Gastrointestinal and hepatic diseases during the COVID-19 pandemic: Manifestations, mechanism and management

doi:10.3748/wjg.v27.i28.4504

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World Journal of Gastroenterology

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World J Gastroenterol. Jul 28, 2021; 27(28): 4504-4535
Published online Jul 28, 2021. doi: 10.3748/wjg.v27.i28.4504

Table 1 Incidence of common gastrointestinal symptoms in patients with severe acute respiratory syndrome coronavirus 2 infection

Ref.	Patient number	Anorexia, nausea or vomiting, n (%)	Diarrhea, n (%)	Abdominal pain, n (%)
Kujawski et al[207], 2020	12	Nausea: 3 (25)	4 (33.3)	2 (16.7)
Hajifathalian et al[44], 2020	1059	Anorexia: 240 (22.7)	234 (22.1)	72 (6.8)
		Nausea: 168 (15.3)
		Vomiting: 91 (8.6)
Young et al[208], 2020	18	NA	3 (17)	NA
Tabata et al[209], 2020	104	NA	8 (9.6)	NA
Wölfel et al[210], 2020	9	NA	2 (22)	NA
Chen et al[26], 2020	99	Nausea and vomiting: 1 (1)	2 (2)	NA
Xu et al[27], 2020	62	NA	3 (8)	NA
Gritti et al[211], 2020	21	NA	5 (23.8)	NA
COVID-19 National Incident Room Surveillance Team[212]	295	Nausea: 34 (11.5)	48 (16.3)	6 (1)
COVID-19 National Emergency response Center[213]	28	NA	2 (7)	1 (4)
Sierpiński et al[214], 2020	1942	NA	470 (24.2)	NA
Wu et al[28], 2020	80	Nausea and vomiting: 1 (1.25)	1 (1.3)	NA
Wang et al[12], 2020	138	Anorexia: 55 (39.9)	14 (10.1)	3 (2.2)
Wang et al[12], 2020	138	Nausea: 14 (10.1)	14 (10.1)	3 (2.2)
Shi et al[29], 2020	81	Anorexia: 1 (1)	3 (4)	NA
Shi et al[29], 2020	81	Vomiting: 4 (5)	3 (4)	NA
Yang et al[30], 2020	50	Vomiting: 2 (4)	NA	NA
Mo et al[31], 2020	155	Anorexia: 26 (31.7)	7 (4.5)	NA
		Nausea: 3 (3.7)
		Vomiting: 3 (3.7)
Qi et al[215], 2020	267	Anorexia: 46 (14.2)	10 (3.7)	NA
Qi et al[215], 2020	267	Nausea: 6 (2.2)	10 (3.7)	NA
Wen et al[216], 2020	417	NA	29 (7)	NA
Dan et al[217], 2020	305	Anorexia: 101(50.2)	146 (49.5)	12 (6)
		Nausea: 59 (29.4)
		Vomiting: 3 (2)
Ma et al[218], 2020	81	NA	6(7.41)	NA
Luo et al[41], 2020	1141	Anorexia: NA	68 (6)	45 (3.9)
		Nausea: 134 (11.7)
		Vomiting: 119 (10.4)
Liu et al[219], 2020	238	Anorexia: 14 (9.2)	14 (9.2)	1 (0.7)
		Nausea: 2 (1.3)
		Vomiting: 3 (2)
Ai et al[220], 2020	102	Anorexia: NA	15 (14.3)	3 (2.9)
		Nausea: 9 (8.8)
		Vomiting: 2 (2)
Zhao et al[221], 2020	75	NA	7 (9.3)	1 (1.3)
Li et al[222], 2020	83	NA	7 (8.4)	7 (8.4)
Lin et al[223], 2020	95	Anorexia: 17 (17.8)	23 (24.2)	2 (2.1)
		Nausea: 17 (17.9)
		Vomiting: 4 (4.2)
Cholankeril et al[224], 2020	207	Anorexia: NA	22 (10.8)	14 (7.1)
		Nausea: 22 (10.8)
		Vomiting: NA
Ferm et al[43], 2020	892	Anorexia: 105 (11.8)	177 (19.8)	70 (7.8)
		Nausea: 148 (16.6)
		Vomiting: 91 (10.2)
Redd et al[225], 2020	318	Anorexia: 110 (34.8)	107 (33.7)	46 (14.5)
		Nausea: 84 (26.4)
		Vomiting: 49 (15.4)
Kluytmans et al[226], 2020	86	NA	16 (18.6)	5 (5.8)

SARS-CoV-2: Severe acute respiratory syndrome coronavirus 2; NA: Not applicable; COVID-19: Coronavirus disease 2019.

