Your search keyword '"Brehmer, Yvonne"' showing total 7 results

1. Dopamine Receptor Genes Modulate Associative Memory in Old Age.

Author

Papenberg, Goran, Becker, Nina, Ferencz, Beata, Naveh-Benjamin, Moshe, Laukka, Erika J., Bäckman, Lars, and Brehmer, Yvonne

Subjects

DOPAMINE receptors, ASSOCIATIVE memory (Psychology), PSYCHOLOGICAL aspects of aging, DOPAMINERGIC mechanisms, SHORT-term memory, EXECUTIVE function, COGNITIVE neuroscience

Abstract

Previous research shows that associative memory declines more than itemmemory in aging. Although the underlyingmechanisms of this selective impairment remain poorly understood, animal and human data suggest that dopaminergic modulation may be particularly relevant for associative binding. We investigated the influence of dopamine (DA) receptor genes on item and associative memory in a population-based sample of older adults (n = 525, aged 60 years), assessed with a face-scene item associative memory task. The effects of single-nucleotide polymorphisms of DA D1 (DRD1; rs4532), D2 (DRD2/ANKK1/Taq1A; rs1800497), and D3 (DRD3/Ser9Gly; rs6280) receptor genes were examined and combined into a single genetic score. Individuals carrying more beneficial alleles, presumably associatedwith higher DA receptor efficacy (DRD1 C allele; DRD2 A2 allele; DRD3 T allele), performed better on associativememory than persons with less beneficial genotypes. There were no effects of these genes on item memory or other cognitive measures, such as working memory, executive functioning, fluency, and perceptual speed, indicating a selective association between DA genes and associative memory. By contrast, genetic risk for Alzheimer disease (AD) was associated with worse item and associative memory, indicating adverse effects of APOE ε4 and a genetic risk score for AD (PICALM, BIN1, CLU) on episodic memory in general. Taken together, our results suggest that DA may be particularly important for associative memory, whereas AD-related genetic variations may influence overall episodic memory in older adults without dementia. [ABSTRACT FROM AUTHOR]

Published

2017

2. Neural correlates of training-related working-memory gains in old age

Author

Brehmer, Yvonne, Rieckmann, Anna, Bellander, Martin, Westerberg, Helena, Fischer, Håkan, and Bäckman, Lars

Subjects

*SHORT-term memory, *MEMORY in old age, *MEMORY disorders in old age, *ATTENTION, *COGNITIVE ability, *BRAIN imaging, *MAGNETIC resonance imaging of the brain, *BRAIN physiology

Abstract

Abstract: Working memory (WM) functioning declines in old age. Due to its impact on many higher-order cognitive functions, investigating whether training can modify WM performance has recently been of great interest. We examined the relationship between behavioral performance and neural activity following five weeks of intensive WM training in 23 healthy older adults (M =63.7years). 12 participants received adaptive training (i.e. individually adjusted task difficulty to bring individuals to their performance maximum), whereas the others served as active controls (i.e. fixed low-level practice). Brain activity was measured before and after training, using fMRI, while subjects performed a WM task under two difficulty conditions. Although there were no training-related changes in WM during scanning, neocortical brain activity decreased post training and these decreases were larger in the adaptive training group than in the controls under high WM load. This pattern suggests intervention-related increases in neural efficiency. Further, there were disproportionate gains in the adaptive training group in trained as well as in non-trained (i.e. attention, episodic memory) tasks assessed outside the scanner, indicating the efficacy of the training regimen. Critically, the degree of training-related changes in brain activity (i.e. neocortical decreases and subcortical increases) was related to the maximum gain score achieved during the intervention period. This relationship suggests that the decreased activity, but also specific activity increases, observed were functionally relevant. [Copyright &y& Elsevier]

Published

2011

3. Preliminary evidence that allelic variation in the LMX1A gene influences training-related working memory improvement

Author

Bellander, Martin, Brehmer, Yvonne, Westerberg, Helena, Karlsson, Sari, Fürth, Daniel, Bergman, Olle, Eriksson, Elias, and Bäckman, Lars

