TY - GEN A1 - Herold, Fabian A1 - Labott, Berit K. A1 - Grässler, Bernhard A1 - Halfpaap, Nicole A1 - Langhans, Corinna A1 - Müller, Patrick A1 - Ammar, Achraf A1 - Dordevic, Milos A1 - Hökelmann, Anita A1 - Müller, Notger Germar T1 - A Link between Handgrip Strength and Executive Functioning: A Cross-Sectional Study in Older Adults with Mild Cognitive Impairment and Healthy Controls T2 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe N2 - Older adults with amnestic mild cognitive impairment (aMCI) who in addition to their memory deficits also suffer from frontal-executive dysfunctions have a higher risk of developing dementia later in their lives than older adults with aMCI without executive deficits and older adults with non-amnestic MCI (naMCI). Handgrip strength (HGS) is also correlated with the risk of cognitive decline in the elderly. Hence, the current study aimed to investigate the associations between HGS and executive functioning in individuals with aMCI, naMCI and healthy controls. Older, right-handed adults with amnestic MCI (aMCI), non-amnestic MCI (naMCI), and healthy controls (HC) conducted a handgrip strength measurement via a handheld dynamometer. Executive functions were assessed with the Trail Making Test (TMT A&B). Normalized handgrip strength (nHGS, normalized to Body Mass Index (BMI)) was calculated and its associations with executive functions (operationalized through z-scores of TMT B/A ratio) were investigated through partial correlation analyses (i.e., accounting for age, sex, and severity of depressive symptoms). A positive and low-to-moderate correlation between right nHGS (rp (22) = 0.364; p = 0.063) and left nHGS (rp (22) = 0.420; p = 0.037) and executive functioning in older adults with aMCI but not in naMCI or HC was observed. Our results suggest that higher levels of nHGS are linked to better executive functioning in aMCI but not naMCI and HC. This relationship is perhaps driven by alterations in the integrity of the hippocampal-prefrontal network occurring in older adults with aMCI. Further research is needed to provide empirical evidence for this assumption. T3 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe - 775 KW - MCI KW - hippocampal-prefrontal network KW - handgrip strength KW - exercise cognition KW - aging KW - brain health Y1 - 2022 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-559251 SN - 1866-8364 SP - 1 EP - 14 PB - Universitätsverlag Potsdam CY - Potsdam ER - TY - GEN A1 - Stelzel, Christine A1 - Schauenburg, Gesche A1 - Rapp, Michael Armin A1 - Heinzel, Stephan A1 - Granacher, Urs T1 - Age-Related Interference between the Selection of Input-Output Modality Mappings and Postural Control BT - a Pilot Study N2 - Age-related decline in executive functions and postural control due to degenerative processes in the central nervous system have been related to increased fall-risk in old age. Many studies have shown cognitive-postural dual-task interference in old adults, but research on the role of specific executive functions in this context has just begun. In this study, we addressed the question whether postural control is impaired depending on the coordination of concurrent response-selection processes related to the compatibility of input and output modality mappings as compared to impairments related to working-memory load in the comparison of cognitive dual and single tasks. Specifically, we measured total center of pressure (CoP) displacements in healthy female participants aged 19–30 and 66–84 years while they performed different versions of a spatial one-back working memory task during semi-tandem stance on an unstable surface (i.e., balance pad) while standing on a force plate. The specific working-memory tasks comprised: (i) modality compatible single tasks (i.e., visual-manual or auditory-vocal tasks), (ii) modality compatible dual tasks (i.e., visual-manual and auditory-vocal tasks), (iii) modality incompatible single tasks (i.e., visual-vocal or auditory-manual tasks), and (iv) modality incompatible dual tasks (i.e., visual-vocal and auditory-manual tasks). In addition, participants performed the same tasks while sitting. As expected from previous research, old adults showed generally impaired performance under high working-memory load (i.e., dual vs. single one-back task). In addition, modality compatibility affected one-back performance in dual-task but not in single-task conditions with strikingly pronounced impairments in old adults. Notably, the modality incompatible dual task also resulted in a selective increase in total CoP displacements compared to the modality compatible dual task in the old but not in the young participants. These results suggest that in addition to effects of working-memory load, processes related to simultaneously overcoming special linkages between input- and output modalities interfere with postural control in old but not in young female adults. Our preliminary data provide further evidence for the involvement of cognitive control processes in postural tasks. T3 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe - 322 KW - aging KW - cognitive-postural dual task KW - modality compatibility KW - postural stability KW - working memory Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-395733 ER - TY - GEN A1 - Mell, Thomas A1 - Wartenburger, Isabell A1 - Marschner, Alexander A1 - Villringer, Arno A1 - Reischies, Friedel M. A1 - Heekeren, Hauke R. T1 - Altered function of ventral striatum