is unknown. There are no reports of enteroscopy in pregnancy. Twelve retrospective studies and one prospective study showed high success rate of therapeutic endoscopic retrograde cholangiopancreatography (ERCP) (> 90%) in all trimesters and can be performed if strongly indicated. Pregnancy was an independent risk factor for post-ERCP pancreatitis in a large nationwide case–control study. Radiation-free ERCP with wire-guided bile observation, stent-guided or precut sphincterotomy, endoscopic ultrasound (EUS) guidance, and spyscopy have been described. Safety of EUS is limited to case series and can be used in intermediate probability of choledocholithiasis to guide ERCP and endoscopic cystogastrostomy.

Conclusion This review concludes that GI endoscopy during pregnancy can be done effectively if strongly indicated with good fetomaternal outcomes. Precautions are advocated during procedures where radiation exposure is expected.


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Introduction

Endoscopy plays a crucial role in managing gastrointestinal (GI) disorders in general population and is considered safe. However, this could not be extrapolated to pregnant women requiring GI endoscopy due to scarcity of robust clinical data and concern regarding fetomaternal complications. Risk factors unique to endoscopy in pregnancy include risk of teratogenicity/premature labor with anesthetic medications, placental abruption or fetal injury with deep intestinal intubation, radiation during endoscopic retrograde cholangiopancreatography (ERCP), and maternal intraprocedure complications like hypotension/hypertension, hypoxia, and arrhythmia.[1]

The literature regarding endoscopy in pregnancy is limited to various small isolated case reports/series, and few retrospective studies although recently few prospective studies and nationwide cohort studies with population control have been reported.[2] [3] [4] [5] Guidelines are limited and outdated.[5] It is difficult for the busy practicing gastroenterologist to find and judge clinical data for endoscopy in pregnancy in the absence of prospective, controlled studies which are scarce due to difficulty and reluctance in research due to concern for fetal safety and medico-legal implications.[1] Moreover, the implications of various endoscopic procedures (esophagogastroduodenoscopy [EGD], sigmoidoscopy, colonoscopy, ERCP, endoscopic ultrasound [EUS], etc.) may vary according to various trimesters of pregnancy. For this reason, our review attempts to address the clinical need of the practicing gastroenterologists contemplating endoscopy in pregnancy. It would be a ready reckoner for all endoscopic procedures including sedation in pregnancy based on latest available data so that endoscopists can take informed decisions, modify procedural techniques, and counsel their patients regarding possible risk and benefits. This will also stimulate clinical research in this unattended area by identifying loopholes of currently available data.[1]

Search Strategy

References for this review were identified through searches of PubMed from 1948 until July 2021 using search terms “(Pregnancy) and (endoscopy).” A total of 12,197 citations were screened by one reviewer. A total of 216 relevant citations were identified. Separate searches were done with keywords like (sedation), (esophagogastroduodenoscopy: EGD), (sclerotherapy), (endoscopic variceal banding), (flexible sigmoidoscopy), (colonoscopy), (endoscopic retrograde cholangiopancreatography: ERCP), (enteroscopy), (capsule endoscopy), (endoscopic ultrasound: EUS), (endoscopic cystogastrostomy), (radiation-free ERCP), (endoscopic spyscopy), and (pregnancy). Important cross-references from selected citations were included. Papers describing endoscopy postpartum or with small sample size (n < 10) were excluded unless describing novel/rare techniques. A total of 66 references are included in the review ([Fig. 1]).

Zoom Image
Fig. 1 Search strategy for systematic review on endoscopy in pregnancy.

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Anesthesia during Endoscopy in Pregnancy

Anesthetic agents during pregnancy can be subdivided into narcotics (meperidine, fentanyl, propofol), sedatives (diazepam and midazolam), general anesthetics (ketamine), and reversal agents (naloxone, flumazenil) or according to the Food and Drug Administration (FDA) pregnancy category (category A: none; category B: propofol, ketamine, naloxone; category C: fentanyl, flumazenil; category D: diazepam, midazolam, high dose, prolonged meperidine at term; category X: none).[1]

Prolonged administration (> 36 hours) of meperidine can cause respiratory depression and seizures. Hence, other safer opioid alternatives like fentanyl (FDA C) with faster onset and offset of action is used more frequently.

Propofol is increasingly being used in general population for sedation during endoscopy. Ketamine is an alternative in cases where propofol is expected to be inadequate. Both agents are short acting with rapid recovery although the safety has not been studied in first trimester. Propofol has narrow therapeutic index and can cause respiratory depression, arrest, and even death if improperly monitored. Prolonged, high dose of ketamine is unsafe in pregnancy.[1] [6]

Among sedatives, diazepam is a category D drug due to possible association with cleft lip, mental retardation, cardiac anomalies, and neurological defect (e.g., Mobius syndrome). Midazolam is preferred over diazepam as it is not associated with cleft lip. However, its use should be restricted specially in first trimester.[1] [6]

Naloxone is indicated for narcotic toxicity but can precipitate opioid withdrawal in dependent patients. Due to a report of fetal death, its use should be restricted in pregnancy. Flumazenil for benzodiazepine overdose has limited safety data in pregnancy and hence benzodiazepines should be used in lowest dose with gradual titration.[6]

Informed consent, review of medical history, routine blood investigations, obstetric consultation, patient stabilization, deferring if possible to second trimester, secure intravenous line, and referral to expert endoscopist for high-risk procedures are prerequisites of endoscopy with anesthetics during pregnancy.[6] Use of smallest effective dose of anesthetics, preferential use of category B drugs over C, minimization of procedure time (e.g., sigmoidoscopy instead of colonoscopy), oxygen supplementation, vitals, and electrocardiography monitoring with optional fetal cardiac monitoring are intraprocedural considerations. Fetal heart sounds should be documented before and after the procedure. At our institute, propofol under supervision of anesthesiologist is the drug of choice in all trimesters of pregnancy.[1]


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Esophagogastroduodenoscopy

Diagnostic EGD in pregnancy should be performed if strongly indicated and going to change the therapy. Upper GI bleed causing hemodynamic instability, ongoing bleed, recent onset progressive dysphagia with weight loss, and suspected upper GI malignancy are strong indications for EGD with high diagnostic yield.

