Neurological symptoms and comorbidity profile of hospitalized patients with COVID-19

Cremaschi, Renata Carvalho; Bahi, Carla Alessandra Scorza; Paola, Angelo Amato Vincenzo de; Arakaki, Jaquelina Sonoe Ota; Ferreira, Paulo Roberto Abrão; Bellei, Nancy Cristina Junqueira; Borges, Vanderci; Coelho, Fernando Morgadinho Santos

doi:10.1055/s-0043-1761433

Abstract

Background

The neurological manifestations in COVID-19 adversely impact acute illness and post-disease quality of life. Limited data exist regarding the association of neurological symptoms and comorbid individuals.

Objective

To assess neurological symptoms in hospitalized patients with acute COVID-19 and multicomorbidities.

Methods

Between June 2020 and July 2020, inpatients aged 18 or older, with laboratory-confirmed COVID-19, admitted to the Hospital São Paulo (Federal University of São Paulo), a tertiary referral center for high complexity cases, were questioned about neurological symptoms. The Composite Autonomic Symptom Score 31 (COMPASS-31) questionnaire was used. The data were analyzed as a whole and whether subjective olfactory dysfunction was present or not.

Results

The mean age of the sample was 55 ± 15.12 years, and 58 patients were male. The neurological symptoms were mostly xerostomia (71%), ageusia/hypogeusia (50%), orthostatic intolerance (49%), anosmia/hyposmia (44%), myalgia (31%), dizziness (24%), xerophthalmia (20%), impaired consciousness (18%), and headache (16%). Furthermore, 91% of the patients had a premorbidity. The 44 patients with subjective olfactory dysfunction were more likely to have hypertension, diabetes, weakness, shortness of breath, ageusia/hypogeusia, dizziness, orthostatic intolerance, and xerophthalmia. The COMPASS-31 score was higher than that of previously published controls (14.85 ± 12.06 vs. 8.9 ± 8.7). The frequency of orthostatic intolerance was 49% in sample and 63.6% in those with subjective olfactory dysfunction (2.9-fold higher risk compared to those without).

Conclusion

A total of 80% of inpatients with multimorbidity and acute COVID-19 had neurological symptoms. Chemical sense and autonomic symptoms stood out. Orthostatic intolerance occurred in around two-thirds of the patients with anosmia/hyposmia. Hypertension and diabetes were common, mainly in those with anosmia/hyposmia.

Keywords:
COVID-19; Neurologic Manifestations; Comorbidity; Anosmia; Orthostatic Intolerance; Autonomic Nervous System Diseases

Resumo

Antecedentes

As manifestações neurológicas na COVID-19 impactam adversamente na enfermidade aguda e na qualidade de vida após a doença. Dados limitados existem em relação a associação de sintomas neurológicos e indivíduos com comorbidades.

Objetivo

Avaliar os sintomas neurológicos em pacientes de hospitalizados com COVID-19 aguda e múltiplas comorbidades.

Métodos

Entre junho e julho de 2020, pacientes de hospitais com idade 18 anos ou acima e COVID-19 laboratorialmente confirmada, admitidos no Hospital São Paulo (Universidade Federal de São Paulo), um centro de referência terciário para casos de alta complexidade, foram perguntados sobre sintomas neurológicos. O questionário Pontuação composta de sintoma autonômico (COMPASS-31) foi usado. Os dados foram analisados no geral e se a disfunção olfatória subjetiva estava presente ou não.

Resultados

A média de idade da amostra foi 55 ± 15.12 anos. 58 pacientes eram homens. Os sintomas neurológicos foram principalmente xerostomia (71%), ageusia/hipogeusia (50%), intolerância ortostática (49%), anosmia/hiposmia (44%), mialgia (31%), tontura (24%), xeroftalmia (20%), comprometimento na consciência (18%) e cefaleia (16%). Além disso, 91 % dos pacientes tinham uma pré-morbidade. Os 44 pacientes com disfunção olfatória tinham maior chance de ter hipertensão, diabetes, fraqueza, falta de ar, ageusia/hipogeusia, tontura, intolerância ortostática e xeroftalmia. A pontuação do COMPASS-31 foi maior do que a de controles previamente publicados (14,85 ± 12,06 vs. 8,9 ± 8,7). A frequência de intolerância ortostática foi 49% na amostra e 63,6% naqueles com disfunção olfatória subjetiva (risco 2.9 vezes maior comparado com os sem).

Conclusão

Um total de 80% dos pacientes hospitalizados com múltiplas morbidades e COVID-19 aguda tinham sintomas neurológicos. Os sintomas do sentido químico e autonômicos se destacaram. A intolerância ortostática ocorreu em cerca de dois terços dos pacientes com anosmia/hiposmia. A hipertensão e o diabetes foram comuns, principalmente naqueles com anosmia/hiposmia.

Palavras-chave:
COVID-19; Manifestações Neurológicas; Comorbidade; Anosmia; Intolerância Ortostática; Doenças do Sistema Nervoso Autônomo

INTRODUCTION

The novel severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) binds mainly to the angiotensin-converting enzyme type 2 (ACE2) receptor in the olfactory and respiratory epithelium. The virus’s interaction can cause anosmia/hyposmia. Because ACE2-expressing cells are widely distributed, the SARS-CoV-2 reaches extrapulmonary sites as well.¹1 Yachou Y, El Idrissi A, Belapasov V, Ait Benali S. Neuroinvasion, neurotropic, and neuroinflammatory events of SARS-CoV-2: understanding the neurological manifestations in COVID-19 patients. Neurol Sci 2020;41(10):2657-2669