Table 2 Therapy-specific considerations for inflammatory bowel disease patients

Drug	Effects
Aminosalicylate acid derivatives (5-ASA)	No proof of increased risk of COVID-19 infection
Aminosalicylate acid derivatives (5-ASA)	Continue treatment even in the case of COVID-19 infection
Corticosteroids	Their safety during COVID-19 infection is uncertain
	They can be used at a low dose and for a short period to treat disease relapses
	Discontinue as soon as possible
	Ileo-cecal CD patients can be treated with Budesonide; IUC patients can be treated with Budesonide MMX
Immunomodulators (Thiopurines and Methotrexate)	No proof of increased risk of COVID-19 infection
	Accompanied by increased risk of other viral infection
	Not recommended to start with monotherapy
	Combination therapy with biologics should be maintained
	Recommendations in stopping
	Stable disease
	Sustained reduction in the case of elderly patients and/or significant comorbidities
	Symptom progression of COVID-19 infection
Anti-TNF therapy	No proof of increased risk of COVID-19 infection
	Infusion and dose intervals should be maintained
	Starting with monotherapy (adalimumab or certolizumab)
	Stop in the case of developing symptoms of COVID-19
Anti-IL-12/23p40 therapy (Ustekinumab)	No proof of increased risk of COVID-19 infection
	Monotherapy is recommended
	Stop in the case of developing symptoms of COVID-19
Anti-a4b7 integrin therapy (Vedolizumab)	No proof of increased risk of COVID-19 infection
	Monotherapy is recommended
	Stop in the case of developing symptoms of COVID-19
Janus Kinase inhibitors (tofacitinib)	Although there is no proof of increasing the risk of COVID-19 infection, it may inhibit the immune reaction against viral infections
	Starting is not recommended
	Therapy should be maintained without elevating the dose
	Stop if symptoms of COVID-19 develop

UC: Ulcerative colitis; CD: Crohn’s disease; COVID-19: Coronavirus disease 2019; TNF: Tumor necrosis factor; IL: Interleukin.

Table 3 Incidence of hepatic abnormalities in patients with severe acute respiratory syndrome coronavirus 2 infection

Ref.	Patient number	ALT (U/L)	AST (U/L)	TB (mg/dL)
Zhou et al[32], 2020	191	↑59 (31%)	None	NA
Shu et al[227], 2021	545	↑41 (7.5%)	↑35 (10.1%)	↑189 (34.7%)
Huang et al[25], 2020	41	NA	↑15 (37%)	NA
Huang et al[228], 2020	36	4 (13.3%)	18 (58%)	↑4 (12.9%)
Chen et al[26], 2020	99	↑28 (28%)	↑35 (35%)	↑18 (18%)
Ai et al[64], 2020	102	↑20 (19.6%)	↑26 (25.5%)	NA
Xu et al[27], 2020	62	↑3 (3.75%)	↑3 (3.75%)	NA
Yang et al[3], 2020	168	↑9 (8%)	↑18 (17.3%)	↑7 (6.4%)
Wu et al[28], 2020	80	↑3 (3.75%)	↑3 (3.75%)	NA
Yao et al[229], 2020	40	↑21 (52.5%)	↑16 (40%)
Xu et al[230], 2020	355	↑91 (25.6%)	↑102 (28.7%)	↑10 (25%)
Cai et al[231], 2020	298	↑39 (13.1%)	↑25 (8.4%)	↑66 (18.6)
Richardson et al[1], 2020	5700	↑2176 (39.0%)	↑3263 (58.4%)	↑24 (8.1%)
Richardson et al[1], 2020	5700	↑2176 (39.0%)	↑3263 (58.4%)	NA
Fan et al[1], 2020	40	↑27 (18.2%)	↑32 (21.6%)	↑9 (6.1%)
Guan et al[39], 2020	355	↑158 (21.3%)	↑168 (22.2%)	↑76 (10.5%)

ALT: Alanine aminotransferase; AST: Aspartate aminotransferase; TB: Total bilirubin; NA: Not applicable.

Table 4 Outcome of the patients with severe elevation of aminotransferases in coronavirus disease 2019

Ref.	Outcome of patients	SARS-CoV-2 patients with hypertransaminasemia (n = 20)	COVID-19 patients without hypertransaminasemia (n = 125)	P value
Ramachandran et al[169], 2020	Shock	9 (45%)	38 (30.4%)	0.207
	Mechanical ventilation	10 (50%)	30 (24%)	0.028
	Died	10 (50%)	46 (36.8%)	0.324
	Length of stay in days, median (IQR)	7 (4.3, 10.3)	7 (5, 10)	0.78

SARS-CoV-2: Severe acute respiratory syndrome coronavirus 2; IQR: Inter-quartile; COVID-19: Coronavirus disease 2019.

