Abstract

Wolfram syndrome is a rare genetic disease with characteristic brain involvement. We reviewed the brain MR images of patients with Wolfram syndrome to determine the frequency and characteristics of common neuroradiologic findings. We retrospectively reviewed the imaging data of patients with genetically-confirmed Wolfram syndrome who had been recruited to the Washington University Wolfram Syndrome Research Clinic. These patients were evaluated between 2010 and 2019 with annual MRIs, along with other measures. MR images were assessed for clinical neuroradiologic signs at each individual's first and last follow-up visits to characterize the frequency, rate of progression, and clinical correlations of these signs. We included 30 patients (13 males/17 females; average age at first visit, 14 years; average age at last visit, 19 years). The median duration of follow-up was 5 years (range, 2-9 years). The most common findings were an absent or diminished posterior pituitary bright spot (first, 53%; last, 70%), T1/T2 pons signal abnormalities (first, 53%; last, 67%), optic nerve atrophy (first, 30%; last, 80%), white matter T2 hyperintensities (first, 27%; last, 35%), and cerebellar atrophy (first, 23%; last, 70%). Patients with Wolfram syndrome present characteristic neuroradiologic findings that involve the posterior pituitary gland, optic nerves, white matter, brain stem, and cerebellum. These abnormal findings appear at an early age and tend to increase in frequency with time. However, the neurologic significance and neuropathologic mechanisms of each sign require more investigation. Neuroradiologists should be aware of the pattern of these features in Wolfram syndrome.

Highlights

  • BACKGROUND AND PURPOSEWolfram syndrome is a rare genetic disease with characteristic brain involvement

  • Neuroradiologists should be aware of the pattern of these features in Wolfram syndrome

  • Wolfram syndrome is a rare genetic multisystem disease characterized by juvenile-onset diabetes mellitus, progressive optic atrophy, sensorineural hearing loss, and diabetes insipidus (DI)

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Summary

MATERIALS AND METHODS

Data from participants in the Washington University Wolfram Syndrome Research Clinic were evaluated. Inclusion criteria were genetically-confirmed Wolfram syndrome (WFS1 mutations on both alleles that are known or suspected to be pathogenic), participant’s awareness of the diagnosis, age younger than 30 years at the time of enrollment, and the ability to travel to St. Louis for the annual research clinic visits. For the Tim Trio, the T1-weighted MPRAGE sequence was used (sagittal acquisition: TR 1⁄4 2400 ms, TE 1⁄4 3.16 ms, TI 1⁄4 1000 ms, voxel resolution 1⁄4 1 Â 1 Â 1 mm, time 1⁄4 8 minutes and 9 seconds). On the Magnetom Prisma scanner, the MPRAGE sequence was slightly different (TR 1⁄4 2500 ms, TE1 1⁄4 1.81 ms, TE2 1⁄4 3.6 ms, TE3 1⁄4 5.39 and 7.18 ms, TI 1⁄4 1000 ms, voxel resolution 1⁄4 0.8 Â 0.8 Â 0.8 mm, maximum acquisition time 1⁄4 8 minutes and 22 seconds).

RESULTS
CONCLUSIONS
Neuroradiologic Findings
DISCUSSION

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