The neurological manifestations were early linked to the coronavirus disease 2019 (COVID-19).²2 Mao L, Jin H, Wang M, et al. Neurologic Manifestations of Hospitalized Patients With Coronavirus Disease 2019 in Wuhan, China. JAMA Neurol 2020;77(06):683-690 The pathophysiology is related to immune activation, neuroinflammation, and damage to brains blood vessels.³3 Iadecola C, Anrather J, Kamel H. Effects of COVID-19 on the Nervous System. Cell 2020;183(01):16-27.e1 Anosmia was associated with low in-hospital mortality.⁴4 Sampaio Rocha-Filho PA, Magalhães JE, Fernandes Silva D, et al. Neurological manifestations as prognostic factors in COVID-19: a retrospective cohort study. Acta Neurol Belg 2022;122(03):725-733,⁵5 Amanat M, Rezaei N, Roozbeh M, et al. Neurological manifestations as the predictors of severity and mortality in hospitalized individuals with COVID-19: a multicenter prospective clinical study. BMC Neurol 2021;21(01):116 Although chemosensory symptoms are primary presentations of neurological features in COVID-19, a broad spectrum of other neurological symptoms accompany them. A sizeable proportion of the patients with anosmia have headache, and others develop mild-to-severe complications, including life-threatening cerebrovascular events.⁶6 Rocha-Filho PAS, Magalhães JE. Headache associated with COVID-19: Frequency, characteristics and association with anosmia and ageusia. Cephalalgia 2020;40(13):1443-1451,⁷7 Lechien JR, Chiesa-Estomba CM, De Siati DR, et al. Olfactory and gustatory dysfunctions as a clinical presentation of mild-to-moderate forms of the coronavirus disease (COVID-19): a multicenter European study. Eur Arch Otorhinolaryngol 2020;277(08):2251-2261

A few symptoms of the illness overlap with the symptoms of autonomic dysfunction. Particularly in the early stages of COVID-19, syncope and silent hypoxemia are the clinical presentations of autonomic impairment, which could be associated with the intrinsic mechanism of the viral infection or other non-COVID causes.⁸8 Baker J, Incognito AV, Wilson RJA, Raj SR. Syncope and silent hypoxemia in COVID-19: Implications for the autonomic field. Auton Neurosci 2021;235:102842 Some patients in recovery have experienced long-term autonomic symptoms, which are reported in long-COVID.⁹9 Buoite Stella A, Furlanis G, Frezza NA, Valentinotti R, Ajcevic M, Manganotti P. Autonomic dysfunction in post-COVID patients with and witfhout neurological symptoms: a prospective multidomain observational study. J Neurol 2022;269(02):587-596,¹⁰10 Dani M, Dirksen A, Taraborrelli P, et al. Autonomic dysfunction in ‘long COVID’: rationale, physiology and management strategies. Clin Med (Lond) 2021;21(01):e63-e67 Cardiovascular autonomic dysfunction was confirmed.¹¹11 Milovanovic B, Djajic V, Bajic D, et al. Assessment of Autonomic Nervous System Dysfunction in the Early Phase of Infection With SARS-CoV-2 Virus. Front Neurosci 2021;15:640835 Dysautonomia was overlooked in critically ill COVID-19 patients.¹²12 Eshak N, Abdelnabi M, Ball S, et al. Dysautonomia: An Overlooked Neurological Manifestation in a Critically ill COVID-19 Patient. Am J Med Sci 2020;360(04):427-429

The studies evaluating COVID-related neurological manifestations are heterogeneous, because they include symptoms and complications. The association between high-risk preexisting comorbidities for COVID-19 hospitalization and related deaths has been established in the literature.¹³13 Atkins JL, Masoli JAH, Delgado J, et al. Preexisting Comorbidities Predicting COVID-19 and Mortality in the UK Biobank Community Cohort. J Gerontol A Biol Sci Med Sci 2020;75(11):2224-2230 About 43.9% of the patients with COVID-19 and neurological symptoms have comorbid conditions.¹⁴14 Vakili K, Fathi M, Hajiesmaeili M, et al. Neurological Symptoms, Comorbidities, and Complications of COVID-19: A Literature Review and Meta-Analysis of Observational Studies. Eur Neurol 2021;84(05):307-324 The impact of morbidities in the neurological symptoms of COVID-19, especially those with a strong ACE2 receptor expression that enhances the viral entry into the host cells, has not been well emphasized.

Even though anosmia/hyposmia is one of the most frequent neurological symptoms observed, not much is known regarding the differences of the other neurological symptoms and the preexisting diseases in patients, regardless of whether subjective olfactory impairment is present or not. This study investigates inpatients with multiple comorbidities from a public reference hospital of Sao Paulo, in the course of the initial outbreak of the pandemic. The objectives were to assess the frequency of neurological symptoms in patients hospitalized for the treatment of COVID-19. We also evaluated the association between subjective anosmia/hyposmia and other neurological symptoms or comorbidities.

METHODS

Standard protocol approval and patient consent

The University’s Institutional Ethics Committee (Comitê de Ética em Pesquisa da Universidade Federal de São Paulo) approved the study, with the ethics board approval number 0547/2020. All participants in the study provided written informed consent for the research.

Study design and sample

This cross-sectional study describes neurological symptoms in patients admitted to a public tertiary referral center for high complexity cases, which turned into a COVID-19 care center. The study was conducted at the São Paulo Hospital, from the Federal University of Sao Paulo (Brazil).

The inclusion criteria were symptomatic patients aged 18 or older, with diagnostic confirmation of SARS-CoV-2 infection by nasopharyngeal swab reverse-transcriptase polymerase chainreaction(RT-PCR). The exclusion criteria were pregnancy or puerperium, dementia as a premorbidity, assessment during mechanical ventilation, or hemodynamic instability. The sampling method was noncasual and convenient, intended to represent a sample of real-life inpatients.

Data acquisition

The hospital capacity was organized to treat COVID-19 patients separately. The occupancy rates were high, but an exact overall value was in accurate. All patients sited at the infectious diseases and pneumology units (48 beds available) were invited to participate, between June 2020 and July 2020. Data collection was performed once a week, during five consecutive weeks. Before recruitment, the assistant physician confirmed the stable clinical condition of each patient, enabling them to join in the research. Two expert neurologists (FMSC, RMCC) interviewed the patients to fill out electronic forms with answers on the experienced symptoms. The completion of all items was checked before sending them for data processing. Clinical data were retrieved manually from electronic medical charts. The reported medications comprised those in use before admission.

