Hot cross bun in pediatric age multi-system atrophy an unusual presentation

Lokesh Naik Mude; Omprakash Shital Shukla; Rinki H. Shah; Rajesh Rambhai Barad

doi:10.18203/2349-3291.ijcp20240105

Authors

Lokesh Naik Mude Department of Pediatrics, Medical College and S.S.G. Hospital, Baroda, Gujarat, India
Omprakash Shital Shukla Department of Pediatrics, Medical College and S.S.G. Hospital, Baroda, Gujarat, India
Rinki H. Shah Department of Pediatrics, Medical College and S.S.G. Hospital, Baroda, Gujarat, India
Rajesh Rambhai Barad Department of Pediatrics, Medical College and S.S.G. Hospital, Baroda, Gujarat, India

DOI:

https://doi.org/10.18203/2349-3291.ijcp20240105

Keywords:

Hot cross bun sign, Multisystem atrophy, Paresis, Neurology

Abstract

A 10-year-old female was brought to emergency department with complaint fever, cold, and cough for 5 days followed by weakness of upper limb weakness more than Lower limb associated with inability to walk/stand, brought to emergency with altered sensorium. Nervous system: Confused and altered, tone is normal, power: 3/3 in upper limbs 2/2 in lower limbs and reflexes in bilateral knee brisk, bilateral plantar-extensor; On general examination revealed hypomimia, dysarthria and bilateral bradykinesia along with ataxic gait and pyramidal signs. Blood investigation were normal and diagnosis made by neuroimaging s/o: Bilaterally symmetrical abnormal signal in both postero-medial thalami, bilateral insular cortices, pons and bilateral middle cerebellar peduncles. It is extending into pons involving transverse pontocerebellar tracts and median pontine raphe nuclei giving 'Hot cross bun sign' (HCBS). During course of treatment child had autonomic disturbances. Child was treated with supportive medication and methyl-presdnisolone followed by oral steroid. Child had responded to treatment given and child has been discharged with no neurological deficit on oral medications. We concluded autonomic dysfunction in any patient presenting with acute onset of weakness with short duration must evaluate for MSA and institute appropriate treatment.

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