| Literature DB >> 34054961 |
Shahroo Etemad-Moghadam1, Mojgan Alaeddini1.
Abstract
The pathogenic mechanism of SARS-CoV-2 infection is unclear, and its symptoms vary in different patients. Initial reports of COVID-19 concentrated on pulmonary issues, but with time, additional features such as hyposmia/anosmia, dysgeusia, and skin lesions were added to the list of COVID-19 symptoms. There have been an increasing number of reports on oral cavity lesions in individuals with COVID-19, which might be relevant considering that this location is one of the first sites coming into contact with the virus and that it contains the SARS-CoV-2 receptor. We hereby aim to familiarize practicing head and neck clinicians with the range of oral lesions reported in COVID-19 patients and to critically appraise the most recent data on the role of SARS-CoV-2 in these lesions. We also discuss the ongoing debate on the direct/indirect association of oral symptoms with the disease. COVID-19 cases with simultaneous oral symptoms were extracted from the literature, and articles discussing the role of SARS-CoV-2 in oral lesions were compiled and methodically analyzed. We found approximately 95 COVID-19 patients with a wide range of oral lesions. Based on current evidence, the exact role of SARS-CoV-2 in the development of oral lesions remains unclear. Oral examination of patients is needed to provide adequate cases for analysis to clarify unknown problems related to COVID-19. There is evidence to support both the direct and indirect roles of SARS-CoV-2 in the development of oral lesions. Awareness of the possibility of oral manifestations in COVID-19 is important to clarify the range of disease signs and symptoms.Entities:
Year: 2021 PMID: 34054961 PMCID: PMC8136299 DOI: 10.1155/2021/6648082
Source DB: PubMed Journal: Int J Dent ISSN: 1687-8728
Reported oral findings in COVID-19 patients, including cases with reactivation of previous infections∗.
| Authors/date of submission (2020) | Basis of diagnosis | Sex | Age (y) | Underlying disease s | General/extraoral symptoms | Chief complaint | Oral manifestation | Outcome | Additional information | |
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| Chaux-Bodard et al./April 11 [ | Nasopharyngeal swab on day 8 | F | 45 | NS | (i) Erythematous painful toe lesion, 3 d after oral lesion, painful for 2 d | 1 d painful inflamed lingual papilla, 1 d red macula, and finally asymptomatic tongue ulcer | (i) Complete healing after 10 d | (i) COVID-19 vasculitis could be responsible for oral macule | ||
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| Martín Carreras-Presas et al./April 20 [ | Bilateral pneumonia | F | 65 | Obesity and hypertension, took diuretics and ACE inhibitor | (i) High fever, diarrhea, bilateral pneumonia | (i) Tongue pain from the beginning | Ex: blisters on internal labial mucosa and desquamative gingivitis 30 d later | Improvement within 3 d after treatment with mouthwash and prednisolone | Biopsy: some criteria suggestive of viral exanthema or urticarial dermatitis with discrete blood extravasation | |
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| Putra et al./April 11 [ | Oropharyngeal and nasopharyngeal swab, PCR (day 3 of symptoms) | M | 29 | None | (i) Fever, sore throat, back pain, myalgia, dry cough, 1st-3rd days | General symptoms | (i) Aphthous stomatitis, day 7 | (i) Skin lesions on day 6 of symptoms, darkening on day 7 | Hand, foot, and mouth disease was rejected based on clinical manifestations and age | |
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| Hedou et al./April 21 (accepted) [ | Nasopharyngeal PCR | NS | Respiratory problems leading to intubation | NS | Oral HSV-1 reactivation during illness | Patient alive | Admitted to intensive care | |||
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| Galván Casas et al./April 28 (accepted) [ | Lab confirmation | M | NS | Maculopapular eruptions, other symptoms NS | NS | Desquamative gingivitis-like lesions, petechiae on the lower lip, and erythema on the palate | NS | Appearance of oral lesions is described based on the images provided by the authors and not the authors' statements | ||