Subjects

*SHORT-term memory, *MESENCEPHALON, *DOPAMINE, *DISEASE risk factors, *PARKINSON'S disease, *GENE expression, *TRANSCRIPTION factors, *GENETIC polymorphisms

Abstract

Abstract: LMX1A is a transcription factor involved in the development of dopamine (DA)-producing neurons in midbrain. Previous research has shown that allelic variations in three LMX1A single nucleotide polymorphisms (SNPs) were related to risk of Parkinson''s disease (PD), suggesting that these SNPs may influence the number of mesencephalic DA neurons. Prompted by the established link between striatal DA functions and working memory (WM) performance, we examined two of these SNPs in relation to the ability to benefit from 4 weeks of WM training. One SNP (rs4657412) was strongly associated with the magnitude of training-related gains in verbal WM. The allele linked to larger gains has previously been suggested to be associated with higher dopaminergic nerve cell density. No differential gains of either SNP were observed for spatial WM, and the genotype groups were also indistinguishable in tests of attention, interference control, episodic memory, perceptual speed, and reasoning for both SNPs. This pattern of data is in agreement with previous findings from our group, suggesting that cognitive effects of DA-related genes may be more easily detected in a training context than for single-assessment performance scores. [Copyright &y& Elsevier]

Published

2011

4. Working memory plasticity modulated by dopamine transporter genotype

Author

Brehmer, Yvonne, Westerberg, Helena, Bellander, Martin, Fürth, Daniel, Karlsson, Sari, and Bäckman, Lars

Subjects

*DOPAMINE, *SHORT-term memory, *NEUROPLASTICITY, *GENETIC polymorphisms, *GENETIC regulation, *COMPARATIVE studies, *DOPAMINERGIC mechanisms, *PERFORMANCE evaluation, *COGNITIVE ability

Abstract

Abstract: Dopamine (DA) is implicated in working memory (WM) functioning. Variations in the DA transporter (DAT1) gene (SLC6A3) regulate DA availability in striatum. Compared to DAT1 9/10-repeat carriers, homozygosity of the DAT1 10-repeat allele has been related to less active dopaminergic pathways. A group of younger adults received 4 weeks of computerized adaptive training on several WM tasks. All participants improved their performance as a function of training. However, DAT1 9/10-repeat carriers showed larger training-related gains than DAT1 10-repeat carriers in visuospatial WM. By contrast, the two groups were indistinguishable in baseline WM performance as well as in a variety of tasks assessing different cognitive abilities. This pattern of results provides novel evidence that WM plasticity is a more sensitive indicator of DAT1 gene-related cognitive differences than single-assessment performance scores. [Copyright &y& Elsevier]

Published

2009

5. Behavioral correlates of changes in hippocampal gray matter structure during acquisition of foreign vocabulary.

Author

Bellander, Martin, Berggren, Rasmus, Mårtensson, Johan, Brehmer, Yvonne, Wenger, Elisabeth, Li, Tie-Qiang, Bodammer, Nils C., Shing, Yee-Lee, Werkle-Bergner, Markus, and Lövdén, Martin

Subjects

*HIPPOCAMPUS physiology, *GRAY matter (Nerve tissue), *LOANWORDS, *EPISODIC memory, *SHORT-term memory, *MAGNETIC resonance imaging of the brain, *COGNITIVE testing

Abstract

Experience can affect human gray matter volume. The behavioral correlates of individual differences in such brain changes are not well understood. In a group of Swedish individuals studying Italian as a foreign language, we investigated associations among time spent studying, acquired vocabulary, baseline performance on memory tasks, and gray matter changes. As a way of studying episodic memory training, the language learning focused on acquiring foreign vocabulary and lasted for 10 weeks. T 1 -weighted structural magnetic resonance imaging and cognitive testing were performed before and after the studies. Learning behavior was monitored via participants' use of a smartphone application dedicated to the study of vocabulary. A whole-brain analysis showed larger changes in gray matter structure of the right hippocampus in the experimental group (N = 33) compared to an active control group (N = 23). A first path analyses revealed that time spent studying rather than acquired knowledge significantly predicted change in gray matter structure. However, this association was not significant when adding performance on baseline memory measures into the model, instead only the participants' performance on a short-term memory task with highly similar distractors predicted the change. This measure may tap similar individual difference factors as those involved in gray matter plasticity of the hippocampus. [ABSTRACT FROM AUTHOR]