Studies on diagnostic EGD in pregnancy have been summarized in [Table 1].1[3] [7] [8] These studies indicate that the highest diagnostic yield of EGD is for upper GI bleeding (95%) and lower for other indications (50–82%). Reflux esophagitis was most common finding in diagnostic EGD whereas peptic ulcer disease (PUD) was less common as compared to the general population. The symptoms of PUD decrease with pregnancy and reflux symptoms increase. The frequency of Mallory–Weiss tear as a cause of upper GI bleed was similar to that of PUD (14%).[7] Intractable vomiting and hyperemesis gravidarum (HG) are other frequent indications for EGD in pregnant female. However, the diagnostic yield of EGD in intractable vomiting (69%) was lower than upper GI bleeding (82%) according to a study from Israel on 60 pregnant patients.[8] More importantly, EGD in case of intractable vomiting does not lead to major change in management as empirical use of proton pump inhibitors and H2 blockers can provide symptomatic relief. Bagis et al have found that Helicobacter pylori infection was more common in pregnant females (n = 20) with HG (90%) compared to 50% in controls (n = 10). Although H. pylori therapy is generally deferred until postpartum period due to teratogenicity of antibiotics, validation of such association can warrant H. pylori therapy for HG.[3]

Table 1

Summary of studies on esophagogastroduodenoscopy (EGD; both diagnostic and therapeutic) and flexible sigmoidoscopy/colonoscopy in pregnancy

Author

Type of study

N

Maternal outcome

Fetal outcome

Abbreviations: AKI, acute kidney injury; APGAR, Appearance, Pulse, Grimace, Activity, and Respiration; DIC, disseminated intravascular coagulation; EHPVO, extrahepatic portal vein obstruction; EST, endoscopic sclerotherapy; EVL, endoscopic variceal ligation; GI, gastrointestinal; IBD, inflammatory bowel disease; NCPF, noncirrhotic portal fibrosis.

Diagnostic EGD

Cappell et al (1996)[7]

Retrospective case–control

83

One case of transient pyrexia resolving spontaneously, adverse pregnancy outcomes related to high-risk pregnancy rather than EGD

Health infants in 95% compared to 94% in controls; EGD did not induce abnormal fetal heart rate during EGD

Debby et al (2008)[8]

Retrospective clinical series

60

No maternal mortality, other complications not described

Fetal death and induced abortion in 2 and 5%, respectively. Eight had preterm delivery. No fetal malformations reported

Bagis et al (2002)[3]

Prospective

30

All 30 mothers had hyperemesis gravidarum. High prevalence of H. pylori infection (95%) compared to 50% in controls

Not available

Cappell (2003)[51]

Literature review of case reports

27

Singe maternal mortality due to metastatic malignancy

3 cases of stillbirth, 1 abortion, 1 preterm labor

Therapeutic EGD

Sclerotherapy for esophageal varices

Author

Type of study

N

Maternal outcome

Fetal outcome

Aggarwal et al (2001)[11]

Case series

17

All patients had acute variceal bleed.10 patients with EHPVO and 7 patients with NCPF underwent EST with absolute alcohol or sodium tetradecyl sulfate 1.5%; 12 patients required repeat EST and 2 required EVL due to failed EST

8 healthy infants (2 preterm), 3 stillbirths, 1 neonatal death, and 5 voluntary abortions

Kochhar et al (1990 and 1999) [9] [10]

Two cases series

10

For active variceal bleed in 5 and for prophylaxis in 5. Men number of sessions required were 3. Esophageal stricture dilated with Savary-Gilliard dilator

All delivered at term as healthy infants by normal vaginal delivery

Cappell (2003)[51]

Review of case reports

7

Successful EST for all

All infants were healthy

Mandal et al (2012)[12]

Retrospective

2

Successful EST, better if diagnosed and treated prior to pregnancy

Better if diagnosed prenatally

Endoscopic variceal ligation for esophageal varices

Mandal (2012)[12]

Retrospective

8

Successful EVL, better if diagnosed and treated prior to pregnancy

Better if diagnosed prenatally

Keepanasseril et al (2020)[13]

Retrospective

9

Maternal complications similar in NCPF and EHPVO. DIC, sepsis and AKI may complicate pregnancy

Perinatal outcomes similar with NCPF and EHPVO. Preterm birth most common fetal complication

Dhiman et al (2000)[14]

Case series

3

2 had uncomplicated delivery, one patient was better until 20th week of gestation (no further data), successful variceal eradication with EVL after faded EST

Uneventful delivery

Nonvariceal upper GI bleed (NVUGIB)

Nguyen et al (2010)[4]

Retrospective cohort study

1,210

Mortality was lower in pregnant women compared to nonpregnant, age-matched controls (n = 6,050)

The incidence of perinatal complications and prematurity was similar between the groups who underwent endoscopy compared to them who did not

Flexible sigmoidoscopy/colonoscopy

Ko et al (2020)[20]

Retrospective cohort study

48

No adverse obstetric events temporally associated with sigmoidoscopy, management changed in 78% following pregnancy

Fetal outcomes like prematurity and low birth weight was more common in IBD population compared to non-IBD pregnant women

Cappell et al (1996)[19]

Case–control study

56

No complications (48 sigmoidoscopies, 8 colonoscopies)

Among sigmoidoscopy group, after excluding voluntary abortions, rest all have delivered healthy babies (27 at term). 1 stillbirth, 1 death due to prematurity, and 1 cleft palate was reported. Complications were not higher compared to control pregnant female who did not undergo sigmoidoscopy. Adverse outcomes were unrelated to colonoscopy

Cappell et al (2010)[21]

Case–control study

20

16 colonoscopies in second trimester, 2 each in first and third trimester. Colonoscopy led to change in management in 35% cases. 2 cases with mild transient hypotension

