# A Comprehensive Overview of the Clinical, Electrophysiological, and Neuroimaging Features of BPAN: Insights From a New Case Series

**Authors:** Seda Susgun, Ozgu Kizek, Sibel Aylin Ugur Iseri, Ibrahim Kamaci, Ayse Deniz Elmali, Pinar Iscen, Berfin Gulkaya Guzel, Gul Yalcin Cakmakli, Bulent Elibol, Berril Donmez, Raif Cakmur, Pinar Topaloglu, Abdullah Acar, Abdullah Acar, Ahmet Acarer, Arzu Karabay, Asuman Ali, Ayla Barlas, Aysegul Gunduz, Banu Ozen Barut, Baris Baslo, Bilge Kocer, Bilgehan Mus, Birsen Karaman, Burcu Gokce Cokal, Cem Ismail Kucukali, Cenk Akbostanci, Ceyhun Sayman, Cagla Turan, Dilek Ince Gunal, Ebru Bilge Dirik, Ebru Erzurumluoglu, Elif Kocasoy Orhan, Enes Demiryurek, Emrah Yucesan, Ercan Kose, Erdem Tuzun, Esen Saka Topcuoglu, Esra Okuyucu, Fatma Betul Ozdilek, Feriha Ozer, Gencer Genc, Gozde Unal, Gulay Kenangil, Gullu Tarhan, Gunes Kiziltan, Halil Onder, Hamit Genc, Hasmet Hanagasi, Hatice Yuksel, Hulya Apaydin, Koray Kirimtay, Mehmet Guney Senol, Melisa Kilic, Meltem Demirkiran, Mert Karaca, Miray Erdem, Muhammet Bilgehan Mus, Murat Gultekin, Nalan Capan, Nazan Karagoz Sakalli, Nazli Basak, Nihan Hande Akcakaya, Ozan Ezer, Ozge Uygun, Ozge Yilmaz Kuspeci, Ozgur Oztop Cakmak, Pervin Iseri, Petek Ballar Kirmizibayrak, Pinar Elkoca, Recep Alp, Remzi Yigiter, Rezzak Yilmaz, Sadika Ozdemir, Selda Keskin, Selen Ilhan Alp, Selen Soylu, Serdar Ceylaner, Serhat Ozkan, Sevda Erer Ozbek, Sevgin Gundogan, Sevil Yasufli, Sezin Alpaydin Baslo, Sibel Ertan, Sultan Cagirici, Seyma Aykac, Vuslat Yilmaz, Yaprak Secil, Yasar Kutukcu, Yeliz Ciftci, Yesim Sucullu Karadag, Yildiz Değirmenci, Zeliha Matur, Nerses Bebek, Murat Emre, Zuhal Yapici

PMC · DOI: 10.1002/acn3.70220 · Annals of Clinical and Translational Neurology · 2025-10-15

## TL;DR

This study explores the clinical and imaging features of BPAN, a rare neurological disorder, using a new case series to better understand its variability and progression.

## Contribution

The study provides new insights into the heterogeneous clinical and neuroimaging features of BPAN across different age groups.

## Key findings

- Cognitive impairment was a consistent finding among BPAN patients, with variable severity.
- FDG-PET imaging showed age-dependent hypometabolism patterns, with cerebellar and pontine involvement in children and frontoparietal in adults.
- EEG abnormalities included age-dependent background slowing and epileptiform discharges, with epilepsy severity decreasing after adolescence.

## Abstract

Neurodegeneration with brain iron accumulation (NBIA) comprises a genetically and clinically heterogeneous group of rare neurological disorders characterized particularly by iron accumulation in the basal ganglia. To date, 15 genes have been associated with NBIA. Among them, WDR45, linked to beta‐propeller protein‐associated neurodegeneration (BPAN), represents the only X‐linked dominant subtype of NBIA. Herein, clinical, electrophysiological, and neuroimaging evaluations were used to broaden the understanding of BPAN in a newly reported case series.

This study included 10 individuals with BPAN, categorized into three age groups. WDR45 variant data retrieved from next‐generation sequencing or Sanger sequencing were reviewed and reassessed. Comprehensive clinical evaluations including magnetic resonance imaging (MRI), fluorodeoxyglucose positron emission tomography (FDG‐PET), and video electroencephalographic monitoring were conducted.

The clinical manifestations were highly heterogeneous, with cognitive impairment being a consistent finding among the patients, with variable severity. The associated WDR45 variants are likely to exert loss‐of‐function effects. Electroencephalogram (EEG) abnormalities included age‐dependent background slowing and epileptiform discharges. MRI indicated a characteristic pattern, while two patients lacked these typical findings. FDG‐PET imaging demonstrated hypometabolism extending beyond cerebral structures, with predominant cerebellar and pontine involvement in pediatric patients and frontoparietal hypometabolism in adults.

This study contributes further to our understanding of the heterogeneous clinical spectrum of BPAN. Genotype–phenotype correlation in BPAN remains unclear due to the absence of sufficiently large cohorts in the literature, including the present study. Nevertheless, even within this small sample, the phenotypic heterogeneity observed among individuals harboring the same genotype highlights the biological complexity of the disease. Neuroimaging findings may reflect progressive and widespread neurological involvement in an age‐dependent pattern, whereas EEG data suggest that epilepsy severity tends to decrease after adolescence.

## Linked entities

- **Genes:** WDR45 (WD repeat domain 45) [NCBI Gene 11152]
- **Diseases:** beta-propeller protein-associated neurodegeneration (MONDO:0010476), BPAN (MONDO:0010476), neurodegeneration with brain iron accumulation (MONDO:0018307), NBIA (MONDO:0018307)

## Full-text entities

- **Genes:** WDR45 (WD repeat domain 45) [NCBI Gene 11152] {aka JM5, NBIA4, NBIA5, WDRX1, WIPI-4, WIPI4}
- **Diseases:** neurological disorders (MESH:D009461), epilepsy (MESH:D004827), NBIA (MESH:D006211), cognitive impairment (MESH:D003072), frontoparietal hypometabolism (MESH:C536673), X-linked dominant (MESH:D040181)
- **Chemicals:** iron (MESH:D007501), FDG (MESH:D019788)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Full text

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## References

42 references — full list in the complete paper: https://tomesphere.com/paper/PMC12968449/full.md

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Source: https://tomesphere.com/paper/PMC12968449