Table 5 Recommendations of the American Association for the Study of Liver Diseases, Asian Pacific Association for the Study of the Liver, and European Association for the Study of the Liver for management of liver disease during coronavirus disease 2019

	Selected recommendations
To limit nosocomial spread	(1) Decrease in-person visits via other alternatives such as virtual platforms
	(2) Symptom investigation before entering hospitals to identify COVID-19 patients
	(3) Reduce staffing to essential staff only
	(4) Reduce the frequency of screening and laboratory examinations
	(5) Adhere to recommended PPE by HCW and patients
	(6) Maintain proper social distancing in hospitals
	(7) Postpone unnecessary or elective operations
Management of CLD patients with COVID-19	(1) These patients should be admitted to hospital early
	(2) Prioritization of COVID-19 testing for patients with cirrhosis, CLD patients taking immunosuppressive agents and acute decompensated patients
	(3) Repeated LFTs are advisable
	(4) Early registration in clinical trials as much as possible
	(5) COVID-19 patients with NAFLD should be kept under supervision
	(6) Screening of hepatitis B surface antigen should be taken into consideration
	(7) Drug-induced liver injury should be monitored
	(8) These patients can receive 2-3 g/d of acetaminophen, while limiting the use of NSAIDs when possible
	(9) HBV prophylaxis should be considered before starting immunosuppressive agents
	(10) Stopping Remdesivir in decompensated liver disease patients with ALT more than 5 times the upper limit of normal
Management of chronic viral hepatitis (HCV and HBV)	(1) Despite COVID-19 status, treatment continuity of chronic HCV and HBV is recommended
	(2) In the absence of flare, HBV treatment should be stopped
	(3) For uninfected individuals, HCV and HBV treatment should be continued according to guidelines
Management of HCC	(1) HCC treatment should be continued according to guidelines; however, it can be delayed if necessary
	(2) In the case of COVID-19 patients, delaying elective transplants and resection surgery, and stopping immunotherapy are advisable
	(3) Early admission to hospital is recommended for HCC patients
Management of pre- and post-transplant recipients	(1) Screening donor and recipient for COVID-19 is suggested
	(2) For donors testing positive for COVID-19, transplantation surgery should be postponed
	(3) Prioritization of patients with short-term prognosis
	(4) For post-transplant patients, a reduction in immunosuppressive dose can be considered for moderate COVID-19 cases, while for mild COVID-19 cases, the dose should not be reduced
	(5) For post-transplant recipients, vaccination against pneumonia and influenza is advisable

PPE: Personal protective equipment; HCWs: Healthcare workers; CLD: Chronic liver disease; COVID-19: Coronavirus disease 2019; LFTs: Liver function tests; NAFLD: Nonalcoholic fatty liver disease; NSAIDs: Non-steroidal anti-inflammatory drugs; HBV: Hepatitis B virus; ALT: Alanine aminotransferase; HCV: Hepatitis C virus; HCC: Hepatocellular carcinoma.

Table 6 Recommendations of the American Association for the Study of Liver Diseases and European Association for the Study of the Liver for the management of auto-immune hepatitis during coronavirus disease 2019

	Selected recommendations
Virtual platforms are recommended to minimize in-person visits as much as possible
COVID-19 testing is advised in cases of acute deterioration and liver failure
Patients with low risk of complications (patients on chronic immunosuppressive therapy)	(1) Frequent patient-provider communications should be closely supervised; (2) Virtual platforms should be used to decrease contact; and (3) Ensure enough drug supply and refills to decrease running out of medications
Patients with moderate risk of complications (symptomatic disease without cirrhosis)	(1) Empiric therapy via virtual healthcare platforms as much as possible; and (2) Preventing liver biopsy whenever possible
Patients with high risk of complications (acute flare, decompensated cirrhosis)	(1) Reduce invasive procedures as much as possible; (2) In the case of COVID-19 patients, if lymphopenia develops, dose reduction of antimetabolites is recommended; and (3) In the case of infection, corticosteroids should be attenuated

COVID-19: Coronavirus disease 2019.

Table 7 Recommendations of the American Association for the Study of Liver Diseases and European Association for the Study of the Liver on the use of immunosuppressive therapies in chronic liver disease during coronavirus disease 2019

	Suggestions
(1) Starting with corticosteroids and immunomodulators should proceed; and (2) Risk benefit ratio assessments should be carried out
Patients on immunosuppressive treatment and not infected with COVID-19	Decreases or adjustment of doses is not advisable
Patients infected with COVID-19 on immunosuppressive drugs	(1) Reduce corticosteroids dose after specialist physician (consider tapering to prevent adrenal insufficiency); and (2) Decreasing the doses of cyclosporine, mycophenolate, and azathioprine is recommended in severe COVID-19 (especially patients with lymphopenia)
Patients requiring initiation of immunosuppressive agents	Starting treatment is suggested in these patients regardless of COVID-19 status

COVID-19: Coronavirus disease 2019.

Citation: Mohamed DZ, Ghoneim MES, Abu-Risha SES, Abdelsalam RA, Farag MA. Gastrointestinal and hepatic diseases during the COVID-19 pandemic: Manifestations, mechanism and management. World J Gastroenterol 2021; 27(28): 4504-4535
URL: https://www.wjgnet.com/1007-9327/full/v27/i28/4504.htm
DOI: https://dx.doi.org/10.3748/wjg.v27.i28.4504