No abnormal fetal heart rate during procedure. 1 involuntary abortion and 1 with congenital abnormality. Trend of better fetal outcomes (lower prematurity, abortion, higher birth weight, similar APGAR score, and congenital anomaly) in cases compared to controls

De Lima et al (2015)[23]

Systematic review

164

Above two studies plus 92 cases in case reports. 100 lower GI endoscopies in case reports (1 spontaneous abortion in first trimester, 1 induced abortion in second trimester, induction of labor and emergency caesarean section in 1 each)

Two fetal deaths, both in second trimester among 100 lower GI endoscopies in case reports

de Lima et al (2015)[2]

Prospective study (IBD)

42

2 spontaneous abortions were related to procedure, but abortion rate not higher compared to controls

(47 procedures, 12 colonoscopy, 35 sigmoidoscopy)

Median birth weight was lower compared to controls, however, prematurity, congenital malformations, and APGAR scores were not different compared to controls


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Maternal Outcomes ([Table 1])

Data from several studies suggest that EGD is safe in pregnancy and no serious adverse events were reported.[1] [3] [7] [8] The risk of EGD in pregnancy is similar to that of general population. Pregnant women are generally young to early middle age and likely to have lower complication rates compared to elderly. Hemodynamic instability should be corrected prior to EGD.


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Fetal Outcomes

Most of the reported fetal adverse outcomes (preterm delivery, still births, spontaneous abortion) occurred in high-risk pregnancies and not temporally related to EGD ([Table 1]).[1] [3] [7] [8] Apgar scores in infants after birth were similar in patients who underwent EGD versus controls.[1] On fetal cardiac monitoring, fetal heart rate remained normal during EGD.[1]


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Therapeutic EGD

Variceal Bleed

Extrahepatic portal vein obstruction and noncirrhotic portal fibrosis are the important causes of variceal bleed in pregnancy as fertility is compromised in cirrhosis due to altered estrogen metabolism. The risk of bleeding increases in pregnancy due to increased blood volume and increased peripheral vascular resistance due to compression of inferior vena cava by gravid uterus. The risk of bleeding is highest in second trimester as portal hypertension peaks and during labor due to increased vascular resistance due to performance of Valsalva man oeuvre. De novo variceal hemorrhage and bleeding from preexisting varices occur in 30 and 75% cases, respectively, in pregnancy. Beta-blockers are useful in reducing portal pressure and should be continued. There is risk of decompensation of preexisting liver disease during variceal bleed in pregnancy leading to poor fetomaternal outcomes and hence prophylactic treatment should be considered whenever pregnancy is contemplated.

Fetal outcomes are favorable (100%) in a study by Kochhar et al compared to that by Aggarwal et al (67%) with regard to endoscopic sclerotherapy (EST) which is mainly due to lower incidence of acute variceal bleed in the former (50 vs. 100% in the later) ([Table 1]).[9] [10] [11] The data regarding safety of endoscopic variceal ligation (EVL) is also limited to case series ([Table 1]).[12] [13] [14] EVL is preferred over EST in pregnancy due to lower incidence of complications, higher efficacy, and conflicting reports on fetal outcomes with EST.


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Nonvariceal Upper GI Bleed

The most common cause of nonvariceal upper GI bleed (NVUGIB) in pregnant women is Mallory–Weiss tear (25%) followed by gastritis (12%), PUD (6.8%), esophagitis (2.5%), anastomotic ulcer (0.2%), and Dieulafoy’s lesion/arteriovenous malformation (0.1%) according to a nationwide study (n = 1,210).[4] A conservative, nonendoscopic management of NVUGIB in pregnant women is not associated with increased fetomaternal complications according to the study. Fetal outcomes were not different compared to controls. Hence, therapeutic EGD is safe in actively bleeding pregnant patients.[4] Rest of the studies are limited to case reports.

The data regarding NVUGIB in pregnancy is difficult to extrapolate given the variety of procedures performed for NVUGIB (epinephrine/glue/thrombin/saline injection, electro/photo/thermo/argon plasma coagulation, or mechanical therapy with hemoclips) and various causes with different stigmata of bleed (active spurt/ooze, nonbleeding visible vessel, and adherent clot).[1]

Special considerations should be made during electrocoagulation and epinephrine injection. During electrocoagulation, the grounding pad should be kept in such a way from the interventional catheter that the current does not traverse the uterus/fetus. Epinephrine (pregnancy category C) exposure during first trimester has been associated with congenital malformation, although it could be due to high-risk pregnancy.[1]


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Endoscopic Therapy for Achalasia

Achalasia during pregnancy can be confused with reflux and hyperemesis. The goal of treatment during pregnancy is to avoid maternal malnutrition and consequent fetal growth retardation and death. Nutrition can be managed initially with nasogastric feeding or parenteral nutrition. In case of intolerance or refusal, botulinum toxin (BT) injection at lower esophageal sphincter or pneumatic balloon dilation (PBD) can be performed.[15] There are five case reports of BT injection for achalasia during pregnancy mainly in the second and third trimester. There are seven case reports of PBD in achalasia with pregnancy.[15] These modalities can have transient effect with recurrence but can be helpful to tide over the crisis. Currently, there are no case reports of peroral endoscopic myotomy (POEM) for achalasia in pregnancy although it could be an effective treatment. There is only one case report of laparoscopic Heller’s myotomy (LHM) in second trimester. POEM or LHM can only be considered in resistant cases where PBD and BT fails.[15]


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Endoscopy to Improve Maternal Nutrition

Percutaneous Endoscopic Gastrostomy and Percutaneous Endoscopic Gastrojejunostomy

Enteral nutrition with percutaneous endoscopic gastrostomy (PEG) or percutaneous endoscopic gastrojejunostomy (PEG- J) may be indicated in pregnancy if maternal nutrition is compromised due to dysphagia, severe odynophagia, obstruction at gastroesophageal junction, intractable HG, eating disorders like anorexia nervosa, chronic intestinal pseudo-obstruction, and neurologic disorders precluding deglutition like motor neurone disease, myotonic dystrophy, or massive stroke. PEG can be beneficial in maintaining maternal nutrition thus improving fetal outcomes as seen in five out of six case reports. Fetal adverse outcome is mainly related to maternal high-risk condition rather than PEG.[1]

