Primary infection with human herpesvirus 6 (HHV-6) typically affects the paediatric population and usually manifests with fever and sudden exanthema.1,2 Manifestation as encephalitis is infrequent.2 After primary infection, the virus remains latent in the brain tissue, mononuclear cells, and salivary glands, and may be reactivated in the event of immunosuppression (for instance, following transplantation, HIV infection, or lymphoproliferative syndrome).1,2 Reactivation may be asymptomatic or may manifest with fever and skin rash, and in exceptional cases with pneumonia, hepatitis, or encephalitis.2 However, the literature includes cases of meningoencephalitis in immunocompetent patients, occasionally associated with co-infection with other pathogens.3,4
We report the case of an immunocompetent adult presenting meningoencephalitis in the context of co-infection with HHV-6 and influenza B virus.
Our patient is a 57-year-old man, a carrier of the factor V Leiden mutation, with history of meningoencephalitis of unknown aetiology, diagnosed 13 years previously, and lacunar ischaemic stroke that left no sequelae. A week after the onset of flu-like symptoms, he presented a 24-h history of fever, headache, neck pain, confusion, and generalised tonic-clonic seizures with subsequent incomplete recovery. The patient was transferred to the emergency department, where the examination revealed stupor, limited speech, neck rigidity, and fever of up to 40 °C. An emergency cerebrospinal fluid (CSF) analysis revealed mild lymphocytic pleocytosis (10 cells/μL), high protein levels (55 mg/dL), and normal glucose levels; a non-contrast brain computed tomography study showed normal results. We started empirical antibiotic and antiviral treatment with ceftriaxone, vancomycin, doxycycline, and aciclovir, and antiepileptic treatment with levetiracetam. Further laboratory analyses and a magnetic resonance imaging (MRI) study performed during admission ruled out vascular, structural, toxic/metabolic, autoimmune, and paraneoplastic origin. A study to determine the aetiology of the infection, including the most frequent pathogens, did not identify the causal agent. Among the results of the remaining complementary tests, we can only highlight the detection of diffuse slowing in the electroencephalography study, without epileptic activity. After a slight initial improvement, the patient presented deterioration of the level of alertness; the CSF study was repeated and the aetiological study was broadened. This time, a study of the nasopharyngeal exudate confirmed the presence of influenza B virus, and the microbiological analysis of the CSF yielded positive PCR results for HHV-6; the bacteria culture and tests for the remaining viruses analysed yielded negative results. In the light of these findings, we changed treatment to ganciclovir and oseltamivir for 14 and 4 days, respectively. Progression was favourable, with complete symptom resolution.
HHV-6 is a neurotropic virus that is increasingly recognised as an emerging pathogen of the nervous system. HHV-6 encephalitis is a severe complication in immunocompromised patients, whereas only isolated cases have been reported in immunocompetent patients.1 HHV-6 viral load has been confirmed in 40% of patients with encephalitis of unknown origin; however, the clinical relevance of the presence of HHV-6 in the CSF of these patients has been questioned.1
According to the available literature, HHV-6 encephalitis most frequently affects young patients (median age, 29 years). Clinically, it manifests with behavioural disorders and altered level of consciousness, focal neurological signs, and epileptic seizures with occasional progression to status epilepticus, encephalomyelitis, or relapsing and remitting encephalitis, especially in immunocompromised individuals.1,5–8 Patients may also present predominantly temporal MRI signal alterations that subsequently resolve. However, neuroimaging results may also be strictly normal.2 CSF usually shows variable lymphocytic pleocytosis (9-155 cells/μL) and eventually variable high protein and low glucose levels.1,2,7 Given the lack of randomised clinical trials, there is no current consensus on treatment. The clinical practice guidelines of the Infectious Diseases Society of America recommend ganciclovir, with a risk of developing resistance, or foscarnet; cases have been published in which both drugs were administered in combination.2,7 Prognosis is generally good.2
In our case, the patient developed similar symptoms to those reported in the literature, with the peculiarity that he presented co-infection with influenza B virus, which made it impossible to exclusively attribute some manifestations to HHV-6. Seizures have been described in adult patients with influenza virus infection.9 Cases of co-infection have been reported in a Japanese paediatric population,3,4 with ours being the first case in an immunocompetent adult, to our knowledge. It has been suggested that primary infection with influenza virus may cause a transient state of immunosuppression, thus triggering viral reactivation.3,4
Despite its rareness, we must consider HHV-6 in the differential diagnosis of lymphocytic meningoencephalitis of unknown origin in immunocompetent adults, especially when the patient presents a trigger factor favouring reactivation, such as influenza virus infection.
Conflicts of interestThe authors have no conflicts of interest to declare.
Please cite this article as: Jiménez Bolaños R, Díaz Díaz A, Sánchez-Miranda Román I, Castellano Santana JP. Meningoencefalitis por HHV-6 en un paciente inmunocompetente asociado a coinfección por virus de la gripe. Neurología. 2021;36:329–330.