According to the manufacturer’s protocols, all quantitative RT-PCR analyses were made in a single laboratory located at the hospital. Additionally, RNA was isolated from the subject’s nasopharyngeal swabs using the Quick-RNA Viral Kit (Zymo Research, Irvine, CA, USA). After extraction, the samples were tested for SARS-CoV-2 using a multiplex RT-PCR commercial kit (Gene Finder, South Korea). Early in the first wave of COVID-19, the identification of the variants was not yet implemented. Different commercially available kits were used in the samples of subjects who had been initially diagnosed at other hospitals. At admission, the degree of radiological involvement was confirmed using chest computed tomography to identify the typical ground-glass opacities extension.

Main outcome measure

Neurological symptoms

As there was no standardized measure of neurological symptoms in COVID-19, a survey was created, based on those of the initial report in China.²2 Mao L, Jin H, Wang M, et al. Neurologic Manifestations of Hospitalized Patients With Coronavirus Disease 2019 in Wuhan, China. JAMA Neurol 2020;77(06):683-690 The Composite Autonomic Symptom Score 31 (COMPASS-31) was added to investigate symptoms of orthostatic intolerance and secretomotor function, which are frequently underrecognized. Later, in the context of long-COVID, this questionary was suggested as a screening tool to track symptoms changes of autonomic dysfunction.¹⁵15 Larsen NW, Stiles LE, Miglis MG. Preparing for the long-haul: Autonomic complications of COVID-19. Auton Neurosci 2021; 235:102841

Olfactory dysfunction (OD), partial hyposmia or total anosmia, is the reduced ability to smell during sniffing (orthonasal olfaction) or eating and drinking (retronasal olfaction). The retronasal olfaction contributes to the taste, whose dysfunction can be partial hypogeusia or total ageusia. The interviewers asked whether smell and taste were reduced or absent during sniffing, chewing, drinking, or digesting food. Orthostatic intolerance, xerophthalmia, and xerostomia were identified according to questions number one, nine, and ten of COMPASS-31. Questions number two and three characterized the frequency and intensity of orthostatic intolerance.

The COMPASS-31 is a 31-item survey, organized in 6-scale domains, which assesses the presence, severity, distribution, frequency, and progression of autonomic symptoms. Regarding the clinical relevance of the domain, the scores provide the total weighted score, which ranges from 0 to 100. The higher scores indicate a more significant symptom load.¹⁶16 Sletten DM, Suarez GA, Low PA, Mandrekar J, Singer W. COMPASS 31: a refined and abbreviated Composite Autonomic Symptom Score. Mayo Clin Proc 2012;87(12):1196-1201 As some COVID-19 symptoms are similar to autonomic symptoms, a score with gastrointestinal domain scored as zero was named COMPASS-31(-GI). The Mayo Clinic Autonomic Laboratory validated the Brazilian Portuguese language version of COMPASS-31. The overall score of patients with COVID-19 was compared to those of healthy controls in previously published literature (mean 8.9±8.7).¹⁷17 Vincent A, Whipple MO, Low PA, Joyner M, Hoskin TL. Patients With Fibromyalgia Have Significant Autonomic Symptoms But Modest Autonomic Dysfunction. PM R 2016;8(05):425-435

Comorbidity profile

As a complete database was available, the co-existing conditions were obtained manually in medical records. The Charlson Comorbidity Index was calculated by the investigators. The method uses 17 comorbidities associated with mortality to classify prognostic comorbidity.¹⁸18 Goldstein DS. The extended autonomic system, dyshomeostasis, and COVID-19. Clin Auton Res 2020;30(04):299-315 The severity of comorbid diseases is mild (scores 1-2), moderate (scores 3-4), and severe (scores ≥ 5).

Statistical analysis

Data were examined using the Statistical Package Social Sciences (SPSS, IBM Corp. Armonk, NY, USA) software for windows 8, version 21.0. Data were analyzed as a whole, and whether the patient has subjective OD or not (s̄OD). Normality and homogeneity tests and parametric analyses were used in the descriptive statistics. The Student T-test was used to compare COMPASS-31 overall total weighted score (TWS) and controls. The Pearson chi-squared and Fisher exact tests were used to analyze categorical variables. Generalized Linear Models, according to the distribution of the dependent variable (gamma and Poisson log-linear), were used to obtain COMPASS-31 scores, with OD as the independent variable. Logistic binary regression, with OD as the predictor, was used to compare the magnitude of the risk factors (odds ratio, OR) in a few neurological symptoms. The results are presented as means ± standard deviation and percentages (%). The significant level considered was p < 0.05.

RESULTS

Demographics

A total of 124 surveys were obtained among the 118 patients enrolled. After reviewing the medical records, our study consisted of 100 patients. The clinical, laboratory, and imaging features of the patients are summarized in ►Table 1. Among the sample, 44 patients had OD. The mean age of the sample was 55.02 ± 15.12 years, with 39 patients being over 60 years of age. There were 58 male patients. The sample’s mean body mass index (BMI) was above normal limits. Furthermore, OD patients had a higher percentage of weakness, shortness of breath, and constipation, compared to s̄OD. The mean lymphocyte count was also higher for OD patients than for s̄OD. There was a higher percentage of thrombocytopenia in s̄OD, compared with OD. Regarding chest imaging, 60.7% of the patients in the s̄OD group had < 25% disease severity, and 43.2% of those in the OD group had 25 to 49% extension.

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Table 1
Clinical, laboratory, and imaging features of hospitalized patients with COVID-19

Both groups had a high percentage of patients on antihypertensive agents, and a low percentage on antidepressants and neuroleptics. Almost all the patients were using ACE inhibitors. The viral load quantitation was missing for 13 patients who had the samples collected at a different hospital. There were no significant differences between the groups in the use of medications, other general symptoms, delay to confirm SARS-Cov2 infection, and other laboratory testing on admission. The ►Supplementary Material Table S1 shows in-hospital standard of care of the patients. Finally, the OD group received more antiviral treatment than s̄OD (11.4 vs. 1.8%), but other differences were not seen, including clinical outcomes and mortality.