Precautions like ultrasound-guided marking of upper border of uterus should be done prior to PEG to avoid inadvertent uterine puncture. Gravid uterus can cause gastric compression leading to pain and leak around stoma. Feeding tube can be placed via the gastrostomy into the jejunum (PEG-J) in case of refractory nausea, vomiting, and aspiration (five cases reports).[1]


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Flexible Sigmoidoscopy and Colonoscopy

Preparations

Sigmoidoscopy preparation with tap water, saline, or sodium phosphate enema can lead to fluid shifts and volume overload/dehydration along with dyselectrolytemia. Chronic use may cause dyselectrolytemia and fetal bone demineralization/growth failure. However, risks are negligible in pregnant female without heart failure, chronic renal insufficiency, or dehydration.[1]

Among orally administered preparations, polyethylene glycol (isotonic, pregnancy category C) is preferred over sodium phosphate preparations as the later can lead to dyselectrolytemia and even renal insufficiency in at-risk or dehydrated patients with consequent effects on fetus.[16] In a prospective study of pregnant patients with constipation, polyethylene glycol relieved constipation in three-fourths without any complications.[17]


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Indications

Acute lower GI bleeding (except in suspected hemorrhoids), sigmoid/rectal mass, or stricture are strong indications of flexible sigmoidoscopy in pregnancy. Severe, persistent diarrhea and severe flare of inflammatory bowel disease are moderate indications and investigation of lower abdominal pain/altered bowel habits are weak indications. Volvulus is an indication of emergency surgery as it can lead to worse fetomaternal outcomes. Reports have described successful decompression of sigmoid volvulus by sigmoidoscopy.[18] The diagnostic value of sigmoidoscopy is highest for hematochezia (76%) compared to other indications (29%).[19] Reported change in management after sigmoidoscopy/colonoscopy ranges from 35 to 78%.[19] [20] [21]

Therapeutic sigmoidoscopy to release uterine incarceration have been reported in five patients by Seubert et al.[22]


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Maternal and Fetal Outcomes

The maternal and fetal outcomes from retrospective and prospective studies and systematic review including various case reports indicate highly favorable fetomaternal outcomes ([Table 1]).[19] [20] [23] Maternal complications were transient, self-limited, or unrelated to procedure. Poor fetal outcomes correlated with high-risk pregnancy. Congenital anomalies were not higher compared to controls. These data suggest safety of sigmoidoscopy when performed for strong indications.

The data for colonoscopy in pregnancy is, however, relatively scanty with strongest evidence in second trimester with lowest risk for fetus. Colonoscopy in first trimester can induce premature labor/neonatal depression. Colonoscopy should generally be deferred in all the trimesters of pregnancy for elective indications. Despite the fact that colonoscopy can be technically difficult due to distortion of normal landmarks in pregnancy, cecal intubation rates are high.


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Endoscopic Retrograde Cholangiopancreatography

Risks of ERCP

Pregnancy increases gallstone formation as estrogen promotes cholesterol synthesis leading to supersaturation of bile and progesterone inhibits gallbladder contractility. Choledocholithiasis complicated by jaundice, pancreatitis, or cholangitis can be treated safely by therapeutic ERCP in pregnant women as compared to complex biliary surgery which increases risk of fetal loss. As compared to EGD, unique risk of ERCP in pregnancy includes radiation exposure. The teratogenic dose of radiation in first trimester is above 50 mGy.[24] Small studies have shown that fetal radiation exposure up to 3.1 mGy can occur during ERCP which is significantly lower than the acceptable threshold.[25] However, more recent studies have shown that fetal radiation dose may not be trivial and exceed 10 mGy when total dose area product was calculated.[26] Prolonged procedure and duodenal intubation time, requirement of higher anesthetic doses, and risk of postsphincterotomy bleeding/perforation are the other unique risks with ERCP.


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Clinical Evidence

Until recently, the data regarding safety of ERCP in pregnancy was based on several retrospective small series of total 350 patients.[27] A nationwide cohort study published in 2015 consisting of 907 pregnant women undergoing ERCP represents the highest study population until now. This matched control study by Inamdar et al have shown that complications of ERCP were similar in pregnant as compared to nonpregnant women although risk of post-ERCP pancreatitis (PEP) was considerably higher in pregnant (adjusted odds ratio [aOR]: 2.8), more so in nonteaching hospitals (aOR: 3.5).[28] Fetomaternal outcomes were noninferior to national rates.[28] Pregnancy was an independent risk factor for PEP. This data emphasizes the fact that although ERCP is safe in pregnancy, it should be done in carefully selected cases with due precautions in specialized centers.

There are several retrospective studies, case series, and reports of ERCP in pregnancy. We have summarized the results of these studies with sample size (n ≥10) in [Table 2].[25] [28] [29] [30] [31] [32] [33] [34] [35] [36] [37] [38] [39] [40] [41] The limitations of existing studies are retrospective in nature (only one prospective), missing fetal outcomes (10–40%), limited follow-up after birth, and lack of control.[1] A large study with control group is required to investigate whether ERCP increases the background risk of teratogenicity (1.8%).

Table 2

Summary of studies (sample size: n ≥10) on endoscopic retrograde cholangiopancreatography (ERCP) in pregnancy

Author

Year

Number

Study type

Gestation

(trimester)

Intervention

Imaging modality

Complication

Fetal outcomes

Abbreviations: BES, biliary endoscopic sphincterotomy; CBD, common bile duct; EPBD, endoscopic papillary balloon dilation; ES, endoscopic sphincterotomy; EUS, endoscopic ultrasound; IUGR, intrauterine growth retardation; NBD, nasobiliary drain; PEP, post-ERCP pancreatitis; USG, ultrasound.

