| Literature DB >> 36187753 |
Pawan Kumar Thada1, Fateen Ata2, Muhammad Ali1, Mohammad Nasser Affas2, Jenish Bhandari3, Sarosh Sarwar4, Bilal Ahmed5, Hassan Choudry6.
Abstract
INTRODUCTION: Severe acute respiratory syndrome-coronavirus 2 (SARSCoV2) pandemic has been an unceasing plight with a wide range of clinical presentations. The direct effects of the virus, increased use of medications, and lifestyle changes have contributed to the vulnerability to co-infections. Fungal and bacterial co-infections led to increased morbidity and mortality during the pandemic. Similarly, the surge of skin signs in conjunction with herpes zoster (HZ) manifestations has been reported. In this study, we pooled the data on the clinical characteristics of SARS-CoV-2 patients co-infected with HZ.Entities:
Keywords: COVID-19; Coronavirus; Herpes zoster; SARS-CoV-2; Varicella zoster virus; vesicular rash; virus reactivation
Year: 2022 PMID: 36187753 PMCID: PMC9483766 DOI: 10.5339/qmj.2022.41
Source DB: PubMed Journal: Qatar Med J ISSN: 0253-8253
Figure 1.PRISMA flow chart of the study selection process, including the added and excluded studies with details.
Summary of the patients with herpes zoster and COVID-19
| Characteristics | Results (n = 12) | |
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| Mean Age (Years) | Mean: 53.97 ± 18.91 | |
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| Age | < 20 years | 3 (3.8%) |
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| groups | 20–44 years | 15 (19%) |
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| 45–54 years | 15 (19%) | |
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| 55–64 years | 20 (25.31%) | |
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| 65–74 years | 18 (22.78%) | |
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| >75 years | 8 (10.1%) | |
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| Gender | Males: 46 (58.2%) Females: 33 (41.8%) | |
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| Clinical | fever | 39 (49.4%) |
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| features | cough | 27 (34.2%) |
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| dyspnea | 13 (16.5%) | |
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| myalgias | 13 (16.5%) | |
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| Loss of taste, smell | 12 (15.2%) | |
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| Sore throat | 10 (12.7%) | |
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| fatigue | 4 (5.1%) | |
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| diarrhea | 4 (5.1%) | |
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| Nasal congestion | 1 (1.3%) | |
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| vomiting | 1 (1.3%) | |
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| Chest pain | 1 (1.3%) | |
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| Loss of consciousness | 2 (2.5%) | |
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Summary of the reported comorbidities of the patients
| Previous Medical History | Frequency | Percent |
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| HTN | 11 | 13.9% |
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| History of Chicken Pox | 9 | 11.4% |
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| History of Herpes Zoster in the past | 5 | 6.3% |
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| Recurrent infections | 4 | 5.1% |
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| Diabetes Mellitus | 4 | 5.1% |
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| Immunodeficiency | 3 | 3.8% |
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| Chronic Kidney Disease | 3 | 3.8% |
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| Malignancy | 1 | 1.3% |
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| Lung Disease | 1 | 1.3% |
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Summary of the clinical course for symptoms development and diagnosis
| Characteristics | N | Median | Mean | Std |
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| Duration of Symptoms before admission (days) | 29 | 5 | 9.52 | 10.33 |
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| Duration from herpes zoster to COVID-19 diagnosis (days) | 15 | 0 | 2.72 | 4.25 |
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| Duration from first COVID symptoms to herpes zoster diagnosis (days) | 43 | 7 | 15.49 | 16.99 |
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| Duration from COVID-19 diagnosis to herpes zoster diagnosis (days) | 44 | 6.50 | 14.80 | 17.03 |
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| Hospital stays (days) | 3 | 32 | 49 | 44.03 |
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Distribution of HZ rash and treatment of patients added to the review
| Author | Age/sex | No. of patients | Location of rash | Treatment |
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| GHOSH B et al | 26 yr. /M | 1 | Thoracic -abdomen tbl11-T12 dermatome | Oral Acyclovir, supportive management |
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| Desai et al | 62 yr./F | 1 | T11, tbl12 | IV Acyclovir, amitriptyline, pregabalin |
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| Kondo et al | 57 yr./M | 1 | Located on the right side of the forehead in the first division of the trigeminal nerve | NA |