Neurological symptoms

►Table 2 shows that the mean number of days from the onset of illness to the neurological symptoms was 1.48 ± 3.41. The neurological symptoms occurred in 80% of the sample. The patients in the s̄OD group reported 64.3% of other neurological symptoms rather than anosmia/hyposmia. The most frequent symptoms were xerostomia (71%), ageusia/hypogeusia (50%), orthostatic intolerance (49%), anosmia/hyposmia (44%), myalgia (31%), dizziness (24%), xerophthalmia (20%), impaired consciousness due to syncope, seizures, daytime sleepiness or insomnia (18%), and headache (16%). The OD group had a higher percentage of ageusia/hypogeusia (97.7 vs. 12.5%, OR = 301, 95% confidence interval [CI] 35.59 to 2,545.42), dizziness (34.1 vs. 16.1%, OR = 2.70, 95% CI 1.04 to 6.96) orthostatic intolerance (63.6 vs. 37.5%, OR = 2.91, 95% CI 1.28 to 6.61), and xerophthalmia (29.5 vs. 12.5%, OR = 2.93,95% CI 1.05 to 8.16) than s̄OD. Orthostatic intolerance occurred more frequently and with moderate and severe intensity in OD. Other neurological symptoms did not differ. The sample had a higher COMPASS-31 mean score than that of healthy controls previously published (14.85 ± 12.06 vs. 8.9, t = 4.939, 95% CI 3.56 to 8.35, p < 0.001). The COMPASS-31 and COMPASS-31(-GI) mean scores for the OD group were higher than for the s̄OD one.

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Table 2
Neurological symptoms of hospitalized patients with COVID-19

Comorbidity profile

The associated diseases are presented in ►Table 3. The majority of the patients (91%) had a comorbid condition. The most frequent premorbidities were hypertension (60%), diabetes (40%), obesity (33%), smoking history (25%), and cardiac (23%) or end-stage renal (31%) diseases. The OD group had a higher percentage of hypertension (72.7 vs. 50%) and diabetes (59.1 vs. 25%), compared to s̄OD. There were no significant differences between these groups concerning other coexisting disorders or the Charlson Comorbidity Index, according to which 65% of the patients had a moderate to severe scores.

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Table 3
Comorbidity profile of hospitalized patients with COVID-19

DISCUSSION

Among hospitalized multimorbidity patients with laboratory-confirmed COVID-19, the neurological symptoms were very frequent, developing shortly after the onset of typical flu symptoms. Our strong results are the presence of chemical sense impairment and underestimated autonomic symptoms. Most of the patients without anosmia/hyposmia also reported another neurological symptom.

The neurological features in COVID-19 vary according to the sample and data collection. Our frequency of olfactory and gustatory dysfunction is comparable to the 46.8 and 52.3% already described. Headache and dizziness were reported in 7.5% and 6.1% of patients, respectively. Diabetes (31.1%) and hypertension (13.5%) were the most common associated comorbidities.¹⁹19 Di Carlo DT, Montemurro N, Petrella G, Siciliano G, Ceravolo R, Perrini P. Exploring the clinical association between neurological symptoms and COVID-19 pandemic outbreak: a systematic review of current literature. J Neurol 2021;268(05):1561-1569 The pooled prevalence of central nervous system or mental associated disorders in COVID-19 is around 50.68%. The most frequent symptom was OD (36.20% in 10 studies of the meta-analysis).²⁰20 Soltani S, Tabibzadeh A, Zakeri A, et al. COVID-19 associated central nervous system manifestations, mental and neurological symptoms: a systematic review and meta-analysis. Rev Neurosci 2021;32(03):351-361 The main neurological symptoms detected among COVID-19 patients were fatigue (42.9%), gustatory (35.4%) and olfactory (25.3%) dysfunctions, 10% headache (10%), and dizziness (6.7%) in another meta-analysis.¹⁴14 Vakili K, Fathi M, Hajiesmaeili M, et al. Neurological Symptoms, Comorbidities, and Complications of COVID-19: A Literature Review and Meta-Analysis of Observational Studies. Eur Neurol 2021;84(05):307-324 An European multinational study with 6,537 SARS-infected patients reported the frequency of headache (18.5%), impaired sense of smell (9.0%) and taste (12.8%), and delirium (6.7%). The patients were mostly hospitalized in complicated/critical (53%) and uncomplicated phases.²¹21 Kleineberg NN, Knauss S, Gülke E, et al; LEOSS Study Group. Neurological symptoms and complications in predominantly hospitalized COVID-19 patients: Results of the European multinational Lean European Open Survey on SARS-Infected Patients (LEOSS). Eur J Neurol 2021;28(12):3925-3937

As expected, the three most frequent diseases found in our patients are risk factors for COVID-19, which seem to negatively affect the clinical course and morbimortality outcomes, but this is not definitely clear.²²22 Buscemi S, Corleo D, Randazzo C. Risk Factors for COVID-19: Diabetes, Hypertension, and Obesity. Adv Exp Med Biol 2021; 1353:115-129 Our groups without and with OD were demographically similar, but the one with OD constituted a majority of those with hypertension, diabetes, and a higher extension on chest imaging.