Jamidar et al [29]

1995

29

Retrospective

1st 15

2nd 8

3rd 6

BES-14 Biliary stent-1

Minor papilla ES-1

PD stent-1

Fluoroscopy time not reported

Post-ERCP Pancreatitis : PEP-1

Spontaneous abortion-1

Neonatal death -1

Preterm-1

Farca et al[30]

1997

10

Prospective

Not known

BES+ stent -10

Fluoroscopy

Impacted stone requiring repeat ERCP-1

None

Tham et al [25]

2003

15

Retrospective

1st 1

2nd 5

3rd 9

ES-6

Biliary stent-1

Median fluoroscopy time 3.2 min

Mild PEP -1

None

Kahaleh et al[31]

2004

17

Retrospective

No information

BES-17

Median fluoroscopy time -14 s

Post ES bleed-1

PEP-1

Pre-ecalampsia-1

None

Gupta et al[32]

2005

18

Retrospective

1st 4

2nd 6

3rd 8

CBD clearance -14

Stents-4

Fluoroscopy -11

USG-5

Bile aspiration-2

Mild PEP-1

Post-ES Bleed-1

Preterm-1

Sharma and Maharshi[33]

2008

11

Retrospective

No information

ES = 11

Stent = 11

Mechanical lithotripsy = 1

Not used

None, 1 required surgery postpartum for large stones

No adverse outcomes

Shelton et al[34]

2008

21

Retrospective

1st 7

2nd 9

3rd 5

ES- 21

EUS-6

Choledochoscopy-5

Not used

EUS/MRCP

Wire-guided bile observation

Mild PEP-1 (4.8%)

1-IUGR

Tang et al[35]

2009

65

Retrospective

1st 17

2nd 20

3rd 31

ES-64

Biliary stent-16

Mechanical lithotripsy-1.5%

Precut and

Prophylactic PD stent-2.9%

Median fluoroscopy time: 1.45 min

Mild PEP-16%

Minor bleeding 7.4%

First trimester ERCP: Preterm-20%

LBW-21.4%

Bani Hani et al[36]

2009

10

Retrospective

1st 2

2nd 5

3rd 3

ES-10

Fluoroscopy all- duration Unknown

PEP-1 (10%)

None

Daas et al[37]

2009

17

Retrospective

1st 2

2nd 3

3rd 17

ES-10

Biliary stent-4

Mean fluoroscopy time 8 s

Nil

None

García-Cano et al [38]

2012

11

Retrospective

1st 1

2nd 4

3rd 6

ES-9

Stent -2

Fluoroscopy 5 cases (median time 30 s)

Hyperamylasemia-1

None

Zhou et al[39]

2013

17

Retrospective

All 3rd

NBD-7

Biliary stent-10

Fluoroscopy time not reported

Post ES bleed-1

PEP-1

6 preterm

Ersoz et al[40]

2016

22

Retrospective

1st 2

2nd 3

3rd 17

ES=22

EPBD-22

Not used

Mild PEP-2/22

None

Inamdar et al[28]

2016

907

National data base review

No information

No information

No information

PEP-12.13%

vs. 5% in matched controls

Preterm-1.87%

Fetal distress-0.33%

Fetal loss-0.67%

Konduk and Bayraktar[41]

2019

25

Retrospective

1st 2

2nd 3

3rd 17

ES-25

Stone extraction-18

Fluoroscopy-18 (6 s)

Nonradiation-7

None

None


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ERCP Interventions in Pregnancy

Interventions described during ERCP in pregnancy include endoscopic biliary sphincterotomy with or without biliary stenting, biliary stenting alone, balloon sweep without sphincterotomy, endoscopic papillary balloon dilation, mechanical lithotripsy, precut sphincterotomy, pancreatic stent placement, nasobiliary tube placement, and choledochoscopy ([Table1]).


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Repeat or Failed ERCP

Technical success is generally high (> 90%). A repeat ERCP/surgery is required due to recurrent biliary disease in < 10% patients (24/296). Failed ERCP was reported in < 5% (14/296) patients.[1]


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Maternal Considerations

The risk of post-ERCP complications (bleeding, perforation) are similar in pregnancy compared to nonpregnant (bleeding risk 2%) except for higher risk of PEP.[28] This is contrary to earlier data describing similar risk of PEP in pregnancy compared to nonpregnant. However, the risk is small and clinically acceptable. Lack of liberal use of intravenous hydration, teratogenic rectal nonsteroidal anti-inflammatory drugs, or an inherent physiological mechanism could explain this.[28] PEP in pregnancy is mostly mild-moderately severe.

Rates of postsphincterotomy bleeding in pregnancy (1%) are lower than general population (2%) and similar to age-matched nonpregnant females (0.96%).[28] Most of the bleeding can be tackled endoscopically. Pregnancy being a mild hypercoagulable state, does not lead to increased bleeding tendency.

Rate of perforation was comparable in pregnant versus nonpregnant age-matched female during ERCP.[28] Postsphincterotomy bilioenteric fistula were reported to be successfully treated with biliary stenting.[42]

Maternal outcomes in those undergoing ERCP is similar to other pregnant women with no increase in maternal mortality.[28]


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Fetal Considerations

Based on an earlier review of literature, among 296 pregnancies fatal outcomes were not reported in 42 cases. Majority had normal term delivery (n = 237) and rest had premature birth (n = 11), spontaneous abortion (n = 3), sudden death after birth (n = 2), and induced abortion (n = 1). Overall, perinatal mortality was less than 1% with no congenital anomalies.[1] However, most of the studies did not look specifically for congenital anomalies and follow-up after birth was limited. Data from national database study showed that the rate of prematurity (1.87%) was lower compared to national average (11.5%). Fetal distress/loss was seen in 1% cases similar to population rates.[28] The data is reassuring and suggests that the fetal risk is small and acceptable although comparatively higher than maternal risk. Overall benefits of ERCP in complicated choledocholithiasis seem to outweigh the risks.


