Atypical imaging presentation of herpes simplex virus encephalitis in paediatric immunocompromised oncology patients

Introduction We aim to assess the imaging manifestations of brain involvement in paediatric immunocompromised patients with haematological malignancies on chemotherapy presenting with encephalitis and positive HSV CSF PCR. We also aim to determine whether our findings are similar or different to tho...

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Veröffentlicht in:Journal of medical imaging and radiation oncology 2022-08, Vol.66 (5), p.609-617
Hauptverfasser: Kapadia, Tejas, Sahu, Arpita, Gupta, Anurag, Dhamne, Chetan, Prasad, Maya, Chinaswamy, Girish, Kembhavi, Seema
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Sprache:eng
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Zusammenfassung:Introduction We aim to assess the imaging manifestations of brain involvement in paediatric immunocompromised patients with haematological malignancies on chemotherapy presenting with encephalitis and positive HSV CSF PCR. We also aim to determine whether our findings are similar or different to those described in literature for paediatric patients in general. Methods A retrospective study was performed in paediatric ALL/lymphoma patients on chemotherapy, and cases with positive CSF HSV‐PCR with at least one head MRI scan were included. On imaging, location(typical/atypical), post‐contrast enhancement and haemorrhage/diffusivity/gliosis were evaluated. Result A total of 28 scans were included in study from 16 patients fulfilling inclusion criteria, 12 (75%) HSV‐1 and 4 (25%) HSV‐2. Of the 16 initial scans (CT n = 10, MRI n = 6), 11 were normal (CT = 7, MRI = 4). Fourteen patients had follow‐up MRI, of which two had normal scans. On the abnormal initial scan (5/16), only 20% had typical medial temporal/inferomedial frontal/cingulate involvement. Most had frontal (80%), parietal (60%) and non‐medial temporal (40%) lesions. Abnormal diffusivity/haemorrhage was absent in all, and postcontrast enhancement was seen in 20%. On follow‐up, more patients (33%) had typical medial temporal/inferomedial frontal/cingulate involvement. Widespread atypical site involvement of frontoparietal (75%), thalamus (58%), non‐medial temporal (50%), occipital/basal ganglia (33%) and cerebellum (8%) was noted. Most lesions were cortical (91%)/subcortical (75%) with few periventricular lesions (58%). Few showed abnormal diffusivity (16%), post‐contrast parenchymal enhancement/haemorrhage (8%), post‐contrast meningeal enhancement (25%) and gliosis (16%). Conclusion Immunocompromised paediatric patients with haematological malignancies have widespread atypical brain involvement in herpes simplex encephalitis with lack of diffusion restriction and post‐contrast enhancement, likely due to haematogenous spread of HSV across the blood–brain barrier, lack of cellular immunity and limited inflammatory cytokine response.
ISSN:1754-9477
1754-9485
DOI:10.1111/1754-9485.13326