The SARs-CoV-2 upregulates ACE2 expression in patients with hypertension, which can increase blood pressure and determine pneumonia. As diabetes has impaired T-cell function and increased interleukin-6, pneumonia-like symptoms can exist in these patients with COVID-19.²³23 Ejaz H, Alsrhani A, Zafar A, et al. COVID-19 and comorbidities: Deleterious impact on infected patients. J Infect Public Health 2020;13(12):1833-1839 The association between COVID-19 and hypertension has generated considerable discussion. Hypertension is normally accompanied by many comorbidities that are major factors for disease severity, and there is little evidence of ACE inhibitors influencing tissue expression or activity of ACE2 in humans.²⁴24 Shibata S, Arima H, Asayama K, et al. Hypertension and related diseases in the era of COVID-19: a report from the Japanese Society of Hypertension Task Force on COVID-19. Hypertens Res 2020;43(10):1028-1046

The increased risk of hyposmia after recovery of patients with type 2 diabetes and mild pneumonia associated with COVID-19, as well as animal experiments, indicate that diabetes could dampen the first-line defense of nasal immunity. There is an impaired nasal-associated lymphoid tissue immunity in diabetes type 2.²⁵25 Zhao Y, Liu Y, Yi F, et al. Type 2 diabetes mellitus impaired nasal immunity and increased the risk of hyposmia in COVID-19 mild pneumonia patients. Int Immunopharmacol 2021;93:107406 The extended autonomic system includes the neuroendocrine and neuroimmune systems.¹⁸18 Goldstein DS. The extended autonomic system, dyshomeostasis, and COVID-19. Clin Auton Res 2020;30(04):299-315 The link between diabetes and OD is controversial. Adults with diabetes on more aggressive treatments showed a trend toward severe hyposmia/anosmia in the pocket smell test, without an association between disease duration and self-reported symptoms.²⁶26 Chan JYK, García-Esquinas E, Ko OH, Tong MCF, Lin SY The Association Between Diabetes and Olfactory Function in Adults. Chem Senses 2017;43(01):59-64 There were no differences in an objective odor test between patients with and without chronic complications of diabetes.²⁷27 Kaya KS, Mazı EE, Demir ST, Tetik F, Tuna M, Turgut S. Relationship between progression of type 2 diabetes mellitus and olfactory function. Am J Otolaryngol 2020;41(02):102365

The slightly increased autonomic load in our sample might be explained, at least partially, by diabetes. The COMPASS-31 scores in all the groups of this study were lower than those of diabetics with cardiovascular autonomic neuropathy and polyneuropathy.²⁸28 Greco C, Di Gennaro F, D’Amato C, et al. Validation of the Composite Autonomic Symptom Score 31 (COMPASS 31 ) for the assessment of symptoms of autonomic neuropathy in people with diabetes. Diabet Med 2017;34(06):834-838 A cut-off of 28.67 indicates autonomic dysfunction in diabetes.²⁹29 Singh R, Arbaz M, Rai NK, Joshi R. Diagnostic accuracy of composite autonomic symptom scale 31 (COMPASS-31) in early detection of autonomic dysfunction in type 2 diabetes mellitus. Diabetes Metab Syndr Obes 2019;12:1735-1742 Even though the symptoms were interrogated during COVID-19, and despite the confounders, such as medication side effects and dehydration, diabetes was a possible factor for orthostatic intolerance in our study.

The elevated frequency of ageusia/hypogeusia in those with OD in our study was likely due to gustatory function being mediated through the sense of smell, pain perception, and somatosensory pathway. Elevated olfactory and gustatory dysfunction occur in mild-to-moderate COVID-19 through sense questionnaires. Of the 18.2% of patients without nasal obstruction or rhinorrhea, 79.7% had OD.⁷7 Lechien JR, Chiesa-Estomba CM, De Siati DR, et al. Olfactory and gustatory dysfunctions as a clinical presentation of mild-to-moderate forms of the coronavirus disease (COVID-19): a multicenter European study. Eur Arch Otorhinolaryngol 2020;277(08):2251-2261 Chemosensory loss of smell and taste occurred in outpatients with influenza-like symptoms and COVID-19.³⁰30 Yan CH, Faraji F, Prajapati DP, Boone CE, DeConde AS. Association of chemosensory dysfunction and COVID-19 in patients presenting with influenza-like symptoms. Int Forum Allergy Rhinol 2020;10(07):806-813

Our frequency of headache was a quarter of the one detected in adult symptomatic patients with laboratory- confirmed COVID-19 from the northeast of Brazil, whose characteristics were usually bilateral and severe, but rarely continuous. We found a comparable frequency of anosmia/hyposmia and ageusia/hypogeusia, but not the elevated risk of headache in those with impairment of smell and taste.⁶6 Rocha-Filho PAS, Magalhães JE. Headache associated with COVID-19: Frequency, characteristics and association with anosmia and ageusia. Cephalalgia 2020;40(13):1443-1451

The autonomic symptoms can arise as para- and post-infectious manifestations, especially in viral infections such as herpes simplex and mononucleosis. A case-control study from Colombia showed that in Zika virus outbreaks, the COMPASS-31 was elevated, mainly in the orthostatic, secretomotor, and bladder domains, about 63 weeks after disease onset.³¹31 Rodríguez Y, Rojas M, Ramírez-Santana C, Acosta-Ampudia Y, Monsalve DM, Anaya JM. Autonomic symptoms following Zika virus infection. Clin Auton Res 2018;28(02):211-214

Two-thirds of the patients with anosmia/hyposmia had orthostatic intolerance answering to: você se sentiu tonto, desorientado, aéreo ou teve dificuldade de pensar quando levantou após ter ficado sentado ou deitado? (did you feel dizzy, disoriented, lightheaded or had difficulty thinking when you got up from sitting or lying down?). They had a 2.9-fold higher risk, compared to those without anosmia/hyposmia. Orthostatic intolerance was more frequent and more intense in those with anosmia/hyposmia. This multifactorial symptom is associated with hyperadrenergic state and hypovolemia, among other factors that may have been present in COVID-19. Similarly, the elevated frequency of xerostomia could be associated with different causes.