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Technical Modifications and Considerations for Radiation-Free ERCP or Reduction in Radiation Exposure during Therapeutic ERCP in Pregnancy

Various technical modifications and procedural strategies like (1) wire-guided bile observation, (2) stent-guided/precut sphincterotomy for biliary access, (3) EUS guidance, (4) spy cholangioscopy, (5) expert endoscopist (reduce radiation exposure by shorter procedure time), (6) two-staged ERCP, (7) contrast-enhanced ultrasound-guided ERCP, and (8) technical modifications in X-ray technique have been described to minimize fetal radiation exposure during ERCP which are listed in [Table 3].[29] [33] [34] [43] [44] [45] [46] [47] [48] [49] [50] [51] [52] [53] [54] [55]

Table 3

Summary of studies describing technical modifications to reduce radiation exposure during therapeutic endoscopic retrograde cholangiopancreatography (ERCP) in pregnancy

Author

Modified ERCP techniques

Rationale

Abbreviations: CBD, common bile duct; ES, endoscopic sphincterotomy; EUS, endoscopic ultrasound.

Brewer et al (2021)[43]

Digital single operator cholangioscopy (DSOC)-guided ERCP (n = 10)

Fluoroscopy-less ERCP in 50% cases, safe and feasible alternative to standard ERCP, acceptable maternal and fetal safety profile

Sharma and Maharshi (2008) [33]

Two-stage technique: ES + stenting without fluoroscopy in pregnancy followed by definitive ERCP postpartum

Avoidance of radiation exposure

Ersoz et al (2016)[40]

ES followed by endoscopic papillary balloon dilation (EPBD) and balloon sweep

Nonradiation technique to facilitate complete stone removal

Shelton et al (2008) [34]

Catheter bile aspiration followed by wire-guided bile observation or stent-guided biliary sphincterotomy or precut sphincterotomy and finally spy cholangioscopy

Nontraditional techniques for ERCP with increase in efficacy with wire-guided observation and spy cholangioscopy

Zhou et al (2013)[39]

Nasobiliary drain or stent followed by definite ERCP postpartum for third trimester pregnancy presenting with cholangitis

Modified ERCP protocol in 3rd trimester acute cholangitis by initial temporizing measure and later definitive therapy

Polydorou et al (2012)[44]

Magnetic resonance cholangiopancreatography (MRCP) and nonradiation ERCP followed by immediate laparoscopic cholecystectomy in biliary pancreatitis

MRCP to clarify the number of stones to guide nonradiation ERCP

Huang et al (2013)[45]

Comparison of ultrasound guidance for ERCP versus nonradiographic ERCP

Higher success rate of complete stone removal, shorter hospital stay, and lower complication rates with ultrasound guidance for ERCP; confirm biliary cannulation by ultrasound

Sethi et al (2015)[46]

EUS guidance followed by same session ERCP with or without spy cholangioscopy

Safe and effective radiation-free ERCP in pregnant patients

Götzberger et al (2012)[47]

EUS followed by contrast-enhanced ultrasound-guided ERCP by injecting ultrasound contest agent via ERCP catheter

Intraductal application of ultrasound contrast clearly delineates biliary pathology

Vohra et al (2014) [48]

Single session EUS followed by scheduled ERCP: If endoscopic ultrasound (EUS) confirms no stone, ERCP can be avoided; if EUS shows stones, it helps to give idea about location, size and number of stones, guide therapy, and confirm stone clearance

Confirm CBD stone and guide therapy and guide nonradiation intervention

Bar-Meir and Rotmensch (1984) [49]

Use of ultrathin caliber baby cholangioscope through biopsy channel of side view endoscope

Investigation of obstructive jaundice without radiation exposure

Baillie et al (1990) [50]

Place lead shielding over mother’s abdomen and radiation dosimetry badge to monitor radiation. Reduction in fluoroscopy time and avoiding spot radiographs for documentation

Methods to reduce radiation exposure during ERCP

Cappell (2003) [51]

Modern X-ray machine, consulting tradition physicist, attending anesthesiologist, avoiding fellow participation, deferring to second trimester if possible, minimize procedure time, referral to tertiary center, prior obstetric consultation, and informed consent

Reduction in radiation scatter and overall reduction in radiation exposure

Baron and Schueler (2009)[52]

Avoid magnification fluoroscopy image, adjust maternal position in fluoroscopy table, digital image acquisition instead of film-screen radiography, variable rate pulsed fluoroscopy rather than continuous fluoroscopy, beam collimation to smallest field, placing image receptor close to patient, and X-ray tube as far as possible

Technical modifications to reduce fetal radiation exposure

Jamidar et al (1995)[29]

Performing pregnancy test prior to ERCP in right clinical setting (missed period in menstruating female), direct sphincterotome cannulation

Avoid ERCP in unrecognized pregnancy, reduce procedure time

Binmoeller and Katon (1990)[53]

Needle knife precut sphincterotomy

Reduction in fluoroscopy time

Nesbitt et al (1996)[54]

Magnesium administration for tocolysis

Decrease biliary tract spasm

Rahmin et al (1994) [55]

Bile aspiration to confirm CBD cannulation

Avoid radiation exposure

Earlier reports focused on wire-guided bile aspiration, precut sphincterotomy, and lead shielding to reduce radiation exposure.[53] [55] Later on, modification in fluoroscopy techniques have been described.[51] [52] Two-staged procedures with nasobiliary drain and stent placement has also been described.[33] [39] [40] The recent trend is toward radiation-free, single-session ERCP in pregnancy with either EUS guidance or by digital single-operator cholangioscopy (DSOC).[43] [46] [47] [48]


#

Endoscopic Spyscopy

Spyscope/baby scope introduced through the biopsy channel of ERCP scope can be used to confirm common bile duct (CBD) stone clearance postsphincterotomy and evaluate intracholedochal tumor or stricture. Five such cases have been described in the literature without any adverse maternal outcomes.[34] Spyscopy has been described along with EUS guidance for management of CBD stone in pregnancy.[56]

Cholangioscopy has been revolutionized with the use of DSOC (SpyGlass DS, Boston Scientific) with disposable cholangioscope and digital image capture. This results in better image quality and maneuverability with advantages like feasibility of radiation-free ERCP, direct visualization of the biliary system, ability for tissue acquisition, and cholangioscopy-directed therapy. ERCP guided by DSOC can help avoid radiation in 50% cases as shown in a recent study.[43] Fetal outcomes have not been described in these reports. Larger studies reporting fetomaternal outcomes are required to establish this attractive radiation-free technology as an alternative to therapeutic ERCP for CBD stones in pregnancy.


