The goal of the proposed study is to elucidate neurologic and neuropsychological improvements associated with Palynziq-related reduction in plasma Phe levels in individuals with PKU. To this end, investigators will utilize state-of-the-art neuropsychological and multi-modal neuroimaging methods to examine the effects of large Phe level reduction (levels \<360 μmol/L for at least 3 consecutive months) on GM and WM brain structures, brain concentrations of Phe, functionality of brain networks, and associated cognitive functioning in a sample of individuals with PKU who are being treated with Palyzniq.
Past studies have documented PKU-related disruptions in brain phenylalanine (Phe) levels, white matter (WM) and gray matter (GM) brain structures, functional connectivity, and neurocognitive functioning. Additional research suggests that the disruptive effects of excessive blood Phe levels likely contribute to these abnormalities, and treatment aimed at lower Phe levels may lead to significant improvements. Within this context, the primary aim is to test the hypotheses that Palynziq-related reductions in blood Phe levels will be associated with: 1. A decrease in brain Phe levels as measured by magnetic resonance spectroscopy (MRS). 2. A decrease in the extent and severity of WM abnormalities as evidenced by increased mean diffusivity values - a measure of microstructural WM integrity that is derived via diffusion-weighted magnetic resonance imaging (MRI) and diffusion tensor imaging (DTI). 3. Closer-to-normal volumetric measurements for GM structures. Nature of this effect will be dependent on structure. For example, PKU is associated with increased volume in basal ganglia but decreased volume in posterior cortex and cerebellum (Aldridge et al., 2020; Bodner et al., 2012; Christ et al., 2016). 4. An increase in functional connectivity within the brain's functional networks as measured by resting state functional MRI (fMRI). 5. Improved performance on neurocognitive tests of executive function, attention, processing speed, and motor control. To accomplish this aim, a total sample of up to 13 adults with PKU who have previously completed baseline (pre-Palnyziq) neurocognitive and neuroimaging evaluations will be recruited from the two sites (University of Missouri, Boston Children's Hospital). Participants will be reassessed following a significant and prolonged Phe response to Palynziq (as reflected by at least 3 consecutive months of Phe levels below 360 μmol/L).
Study Type
OBSERVATIONAL
Enrollment
6
Participants will have been prescribed pegvaliase-pqpz (Palynziq) by their primary metabolic care providers as part of their standard care. \[Note that prescription and standard care are independent of the present study.\]
Boston Children's Hospital
Boston, Massachusetts, United States
University of Missouri
Columbia, Missouri, United States
Neurologic Integrity
Brain phenylalanine (Phe) levels, white matter integrity, gray matter integrity, functional connectivity as measured using magnetic resonance imaging (MRI)
Time frame: Single timepoint for 1 hour
Neuropsychological Functioning
Neuropsychological functioning as assessed using a comprehensive battery of standardized neuropsychological tests
Time frame: Single timepoint for 2 hours
Cookie Theft Picture Test
Verbal linguistics as assessed using the Cookie Theft Picture Test from the Boston Diagnostic Aphasia Exam
Time frame: Single timepoint for 10 minutes
In-the-moment Psychoemotional Symptomatology
Cell phone-based ecological momentary assessment (EMA) to measure in-the-moment psychoemotional symptomatology
Time frame: 30 minutes total per day for 7 consecutive days
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