Our COMPASS-31 score is almost 2-fold higher in healthy individuals than noted in previous studies, and another analysis reduced the overstatement of gastrointestinal symptoms as a bias. As the patients were asked about the presence and progression of such symptoms during COVID-19, our findings confirm these symptoms in the acute disease, especially in patients with subjective OD. Our scores are comparable to those of outpatients with post-COVID, using the same instrument. Orthostatic hypotension and hyposmia/hypogeusia occurred in 13.8 and 37.1% of them;⁹9 Buoite Stella A, Furlanis G, Frezza NA, Valentinotti R, Ajcevic M, Manganotti P. Autonomic dysfunction in post-COVID patients with and witfhout neurological symptoms: a prospective multidomain observational study. J Neurol 2022;269(02):587-596 autonomic symptoms may start within the first weeks of illness, or after hospital discharge.¹⁰10 Dani M, Dirksen A, Taraborrelli P, et al. Autonomic dysfunction in ‘long COVID’: rationale, physiology and management strategies. Clin Med (Lond) 2021;21(01):e63-e67,³²32 Goldstein DS. The possible association between COVID-19 and postural tachycardia syndrome. Heart Rhythm 2021;18(04):508-509,³³33 Yong SJ. Long COVID or post-COVID-19 syndrome: putative pathophysiology, risk factors, and treatments. Infect Dis (Lond) 2021;53(10):737-754

The most frequent autonomic symptoms in patients referred to autonomic testing after COVID-19 were orthostatic such as lightheadedness (93%) and headache (22%). Orthostatic intolerance without tachycardia or hypotension was more frequent than postural orthostatic tachycardia syndrome.³⁴34 Shouman K, Vanichkachorn G, Cheshire WP, et al. Autonomic dysfunction following COVID-19 infection: an early experience. Clin Auton Res 2021;31(03):385-394 Cardiovascular reflex alterations in early COVID-19 without associated diseases were remarkable in those with mild disease or with confirmed interstitial pneumonia. Orthostatic hypotension frequency was 33%.¹¹11 Milovanovic B, Djajic V, Bajic D, et al. Assessment of Autonomic Nervous System Dysfunction in the Early Phase of Infection With SARS-CoV-2 Virus. Front Neurosci 2021;15:640835

Impaired consciousness occurred in 18% of our sample. Syncope and presyncope occurred around 4.2% in COVID-19, mainly due to unexplained causes.³⁵35 de Freitas RF, Torres SC, Martín-Sánchez FJ, Carbó AV, Lauria G, Nunes JPL. Syncope and COVID-19 disease - A systematic review. Auton Neurosci 2021;235:102872 As a deficient compensatory heart rate increase was observed in a few patients with syncope during the acute hypocapnic hypoxemia, researchers hypothesize that SARS-CoV-2 could have caused ACE2 internalization in midbrain nuclei changing the baroreflex and chemoreceptor responses.³⁶36 Canetta C, Accordino S, Buscarini E, et al. Syncope at SARS-CoV-2 onset. Auton Neurosci 2020;229:102734

The neuropathogenesis in COVID-19 includes a direct attack on the nervous system, and in direct effects of systemic factors, with postinfectious immune-mediated complications.³⁷37 Pezzini A, Padovani A. Lifting the mask on neurological manifestations of COVID-19. Nat Rev Neurol 2020;16(11):636-644 The neurotropism of SARS-CoV-2 may partially contribute to respiratory failure.³⁸38 Li YC, Bai WZ, Hashikawa T. The neuroinvasive potential of SARSCoV2 may play a role in the respiratory failure of COVID-19 patients. J Med Virol 2020;92(06):552-555 Older adults and those with multiple diseases have reduced homeostatic capabilities. The happy or silent hypoxemia, a term applied to the deficient blood oxygenation without dyspnea, is a blood-gas disorder that may occur due to an autonomic impairment. The allostasis, coordinated alterations to maintain homeostasis, is present in COVID-19 stress response.³⁹39 González-Duarte A, Norcliffe-Kaufmann L. Is ‘happy hypoxia’ in COVID-19 a disorder of autonomic interoception? A hypothesis. Clin Auton Res 2020;30(04):331–333

In conclusion, this study has limitations. Data collection was during the increasing rate of cases. To reduce the risk of in-hospital contamination, owing to the access of units with and without COVID-19 cases, it was not possible to recruit controls. We could not use objective methods to measure sense functions. We were unable to collect the duration of flow oxygen therapy, which excites nerve endings (common chemical sense) to cause burning sensations. They can confound taste symptoms and xerostomia. Given the small number of patients without diabetes, but with anosmia, a subcategory analysis was not possible.

The COVID-19 neurological complications are associated with a poor in-hospital outcome and a high risk of mortality.⁴⁰40 Frontera JA, Sabadia S, Lalchan R, et al. A Prospective Study of Neurologic Disorders in Hospitalized Patients With COVID-19 in New York City. Neurology 2021;96(04):e575-e586 However, the growing evidence of OD as a prognostic marker of better in-hospital outcome for patients with COVID-19 was not observed in this study, probably due to the sample size (►Supplementary Material).⁴4 Sampaio Rocha-Filho PA, Magalhães JE, Fernandes Silva D, et al. Neurological manifestations as prognostic factors in COVID-19: a retrospective cohort study. Acta Neurol Belg 2022;122(03):725-733

The causes underlying the neurological symptoms of inpatients with COVID-19, especially those with associated diseases, can be multiple and unclear. Our results reinforce that they can be related to the COVID-19 itself, comorbidities, pharmacotherapies, and other factors. Given that the symptoms may persist, their recognition is critical to recovery, mainly those not frequently explored. The management of orthostatic symptoms could reduce the severity of chronic illness in long-COVID.

Acknowledgments

The authors are grateful to the Hospital Sao Paulo from the Federal University of Sao Paulo (Sao Paulo, Brazil) for financial and logistical support, including personal protective equipment for data collection. Dr. David Sletten and Dr. Wolfgang Singer from the Autonomic Laboratory of Mayo Clinic College of Medicine and Science (Rochester EUA) for the Brazilian Portuguese version of COMPASS-31.

Support

This work was supported by the Hospital São Paulo and the Department of Neurology and Neurosurgery, Federal University of São Paulo, Brazil.