during reward-based decision making in old age N2 - Normal aging is associated with a decline in different cognitive domains and local structural atrophy as well as decreases in dopamine concentration and receptor density. To date, it is largely unknown how these reductions in dopaminergic neurotransmission affect human brain regions responsible for reward-based decision making in older adults. Using a learning criterion in a probabilistic object reversal task, we found a learning stage by age interaction in the dorsolateral prefrontal cortex (dIPFC) during decision making. While young adults recruited the dlPFC in an early stage of learning reward associations, older adults recruited the dlPFC when reward associations had already been learned. Furthermore, we found a reduced change in ventral striatal BOLD signal in older as compared to younger adults in response to high probability rewards. Our data are in line with behavioral evidence that older adults show altered stimulus-reward learning and support the view of an altered fronto-striatal interaction during reward-based decision making in old age, which contributes to prolonged learning of reward associations. T3 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe - paper 182 KW - aging KW - fMRI KW - reward association learning KW - ventral striatum KW - decision making KW - dorsolateral prefrontal cortex Y1 - 2009 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus-45235 ER - TY - THES A1 - Junker, Martina T1 - Der verflixte Akkusativ : Altersunterschiede und Altersinvarianz beim Verstehen von Sätzen mit unterschiedlich komplexer syntaktischer Struktur T1 - Tricky accusative : age-related differences in comprehension of sentences with different syntactical structure N2 - In dieser Arbeit wird in mehreren Experimenten untersucht, wie gut junge und alte Erwachsene Sätze mit unterschiedlich komplexer syntaktischer Struktur verstehen können. Zentrales Thema dabei sind die Schwierigkeiten, die ältere Erwachsene mit der Objekt-vor-Subjekt-Wortstellung haben. Untersucht wird, inwiefern diese beobachteten Altersunterschiede durch eine reduzierte verbale Arbeitsgedächtniskapazität der älteren Erwachsenen erklärt werden können. Dabei stellt sich die Frage, ob die Defizite ein generelles verbales Arbeitsgedächtnis betreffen oder ob es ein eigenes Verarbeitungs-system für syntaktische Informationen gibt, dessen Kapazität mit dem Alter abnimmt. Es wurde versucht, die postulierte reduzierte Arbeitsgedächtniskapazität der älteren Erwachsenen an jungen Erwachsenen zu simulieren, indem deren Arbeitsgedächtniska-pazität durch eine Zusatzaufgabe künstlich eingeschränkt wurde. Weiterhin wurden die Altersunterschiede bei syntaktisch komplexen zentraleingebetteten Relativsätzen mit denen bei syntaktisch einfacheren koordinierten Hauptsätzen verglichen. Um die Studienteilnehmer mit den seltenen objektinitialen Strukturen zu konfrontieren und ihre Erfahrung mit solchen Sätzen zu verändern, wurden schließlich sowohl junge als auch alte Erwachsene mit Sätzen mit Objekt-vor-Subjekt-Wortstellung trainiert. N2 - In this paper several experiments about age differences in comprehension of sentences with different syntactical structure are reported. The main focus is on the difficulties old adults experience when a sentence starts with an object. Can the age differences be explained by differences in working memory capacity? Have old adults less working memory capacity, or does there exist a separate working memory for syntactic information which declines with age? In an age simulation, young adults working memory capacity was reduced by an additional digit load. Age differences in comprehension of syntactical complex sentences were compared with age differences in sentences with less complex syntactical structure. To change their experience with the rare object initial word order participants were trained with object initial sentences. KW - Gerontologie KW - Psycholinguistik KW - Arbeitsgedächtnis KW - aging KW - speech processing KW - working memory Y1 - 2004 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus-3784 ER - TY - GEN A1 - Zouita, Sghaier A1 - Zouhal, Hassane A1 - Ferchichi, Habiba A1 - Paillard, Thierry A1 - Dziri, Catherine A1 - Hackney, Anthony C. A1 - Laher, Ismail A1 - Granacher, Urs A1 - Ben Moussa Zouita, Amira T1 - Effects of Combined Balance and Strength Training on Measures of Balance and Muscle Strength in Older Women With a History of Falls T2 - Postprints der Universität Potsdam : Humanwissenschaftliche Reihe N2 - Objective: We investigated the effects of combined balance and strength training on measures of balance and muscle strength in older women with a history of falls. Methods: Twenty-seven older women aged 70.4 ± 4.1 years (age range: 65 to 75 years) were randomly allocated to either an intervention (IG, n = 12) or an active control (CG, n = 15) group. The IG completed 8 weeks combined balance and strength training program with three sessions per week including visual biofeedback using force plates. The CG received physical therapy and gait training at a rehabilitation center. Training volumes were similar between the groups. Pre and post training, tests were applied for the assessment of muscle strength (weight-bearing squat [WBS] by measuring the percentage of body mass borne by each leg at different knee flexions [0°, 30°, 60°, and 90°], sit-to-stand test [STS]), and balance. Balance tests used the modified clinical test of