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| Sakaida et al. /April 29 [ | PCR negative 8 d after oral/skin lesions, turned positive 11 d after oral/skin lesions | F | 52 | NS | Initially had erythematous skin/oral lesions but after 8 d developed high fever, cough, chills, fatigue, dyspnea, WBC and CRP, lymphopenia, neutrophilia, and opacity in lower lung lobes on CT | Itchy erythema on limbs, erosions on lips, and buccal mucosa | Erosions on lips and buccal mucosa 2 d after antibiotic and NSAID | Transferred to an intensive care unit in another hospital | Skin biopsy showed deep lymphocytic infiltrations, which are not typical in drug eruptions | |
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| Jimenez-Cauhe et al./May 5 (accepted) [ | NS | F | 58–77 | NS | Erythema multiforme skin lesions | NS | Palatal macules and petechiae | 2-3 w after corticosteroid treatment | In at least 2 of them, skin rashes appeared after discharge and their CRP, D-dimer, and lymphocyte count worsened; at least one of them was negative for infectious diseases | |
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| Aghazadeh et al./May 7 (received) [ | Nasopharyngeal swab RT-PCR | F | 9 | None | (i) Weakness, loss of appetite, fever, abdominal pain, diarrhea, and red edematous papules and plaques on dorsal hands and feet | Malaise and oral/skin eruptions | Ex: vesicles, erosions, and herpetiform eruptions on lips, anterior tongue, and buccal mucosa | General symptoms improved in a few weeks, mucocutaneous eruption resolved in about a week | (i) HFMD was rejected due to acral eruption | |
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| Ansari et al./May 11 [ | Nasopharyngeal swab PCR | F | 56 | Diabetes mellitus | Fever and dyspnea | Sores in the mouth on 5th day of general symptoms | Ex: multiple painful ulcers on red nonbleeding background on the entire hard palate | Healing 1 w later, no scarring | (i) Negative HSV1/2 AB | |
| Nasopharyngeal swab PCR | M | 75 | Hypertension | Hypoxia upon admission | Dysphasia 1 w after admission | Ex: multiple painful ulcers on red nonbleeding background the on anterior tongue | ||||
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| Askin et al./May 14 [ | RT-PCR or chest CT | NS | NS | Ex: enanthema and aphthous stomatitis | NS | |||||
| M | Ex: aphthous stomatitis on lateral tongue | |||||||||
| NS | Ex: rash and enanthema | |||||||||
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| Llamas-Velasco et al./May 20 (available online) [ | Nasopharyngeal swab | F | 59 | None | Fever, dry cough, dyspnea, bilateral interstitial pneumonia | NS | Vesicles and punched out perioral erosions | NS | Combination of HSV-1, HSV-6, and EBV based on a herpesvirus family microarray PCR of the vesicle fluid | |
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| Fernandez-Nieto et al./May 27 (received date) [ | Nasopharyngeal swab for SARS-CoV-2 | M | 69 | None | Bilateral interstitial pneumonia (ICU admittance) | NS | Orolabial recurrent herpes simplex | NS | Vesicular content: HSV-1 + (multiplex herpes PCR), SARS-CoV-2-(RT-PCR) | |
| F | 96 | Hypertension, chronic kidney disease, hyperuricemia | Bilateral interstitial pneumonia | Vesicular content: HSV-1 + (multiplex herpes PCR), SARS-CoV-2-(RT-PCR) | ||||||
| F | 77 | Primary biliary cholangitis, Alzheimer | Bilateral interstitial pneumonia | Vesicular content: HSV-1 + (multiplex herpes PCR) | ||||||
| M | 65 | Hypertension, dyslipidemia | Bilateral interstitial pneumonia (ICU admittance) | Vesicular content: HSV-1 + (multiplex herpes PCR) | ||||||
| M | 38 | Colorectal cancer with chemotherapy | Bilateral interstitial pneumonia | Vesicular content: HSV-1 + (multiplex herpes PCR) | ||||||
| M | 61 | None | Bilateral interstitial pneumonia (ICU admittance) | Vesicular content: HSV-1 + (multiplex herpes PCR) | ||||||
| F | 45 | None | Bilateral interstitial pneumonia | |||||||
| M | 76 | Hypertension, dyslipidemia | Bilateral interstitial pneumonia | |||||||
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| Amorim Dos Santos et al./May 29 [ | Nasopharyngeal swab, RT-PCR | M | 67 | Revascularized respiratory disease, hypertension, ADPKD, and kidney transplant | (i) Respiratory symptoms, progressive dyspnea on exertion, fever, and diarrhea (10 d before admission) | General symptoms and hypogeusia (admission) | Ex: viscous saliva, persistent white plaque, and pinpoint yellowish ulcers on dorsal tongue similar to late-stage herpetic recurrent lesions | (i) Lingual white plaque remained after oral nystatin and IV fluconazole in the hospital | (i) Received supplemental O2 and orotracheal intubation | |