References

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Mao L, Jin H, Wang M, et al. Neurologic Manifestations of Hospitalized Patients With Coronavirus Disease 2019 in Wuhan, China. JAMA Neurol 2020;77(06):683-690
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Sampaio Rocha-Filho PA, Magalhães JE, Fernandes Silva D, et al. Neurological manifestations as prognostic factors in COVID-19: a retrospective cohort study. Acta Neurol Belg 2022;122(03):725-733
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Amanat M, Rezaei N, Roozbeh M, et al. Neurological manifestations as the predictors of severity and mortality in hospitalized individuals with COVID-19: a multicenter prospective clinical study. BMC Neurol 2021;21(01):116
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Rocha-Filho PAS, Magalhães JE. Headache associated with COVID-19: Frequency, characteristics and association with anosmia and ageusia. Cephalalgia 2020;40(13):1443-1451
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Lechien JR, Chiesa-Estomba CM, De Siati DR, et al. Olfactory and gustatory dysfunctions as a clinical presentation of mild-to-moderate forms of the coronavirus disease (COVID-19): a multicenter European study. Eur Arch Otorhinolaryngol 2020;277(08):2251-2261
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Baker J, Incognito AV, Wilson RJA, Raj SR. Syncope and silent hypoxemia in COVID-19: Implications for the autonomic field. Auton Neurosci 2021;235:102842
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Buoite Stella A, Furlanis G, Frezza NA, Valentinotti R, Ajcevic M, Manganotti P. Autonomic dysfunction in post-COVID patients with and witfhout neurological symptoms: a prospective multidomain observational study. J Neurol 2022;269(02):587-596
¹⁰
Dani M, Dirksen A, Taraborrelli P, et al. Autonomic dysfunction in ‘long COVID’: rationale, physiology and management strategies. Clin Med (Lond) 2021;21(01):e63-e67
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Milovanovic B, Djajic V, Bajic D, et al. Assessment of Autonomic Nervous System Dysfunction in the Early Phase of Infection With SARS-CoV-2 Virus. Front Neurosci 2021;15:640835
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Eshak N, Abdelnabi M, Ball S, et al. Dysautonomia: An Overlooked Neurological Manifestation in a Critically ill COVID-19 Patient. Am J Med Sci 2020;360(04):427-429
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Atkins JL, Masoli JAH, Delgado J, et al. Preexisting Comorbidities Predicting COVID-19 and Mortality in the UK Biobank Community Cohort. J Gerontol A Biol Sci Med Sci 2020;75(11):2224-2230
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Vakili K, Fathi M, Hajiesmaeili M, et al. Neurological Symptoms, Comorbidities, and Complications of COVID-19: A Literature Review and Meta-Analysis of Observational Studies. Eur Neurol 2021;84(05):307-324
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Larsen NW, Stiles LE, Miglis MG. Preparing for the long-haul: Autonomic complications of COVID-19. Auton Neurosci 2021; 235:102841
¹⁶
Sletten DM, Suarez GA, Low PA, Mandrekar J, Singer W. COMPASS 31: a refined and abbreviated Composite Autonomic Symptom Score. Mayo Clin Proc 2012;87(12):1196-1201
¹⁷
Vincent A, Whipple MO, Low PA, Joyner M, Hoskin TL. Patients With Fibromyalgia Have Significant Autonomic Symptoms But Modest Autonomic Dysfunction. PM R 2016;8(05):425-435
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Goldstein DS. The extended autonomic system, dyshomeostasis, and COVID-19. Clin Auton Res 2020;30(04):299-315
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Di Carlo DT, Montemurro N, Petrella G, Siciliano G, Ceravolo R, Perrini P. Exploring the clinical association between neurological symptoms and COVID-19 pandemic outbreak: a systematic review of current literature. J Neurol 2021;268(05):1561-1569
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Zhao Y, Liu Y, Yi F, et al. Type 2 diabetes mellitus impaired nasal immunity and increased the risk of hyposmia in COVID-19 mild pneumonia patients. Int Immunopharmacol 2021;93:107406
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Singh R, Arbaz M, Rai NK, Joshi R. Diagnostic accuracy of composite autonomic symptom scale 31 (COMPASS-31) in early detection of autonomic dysfunction in type 2 diabetes mellitus. Diabetes Metab Syndr Obes 2019;12:1735-1742
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Shouman K, Vanichkachorn G, Cheshire WP, et al. Autonomic dysfunction following COVID-19 infection: an early experience. Clin Auton Res 2021;31(03):385-394
³⁵
de Freitas RF, Torres SC, Martín-Sánchez FJ, Carbó AV, Lauria G, Nunes JPL. Syncope and COVID-19 disease - A systematic review. Auton Neurosci 2021;235:102872
³⁶
Canetta C, Accordino S, Buscarini E, et al. Syncope at SARS-CoV-2 onset. Auton Neurosci 2020;229:102734
³⁷
Pezzini A, Padovani A. Lifting the mask on neurological manifestations of COVID-19. Nat Rev Neurol 2020;16(11):636-644
³⁸
Li YC, Bai WZ, Hashikawa T. The neuroinvasive potential of SARSCoV2 may play a role in the respiratory failure of COVID-19 patients. J Med Virol 2020;92(06):552-555
³⁹
González-Duarte A, Norcliffe-Kaufmann L. Is ‘happy hypoxia’ in COVID-19 a disorder of autonomic interoception? A hypothesis. Clin Auton Res 2020;30(04):331–333
⁴⁰
Frontera JA, Sabadia S, Lalchan R, et al. A Prospective Study of Neurologic Disorders in Hospitalized Patients With COVID-19 in New York City. Neurology 2021;96(04):e575-e586

Publication Dates

Publication in this collection
15 May 2023
Date of issue
2023

History

Received
16 Feb 2022
Reviewed
10 May 2022
Accepted
05 June 2022

This is an Open Access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.

[1] Support

This work was supported by the Hospital São Paulo and the Department of Neurology and Neurosurgery, Federal University of São Paulo, Brazil.