#

Endoscopic Ultrasound

EUS is safe in pregnancy as it involves EGD followed by ultrasound examination of pancreaticobiliary tract.[57] However, EUS may require prolonged procedure time exposing the mother to higher anesthetic doses and the indicated patients could be sicker (e.g., biliary pancreatitis) compared to those undergoing EGD. Clinical data in EUS safety in pregnancy is limited to small case series. In the largest series, Shelton et al used EUS in suspected CBD stone.[34] Adverse fetal outcomes like death due to recurrent cholangitis and HELLP syndrome are mostly unrelated to EUS and due to severe maternal illness and conservative management of biliary pancreatitis.[58] Hence, in the absence of strong clinical data, EUS should be used if there is intermediate probability of CBD stone and magnetic resonance cholangiopancreatography is not desirable. EUS can be done in the same session prior to ERCP.[48] [59] Performing ERCP through linear echo-endoscope ultrasound guidance has been described.[60]


#

Small Bowel Endoscopy

Enteroscopy

Enteroscopy in pregnancy is technically difficult due to compression of small bowel loops by gravid uterus precluding deep intubation. The challenges of performing enteroscopy in pregnancy are prolonged procedure time, higher requirement of anesthetic doses, and possibility of placental abruption due to pressure from enteroscope. There is currently no published clinical data on enteroscopy in pregnant females. Only indication of balloon-assisted enteroscopy could be small bowel tumor presumed to be malignant and life-threatening small bowel bleeding not reachable by push enteroscopy. Push enteroscopy could be technically easier given no need for deep small bowel intubation and shorter procedure time than balloon-assisted enteroscopy. Spiral enteroscopy is contraindicated in pregnancy.[1]


#

Video Capsule Endoscopy

Video capsule endoscopy (VCE) is an attractive option in pregnancy for small bowel imaging due to absence of radiologic exposure and need for deep enteroscopy although there is concern regarding microwave emission from active capsule. Prolonged small bowel transit in pregnancy due to inhibitory effect of progestin on small bowel smooth muscle contractility can theoretically increase the risk of capsule retention in pregnancy and can lead to incomplete small bowel examination. However, two cases of VCE have been described in the literature. In a case of esophageal varices postsclerotherapy, esophageal VCE ruled out active bleeding from esophageal varices resulting in normal delivery.[61] In the another case with active small bowel bleed, jejunal ulcerated lesion was identified which turned out to be carcinoid.[62] In one case of Crohn’s disease with missed retained capsule became pregnant which led to ileal resection.[63] Hence, VCE can be beneficial in pregnancy if strongly indicated unless other risk factors of retention are present.


#

Endoscopic Cystogastrostomy

Two cases of endoscopic cystogastrostomy have been described in the literature under abdominal ultrasound guidance (not EUS) at 17th and 21st week of gestation.[64] [65] Postprocedure pain and leucocytes have been described which was successfully treated with antibiotics and placement of additional cyst-gastric stents. Hence, endoscopic cystogastrostomy in the current era with EUS guidance is a useful option in pregnant female with symptomatic pancreatic fluid collections as an alternative to surgical cystogastrostomy. Proper informed consent and explanation of alternative modalities of treatment are essential in these settings.


#
#

Conclusion

This review highlights the fact that endoscopy should be done in pregnancy only if strongly indicated. Whenever possible it is wise to defer endoscopy in first trimester and peripartum period unless an emergency like significant GI bleed or suspected malignancy is present. Minimally invasive, short-duration procedures should be substituted for long invasive procedures (e.g., flexible sigmoidoscopy rather than colonoscopy). Stabilizing patient prior to procedure is vital and it should be performed by expert endoscopist in a hospital-based settings. Informed consent with clear explanation of limited clinical data on fetomaternal safety is a prerequisite. Documentation of fetal heart sound pre- and postprocedure is mandatory with optional intraprocedure fetal heart rate monitoring. Pulse oximetry, oxygen supplementation, and electrocardiography monitoring is needed during procedure. It is important to perform EGD in left lateral position to avoid reflux and to avoid abdominal compression (during colonoscopy) and prone or supine position (to avoid compression of inferior vena cava by gravid uterus).

More prospective or case–control studies are required to establish safety of various endoscopic procedures during pregnancy. Most of the current evidence and recommendations are based on retrospective data ([Fig. 2]). Randomized controlled studies are unlikely due to medico-legal issues. Ultrathin scopes and EUS guidance can help avoid radiation during ERCP with minimal anesthesia and pressure on graved uterus. Smaller, steerable video capsule endoscopes in future can help evaluate entire intestine noninvasively in a pregnant female as an alternative to invasive endoscopy.

Zoom Image
Fig. 2 Recommendations for various endoscopic procedures in pregnancy with available clinical evidence and data on fetomaternal outcomes. BT, botulinum toxin; EGD, esophagogastroduodenoscopy; EST, endoscopic sclerotherapy; ERCP, endoscopic retrograde cholangiopancreatography; EUS, endoscopic ultrasound; EVL, endoscopic variceal ligation; H. pylori, Helicobacter pylori; IBD, inflammatory bowel disease; LBW, low birth weight; NVUGIB, nonvariceal upper gastrointestinal bleed; PBD, pneumatic balloon dilation; PEG, percutaneous endoscopic gastrostomy; PEG-J, percutaneous endoscopic gastrojejunostomy; PEP, post-ERCP pancreatitis; VCE, video capsule endoscopy.

#
#

Conflict of Interest

None declared.

