4.5 Article

Changes in cognitive functions and cerebral grey matter and their associations with inflammatory markers, endocrine markers, and APOE genotypes in testicular cancer patients undergoing treatment

Journal

BRAIN IMAGING AND BEHAVIOR
Volume 11, Issue 3, Pages 769-783

Publisher

SPRINGER
DOI: 10.1007/s11682-016-9552-3

Keywords

Cancer; Testicular cancer; Germ cell tumor; Cognition; Neuropsychological function; Neurocognitive function; Voxel-based morphometry; MRI; Cytokine; Cortisol; APOE

Categories

Funding

  1. Danish Cancer Society [R17-A698]
  2. Savaerksejer Jeppe Juhls og Hustru Ovita Juhls Mindelegat
  3. National Cancer Institute of the National Institutes of Health [7K07CA184145-02]
  4. Lundbeck Foundation
  5. Lundbeck Foundation [R155-2014-1724] Funding Source: researchfish
  6. The Danish Cancer Society [R124-A7904] Funding Source: researchfish

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Evidence suggests that testicular cancer (TC) and its treatment are associated with cognitive impairment. However, the underlying neural substrate and biological mechanisms are poorly understood. This study aimed to investigate changes in cognition and brain grey matter (GM) morphology in TC patients undergoing treatment, and to explore associations with immune markers, endocrine markers, and genotype. Sixty-five patients with stage I-III TC underwent assessment after surgery but prior to further treatment and again 6 months after. Twenty-two patients received chemotherapy (+CT), while 43 did not (-CT). Assessments included neuropsychological testing, whole-brain magnetic resonance imaging, and blood samples. Twenty-five healthy controls (HCs) underwent neuropsychological testing with a matching time interval. A regression-based approach was used to determine cognitive changes and longitudinal voxel-based morphometry (VBM) was performed to investigate changes in GM density in the TC groups. Compared with the HCs, both TC groups showed higher rates of cognitive decline (p < 0.05). A trend towards greater decline was observed in + CT (63.6 %) compared with -CT patients (39.5 %) (p = 0.07). VBM revealed widespread GM reductions in both TC groups, but a group-by-time interaction analysis revealed prefrontal reductions specific to the + CT group (p = 0.02), which were associated with poorer cognitive performance. Poorer cognitive performance was also associated with an increase in tumor necrosis factor alpha in + CT patients. Furthermore, an interaction effect was found between the APOE epsilon 4 genotype and chemotherapy on cognitive performance with epsilon 4 carriers performing significantly worse. These findings provide novel evidence of changes in cognition and brain morphology in TC patients undergoing treatment.

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