		Overall	OD		p-value
		Overall	without	with	p-value
		(N = 100)	(N = 56)	(N = 44)
Age, years		55.02 ± 15.12	55.16 ± 15.26	54.84 ± 15.11	0.91
Age category, %	18–60 years	61	57.1	65.9	0.37
Age category, %	>60 years	39	42.9	34.1	0.37
Male gender, %		58	66.1	47.7	0.06
BMI, kg/m²		27.66 ± 5.96	27.49 ± 5.38	27.79 ± 6.42	0.80
Regular medications use	Antihypertensives¹	66	67.9	63.6	0.65
	Antidepressants and neuroleptics	6	3.6	9.1	0.40
	Immunosuppressants	31	30.4	31.8	0.87
	Oral corticosteroids	27	26.8	27.3	0.95
	Oral anticoagulants	4	3.6	4.5	1
General symptoms, %	Anorexia	50	42.9	59.1	0.10
	Fever/chill	66	66.1	65.9	0.98
	Weakness	60	50.0	72.7	0.02
	Cough	68	62.5	75.0	0.18
	Sore throat	25	19.6	31.8	0.16
	Rhinorrhea	21	23.2	18.2	0.54
	Shortness of breath	66	57.1	77.3	0.03
	Diarrhea	50	50	50	1
	Nausea/vomiting	35	35.7	34.1	0.86
	Constipation	15	7.1	25	0.01
Viral load quantitation, %	High	44	40.0	59.5	0.07
	Low	45	60.0	40.5
	Missing²	13	6	7
Delay to confirmation, days³		6.08 ± 4.24	6.25 ± 4.49	5.86 ± 3.93	0.65
White blood cells⁴	Leucocyte count	9,164 ± 6,581	8,636 ± 6,831	9,835 ± 6,262	0.36
	Neutrophils count	6,859 ± 4,815	6,638 ± 5,286	7,140 ± 4,182	0.60
	Lymphocytes count	1,202 ± 876	1,011 ± 724	1,445 ± 995	0.01
Platelet	Count⁴ *1000	214.85 ± 95.71	198.84 ± 92.86	235.23 ± 96.45	0.05
Platelet	Thrombocytopenia, % (<100,000⁴)	27	35.7	15.9	0.02
Serum creatinine⁵		2.82 ± 7.07	2.28 ± 3.04	3.51 ± 10.12	0.39
Blood urea nitrogen⁵		63.47 ± 53.59	66.29 ± 61.09	59.95 ± 42.85	0.56
C-reactive protein⁶		104.23 ± 79.82	104.96 ± 78.76	103.3 ± 82.07	0.91
Lactose dehydrogenase⁷		384.12 ± 164.71	351.3 ± 140.63	420.23 ± 182.7	0.05
Chest CT category, %⁸	0 (none)	7	5.4	9.1	0.001
	1 (<25%)	43	60.7	20.5*
	2 (25–49%)	31	21.4	43.2*
	3 (50–75%)	18	12.5	25.7
	4 (>75%)	1	0.0	2.3

		OD
	Overall	without	with	p-value
	(N = 100)	(N = 56)	(N = 44)
Delay, days¹	1.48 ± 3.41	1.39 ± 3.48	1.55 ± 3.39	0.84
Neurological symptom, %	80	64.3	100	<0.001
Ageusia/hypogeusia²	50	12.5	97.7	<0.001
Vision impairment	11	8.9	13.6	0.45
Dizziness³	24	16.1	34.1	0.03
Irritability	12	7.1	18.2	0.09
Impaired consciousness⁴	18	23.2	11.4	0.12
Confusion	9	8.9	9.1	0.97
Muscle weakness⁵	2	1.8	2.3	1
Myalgia	31	23.2	40.9	0.05
Headache	16	12.5	20.5	0.28
Orthostatic intolerance⁶	49	37.5	63.6	0.01
Frequency
Never	51	62.5	36.4*	0.02
Rarely	14	12.5	15.9
Occasionally	19	17.9	20.5
Frequently	15	7.1	25*
Almost always	1	0	2.3
Intensity				0.01
None	51	62.5*	36.4*
Mild	23	23.2	22.7
Moderate	20	12.5	29.5*
Severe	6	1.8*	11.4*	0.03
Xerophthalmia⁷	20	12.5	29.5	0.03
Xerostomia	71	64.3	79.5	0.09
COMPASS-31 TWS (0–100)	16.69 ± 11.52	12.92 ± 13.72	20.90 ± 23.47	0.002
TWS minus GI (0–75)	13.82 ± 9.71	10.58 ± 12.16	17.21 ± 20.26	0.003

		OD
	Overall	without	with	p-value
	(N = 100)	(N = 56)	(N = 44)
Associated medical disease, %
Hypertension	60	50	72.7	0.02
Diabetes mellitus	40	25	59.1	0.001
Obesity (BMI >30 kg/m²)	33	32.1	34.1	0.83
Smoking history¹	25	26.8	22.7	0.64
Cardiac diseases²	23	25	20.5	0.59
Chronic pulmonary disease³	10	12.5	6.8	0.34
End-stage renal disease	31	30.4	31.8	0.87
Kidney transplantation	24	23.2	25	0.83
Hemodialysis	7	7.1	6.8	1
Malignancy	9	8.9	9.1	0.97
Asthma	7	3.6	11.4	0.23
Vasculiti⁴	7	8.9	4.5	0.46
Cerebrovascular	7	3.6	11.4	0.23
Peripheral artery and aneurysm	2	0	4.5	0.37
Falciform anemia	2	1.8	2.3	1
Pulmonary tuberculosis	1	1.8	0	1
Other⁵	24	30.4	15.9	0.09
Charlson Comorbidity Index grade, %				0.64
None (CCI = 0)	9	10.7	6.8	0.49
Mild (CCI = 1–2)	26	26.8	25	0.84
Moderate (CCI = 3–4)	39	41.1	36.4	0.63
Severe (CCI ≥ 5)	26	21.4	31.8	0.24

Brasil

Brasil

Neurological symptoms and comorbidity profile of hospitalized patients with COVID-19

Sintomas neurológicos e perfil de comorbidades de pacientes hospitalizados com COVID-19

Abstract

Background

Objective

Methods

Results

Conclusion

Resumo

Antecedentes

Objetivo

Métodos

Resultados

Conclusão

INTRODUCTION

METHODS

Standard protocol approval and patient consent

Study design and sample

Data acquisition

Main outcome measure

Neurological symptoms

Comorbidity profile

Statistical analysis

RESULTS

Demographics

Neurological symptoms

Comorbidity profile

DISCUSSION

Acknowledgments

References

Publication Dates

History