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| Soares et al./June 2 [ | PCR | M | 42 | Diabetes and hypertension | (i) Fever, cough, shortness of breath | Painful ulceration in buccal mucosa | Ex: ulcerations and multiple reddish macules scattered throughout the hard palate, tongue, and lips | Complete resolution of oral lesions after 3 w | Biopsy: epithelial vacuolization, chronic inflammation, focal necrosis, hemorrhage, vessel thrombi, and CD3+ and CD8+ infiltration of minor salivary glands | |
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| Ciccarese et al./June 2 [ | Nasopharyngeal swab, RT-PCR | F | 19 | None | (i) Ex: afebrile, red macules, papules, and petechiae on lower extremities | Fever/sore throat for 7 d, fatigue, hyposmia, and skin/oral/pharyngeal lesions (day 5) | Ex: erosions, ulcerations, and hemorrhagic crusts on labial mucosae | (i) Regression of systemic lesions, day 5 after treatment | (i) Thrombocytopenia seen from initial stages—petechial lesions probably due to severe thrombocytopenia, triggered by SARS‐CoV‐2, worsened by cefixime | |
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| Cebeci Kahraman and Çaşkurlu/June 4 [ | 2 positive rapid COVID-19 IgM tests 1 d apart | M | 51 | None | (i) Fever, fatigue, dry cough, sore throat, and taste and smell issues | Sore throat, which worsened 10 d after symptom onset | (i) Ex: erythema on oropharynx and hard palate, midline petechiae, soft palate pustular enanthema (border) | Resolved after a few days of antibiotic therapy | (i) COVID-19 IgM+ and IgG+ after 2 w, | |
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| Tomo et al./July 2 (received) [ | Nasopharyngeal swab, PCR | F | 37 | None | Fever, asthenia, anosmia | Worsening of dysgeusia, burning tongue, and dry mouth on day 9 | (i) Dysgeusia, burning tongue, and dry mouth for 3 d | Symptomless. 2 w after COVID-19 onset and treatments | ||
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| Cant et al./July 3 (published online) [ | NS | M | 9 | Severe dystonia and epilepsy | Fever, malaise, and GI upset | Swollen lip and oral ulcer 2nd time in 2 w, each followed by fever, malaise, and GI upset | Swollen lip and oral ulcerations | Improvement 3 d after hydrocortisone treatment | (i) Eight other children with the same oral lesions before pediatric multisystem inflammatory syndrome associated with COVID-19, in the same unit | |
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| Díaz Rodríguez et al./July 22 (accepted manuscript) [ | PCR | F | 43 | NS | Fever, malaise, dysgeusia, anosmia, diarrhea, pneumonia, risk of thrombosis, based on lab test | Aphthous-like lesions, burning sensation | Photograph: aphthous-like lesions, progressive tongue depapillation | Disappearance of ulcers and burning 10 d after triamcinolone rinse but not the depapillation | ||
| Positive for SARS-CoV-2, method not specified | M | 53 | Hospital admission | Burning mouth, unilateral commissural fissures, anosmia, and dysgeusia | Ex: commissural cheilitis | Angular cheilitis, but not anosmia and dysgeusia, disappeared after antibiotics, nystatin, and hygiene measure | Oral manifestations were found few days after hospital discharge | |||
| Positive for SARS-CoV-2, method not specified | F | 78 | NS | Hospital admission | Dry mouth sensation | Ex: angular cheilitis and pseudomembranous candidiasis-like lesions on tongue, palate, and lip commissure | Angular cheilitis and pseudomembranous lesions disappeared after nystatin and antibiotics, dry mouth improved after solutions/gels prescription | Symptoms appeared since hospitalization | ||
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| Glavina et al./August 9 (accepted online) [ | PCR | F | 40 | Frequent recurrent herpes labialis eruption | Weakness, fever, and acute loss of taste | Malaise, fever, ageusia, oral pain,andburning7 d after diagnosis | Telemedically: recurrent palatal HSV, white hairy tongue, nonspecific white lateral tongue lesion | Healing after 3 w and double-negative PCR | ||
NS: not specified; d: day; ACE: angiotensin-converting enzyme; w: week; Ex: examination; WBC: white blood cell; CRP: C-reactive protein; CT: computerized tomography; NSAID: nonsteroid anti-inflammatory drug; HSV-1/HSV-2: herpes simplex virus 1 and 2; AB: antibody; EBV: Epstein–Barr virus; LAP: lymphadenopathy; ADPKD: autosomal dominant polycystic kidney disease; ICU: intensive care unit; GI: gastrointestinal; HFMD: hand, foot, and mouth disease. ∗A total of 53 COVID-19 hospitalized patients were reported to have oropharyngeal candidiasis, without detailed information for each individual patient [25].