Published

2016

6. Dopamine D1 receptors and age differences in brain activation during working memory

Author

Bäckman, Lars, Karlsson, Sari, Fischer, Håkan, Karlsson, Per, Brehmer, Yvonne, Rieckmann, Anna, MacDonald, Stuart W.S., Farde, Lars, and Nyberg, Lars

Subjects

*SHORT-term memory, *DOPAMINE receptors, *AGE differences, *BRAIN stimulation, *PREFRONTAL cortex, *NEURAL transmission, *AGING

Abstract

Abstract: In an fMRI study, 20 younger and 20 healthy older adults were scanned while performing a spatial working-memory task under two levels of load. On a separate occasion, the same subjects underwent PET measurements using the radioligand [11C] SCH23390 to determine dopamine D1 receptor binding potential (BP) in caudate nucleus and dorsolateral prefrontal cortex (DLPFC). The fMRI study revealed a significant load modulation of brain activity (higher load>lower load) in frontal and parietal regions for younger, but not older, adults. The PET measurements showed marked age-related reductions of D1 BP in caudate and DLPFC. Statistical control of caudate and DLPFC D1 binding eliminated the age-related reduction in load-dependent BOLD signal in left frontal cortex, and attenuated greatly the reduction in right frontal and left parietal cortex. These findings suggest that age-related alterations in dopaminergic neurotransmission may contribute to underrecruitment of task-relevant brain regions during working-memory performance in old age. [Copyright &y& Elsevier]

Published

2011

7. Simulating Neurocognitive Aging: Effects of a Dopaminergic Antagonist on Brain Activity During Working Memory

Author

Fischer, Håkan, Nyberg, Lars, Karlsson, Sari, Karlsson, Per, Brehmer, Yvonne, Rieckmann, Anna, MacDonald, Stuart W.S., Farde, Lars, and Bäckman, Lars

Subjects

*DOPAMINERGIC mechanisms, *SHORT-term memory, *POSITRON emission tomography, *BRAIN, *AGING, *DOPAMINE, *EFFECT of drugs on the brain, *NEUROPHARMACOLOGY, *MAGNETIC resonance imaging of the brain

Abstract

Background: Previous correlational studies have indirectly linked dysfunctional dopaminergic neurotransmission to age-related cognitive deficits and associated reductions in task-induced functional brain activity. Methods: We used an experimental-pharmacological functional magnetic resonance imaging (fMRI) approach to more directly examine the role of dopamine in neurocognitive aging. Twenty younger and 20 healthy older adults were included. During fMRI scanning, a spatial working memory (SWM) task was administered under two conditions, varying in cognitive load. Positron emission tomography measurements with the D1 receptor antagonist [11C]SCH23390 confirmed that a given experimental dose of unlabeled solution occupied 50% of D1 receptors in younger adults. Results: An age-related reduction in SWM performance was observed, and fMRI data revealed that, relative to younger adults under placebo conditions, elderly persons under-recruited load-sensitive fronto-parietal regions during SWM. Critically, in younger adults, the D1 antagonist resulted in a similar reduction in SWM performance and fMRI response. Conclusions: These results suggest that depletion of dopamine, whether ontogenetically or pharmacologically, results in decreased SWM performance as well as reduced load-dependent modulation of the blood oxygen level dependent signal in fronto-parietal regions, possibly by decreasing the signal-to-noise ratio in relevant neural networks. [Copyright &y& Elsevier]

Published

2010