Authors’ Contribution

Conceptualization: P.P., MT; Literature review and writing original draft: P.P.; Illustrations: P.P.; Images: P.P.; Proof reading and critical review: M.T., D.N.R.; approving final manuscript: M.T., P.P., D.N.R.

Acknowledgment

None.

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Address for correspondence

Partha Pal, MD, DNB, MRCP (UK)
Medical Gastroenterology, Asian Institute of Gastroenterology
6-3-661, Somajiguda, Hyderabad, Telangana 500082
India   

Publication History

Article published online:
17 November 2021

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  • References

  • 1 Cappell MS. Risks versus benefits of gastrointestinal endoscopy during pregnancy. Nat Rev Gastroenterol Hepatol 2011; 8 (11) 610-634
  • 2 de Lima A, Zelinkova Z, van der Woude CJ. A prospective study of the safety of lower gastrointestinal endoscopy during pregnancy in patients with inflammatory bowel disease. J Crohn’s Colitis 2015; 9 (07) 519-524
  • 3 Bagis T, Gumurdulu Y, Kayaselcuk F, Yilmaz ES, Killicadag E, Tarim E. Endoscopy in hyperemesis gravidarum and Helicobacter pylori infection. Int J Gynaecol Obstet 2002; 79 (02) 105-109
  • 4 Nguyen GC, Dinani AM, Pivovarov K. Endoscopic management and outcomes of pregnant women hospitalized for nonvariceal upper GI bleeding: a nationwide analysis. Gastrointest Endosc 2010; 72 (05) 954-959
  • 5 Shergill AK, Ben-Menachem T, Chandrasekhara V. ASGE Standard of Practice Committee. et al Guidelines for endoscopy in pregnant and lactating women. Gastrointest Endosc 2012; 76 (01) 18-24 Erratum in: Gastrointest Endosc. 2013 May;77(5):833. PMID: 22579258
  • 6 Cappell MS. Sedation and analgesia for gastrointestinal endoscopy during pregnancy. Gastrointest Endosc Clin N Am 2006; 16 (01) 1-31
  • 7 Cappell MS, Colon VJ, Sidhom OA. A study of eight medical centers of the safety and clinical efficacy of esophagogastroduodenoscopy in 83 pregnant females with follow-up of fetal outcome with comparison control groups. Am J Gastroenterol 1996; 91 (02) 348-354
  • 8 Debby A, Golan A, Sadan O, Glezerman M, Shirin H. Clinical utility of esophagogastroduodenoscopy in the management of recurrent and intractable vomiting in pregnancy. J Reprod Med 2008; 53 (05) 347-351
  • 9 Kochhar R, Kumar S, Goel RC, Sriram PV, Goenka MK, Singh K. Pregnancy and its outcome in patients with noncirrhotic portal hypertension. Dig Dis Sci 1999; 44 (07) 1356-1361
  • 10 Kochhar R, Goenka MK, Mehta SK. Endoscopic sclerotherapy during pregnancy. Am J Gastroenterol 1990; 85 (09) 1132-1135
  • 11 Aggarwal N, Sawhney H, Vasishta K, Dhiman RK, Chawla Y. Non-cirrhotic portal hypertension in pregnancy. Int J Gynaecol Obstet 2001; 72 (01) 1-7
  • 12 Mandal D, Dattaray C, Sarkar R, Mandal S, Choudhary A, Maity TK. Is pregnancy safe with extrahepatic portal vein obstruction? An analysis. Singapore Med J 2012; 53 (10) 676-680
  • 13 Keepanasseril A, Gupta A, Ramesh D, Kothandaraman K, Jeganathan YS, Maurya DK. Maternal-fetal outcome in pregnancies complicated with non-cirrhotic portal hypertension: experience from a tertiary centre in South India. Hepatol Int 2020; 14 (05) 842-849
  • 14 Dhiman RK, Biswas R, Aggarwal N, Sawhney H, Chawla Y. Management of variceal bleeding in pregnancy with endoscopic variceal ligation and N-butyl-2-cyanoacrylate: report of three cases. Gastrointest Endosc 2000; 51 (01) 91-93
  • 15 Vosko S, Cohen DL, Neeman O, Matalon S, Broide E, Shirin H. Achalasia during pregnancy: proposed management algorithm based on a thorough literature review. J Neurogastroenterol Motil 2021; 27 (01) 8-18
  • 16 Patel V, Nicar M, Emmett M. et al Intestinal and renal effects of low-volume phosphate and sulfate cathartic solutions designed for cleansing the colon: pathophysiological studies in five normal subjects. Am J Gastroenterol 2009; 104 (04) 953-965
  • 17 Neri I, Blasi I, Castro P, Grandinetti G, Ricchi A, Facchinetti F. Polyethylene glycol electrolyte solution (Isocolan) for constipation during pregnancy: an observational open-label study. J Midwifery Womens Health 2004; 49 (04) 355-358
  • 18 Rottenstreich M, Mosmar K, Ehrlich Z, Kitroser E, Grisaru-Granovsky S. Flexible endoscopic decompression for treatment of sigmoid volvulus in pregnancy. Eur J Obstet Gynecol Reprod Biol 2019; 242: 184-185
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Fig. 1 Search strategy for systematic review on endoscopy in pregnancy.
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Fig. 2 Recommendations for various endoscopic procedures in pregnancy with available clinical evidence and data on fetomaternal outcomes. BT, botulinum toxin; EGD, esophagogastroduodenoscopy; EST, endoscopic sclerotherapy; ERCP, endoscopic retrograde cholangiopancreatography; EUS, endoscopic ultrasound; EVL, endoscopic variceal ligation; H. pylori, Helicobacter pylori; IBD, inflammatory bowel disease; LBW, low birth weight; NVUGIB, nonvariceal upper gastrointestinal bleed; PBD, pneumatic balloon dilation; PEG, percutaneous endoscopic gastrostomy; PEG-J, percutaneous endoscopic gastrojejunostomy; PEP, post-ERCP pancreatitis; VCE, video capsule endoscopy.