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| Gupta et al | 75 yr./F | 1 | NA | Oral valganciclovir, valaciclovir |
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| Xu et al | 73 yr. /M | 1 | Shoulder and neck | IV Acyclovir and supportive management |
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| Fernandez-Nieto et al | 56 yr./M,52 yr. /M,63 yr./ M,56 yr./F,82 yr./F,72 yr./F,78 yr./F | 7 | Ophthalmic in 2/ NA in others | Valacyclovir in 3 cases and NA in others |
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| Karimi et al | 12 yr. /M | 1 | Trunk. face and limbs | Acyclovir, acetaminophen |
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| Ferreira et al | 39 yr. /M | 1 | Left orofacial | Acyclovir, pregabalin |
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| Patel et al | 83 yr./M | 1 | NA | IV Acyclovir |
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| Maldonado et al | 25 yr./F | 1 | Right lumbar and right hand and leg | paracetamol, calamine lotion |
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| Mar Llamas-Velasco | 79 yr. /F | 1 | Anterior posterior trunk | NA |
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| Puri et al | 83 yr./M | 1 | NA | IV Acyclovir |
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| Goyal et al | 50 yr./M,60 yr./M | 2 | Right shoulder and back, left trunk | Acyclovir, topical fusidic acid cream |
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| Voisin et al | 80 yr./F | 1 | Chonca and external auditory canal | NA |
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| Solanki et al | 64 yr./M | 1 | Face bilateral, upper extremity | IV Valacyclovir |
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| Katz et al | 10 F,6 M | 16 | NA | NA |
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| Elsaie et al | 44 yr. /M | 1 | Front chest | Valacyclovir |
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| Cao et al | 70 yr./F | 1 | Right tbl10-T12 | IV Acyclovir, pregabalin, ibuprofen |
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| Shors et al | 49 yr./F | 1 | FACE trigeminal V2 | Valacyclovir, gabapentin. Topical lidocaine |
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| Pona et al | 70 yr. /F | 1 | left hip | Gabapentin |
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| Saati et al | 54 yr./M | 1 | right chest and tip of the scapula | Famciclovir, acetaminophen |
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| Altaf et al | 52 yr,75 yr,34 yr./all male | 3 | RIGHT SIDE OF NECK AND UPPER CHEST, right side of the chest, right tbl8 | Oral acyclovir, prednisolone, calamine |
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| Veraldi et al | 48 yr./M | 1 | bilateral asymmetric dermatome | Valaciclovir, citalopram |
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Summary of commonly reported medications used for COVID-19 and herpes zoster
| Medications | Frequency | Percent |
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| For COVID-19 | ||
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| Hydroxychloroquine/chloroquine | 14 | 17.8% |
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| Antibiotics | 8 | 10.1% |
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| Remdesivir | 3 | 3.8% |
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| Oseltamivir | 3 | 3.8% |
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| AC (Enoxaparin/Heparin) | 3 | 3.8% |
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| Steroids | 2 | 2.5% |
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| Favipiravir | 2 | 2.5% |
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| Tocilizumab | 2 | 2.5% |
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| Ritonavir/Lopinavir | 1 | 1.3% |
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| For Herpes Zoster | ||
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| Acyclovir | 42 | 53.2% |
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| Valacyclovir | 15 | 18.98% |
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| Steroids (Dexamethasone, Prednisolone, Methylprednisolone) | 11 | 13.9% |
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| Calamine lotion | 5 | 6.32% |
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| Famciclovir | 2 | 2.5% |
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Patient's laboratory investigations in the early (first week) and late disease (second week) periods
| Parameters | Early Disease (Day 1) | Late Disease (Day 14) |
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| Hemoglobin (mg/dl) | 10.1 | 10.6 |
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| Leukocyte Count (per mm3) | 11650 | 13900 |
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| Lymphocytes | 19% | 4% |
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| Platelets (per mm3) | 195000 | 181000 |
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| D-Dimer (ng/ml) | 783 | 1399 |
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| Ferritin (ng/ml)) | 398 | 12 |
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| CRP (mg/dl) | 48 | 22 |
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| Lactate Dehydrogenase (u/l) | 758 | 620 |
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Figure 2.Proposed pathophysiology of SARS-CoV-2-led immunosuppression that might be the potential trigger of co-infections.