sensory interaction (mCTSIB) with eyes closed (EC) and opened (EO), on stable (firm) and unstable (foam) surfaces as well as spatial parameters of gait such as step width and length (cm) and walking speed (cm/s). Results: Significant group × time interactions were found for different degrees of knee flexion during WBS (0.0001 < p < 0.013, 0.441 < d < 0.762). Post hoc tests revealed significant pre-to-post improvements for both legs and for all degrees of flexion (0.0001 < p < 0.002, 0.697 < d < 1.875) for IG compared to CG. Significant group × time interactions were found for firm EO, foam EO, firm EC, and foam EC (0.006 < p < 0.029; 0.302 < d < 0.518). Post hoc tests showed significant pre-to-post improvements for both legs and for all degrees of oscillations (0.0001 < p < 0.004, 0.753 < d < 2.097) for IG compared to CG. This study indicates that combined balance and strength training improved percentage distribution of body weight between legs at different conditions of knee flexion (0°, 30°, 60°, and 90°) and also decreased the sway oscillation on a firm surface with eyes closed, and on foam surface (with eyes opened or closed) in the IG. Conclusion: The higher positive effects of training seen in standing balance tests, compared with dynamic tests, suggests that balance training exercises including lateral, forward, and backward exercises improved static balance to a greater extent in older women. T3 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe - 699 KW - aging KW - exercise KW - postural sway KW - force KW - tasks Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-490932 SN - 1866-8364 IS - 699 ER - TY - GEN A1 - Baesler, Jessica A1 - Michaelis, Vivien A1 - Stiboller, Michael A1 - Haase, Hajo A1 - Aschner, Michael A1 - Schwerdtle, Tanja A1 - Sturzenbaum, Stephen R. A1 - Bornhorst, Julia T1 - Nutritive manganese and zinc overdosing in aging c. elegans result in a metallothionein-mediated alteration in metal homeostasis T2 - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe N2 - Manganese (Mn) and zinc (Zn) are not only essential trace elements, but also potential exogenous risk factors for various diseases. Since the disturbed homeostasis of single metals can result in detrimental health effects, concerns have emerged regarding the consequences of excessive exposures to multiple metals, either via nutritional supplementation or parenteral nutrition. This study focuses on Mn-Zn-interactions in the nematode Caenorhabditis elegans (C. elegans) model, taking into account aspects related to aging and age-dependent neurodegeneration. T3 - Zweitveröffentlichungen der Universität Potsdam : Mathematisch-Naturwissenschaftliche Reihe - 1364 KW - aging KW - C. elegans KW - homeostasis KW - manganese KW - zinc Y1 - 2021 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-514995 SN - 1866-8372 IS - 8 ER - TY - THES A1 - Kehm, Richard T1 - The impact of metabolic stress and aging on functionality and integrity of pancreatic islets and beta-cells T1 - Der Einfluss von metabolischem Stress und Alterung auf die Funktionalität und Integrität von Langerhans-Inseln und β-Zellen N2 - The increasing age of worldwide population is a major contributor for the rising prevalence of major pathologies and disease, such as type 2 diabetes, mediated by massive insulin resistance and a decline in functional beta-cell mass, highly associated with an elevated incidence of obesity. Thus, the impact of aging under physiological conditions and in combination with diet-induced metabolic stress on characteristics of pancreatic islets and beta-cells, with the focus on functionality and structural integrity, were investigated in the present dissertation. Primarily induced by malnutrition due to chronic and excess intake of high caloric diets, containing large amounts of carbohydrates and fats, obesity followed by systemic inflammation and peripheral insulin resistance occurs over time, initiating metabolic stress conditions. Elevated insulin demands initiate an adaptive response by beta-cell mass expansion due to increased proliferation, but prolonged stress conditions drive beta-cell failure and loss. Aging has been also shown to affect beta-cell functionality and morphology, in particular by proliferative limitations. However, most studies in rodents were performed under beta-cell challenging conditions, such as high-fat diet interventions. Thus, in the first part of the thesis (publication I), a characterization of age-related alterations on pancreatic islets and beta-cells was performed by using plasma samples and pancreatic tissue sections of standard diet-fed C57BL/6J wild-type mice in several age groups (2.5, 5, 10, 15 and 21 months). Aging was accompanied by decreased but sustained islet proliferative potential as well as an induction of cellular senescence. This was associated with a progressive islet expansion to maintain normoglycemia throughout lifespan. Moreover, beta-cell function and mass were not impaired although the formation and accumulation of AGEs occurred, located predominantly in the islet vasculature, accompanied by an induction of oxidative and nitrosative (redox) stress. The nutritional behavior throughout human lifespan; however, is not restricted to a balanced diet. This emphasizes the significance to investigate malnutrition by the intake of high-energy diets, inducing metabolic stress conditions that synergistically with aging might amplify the detrimental effects on endocrine pancreas. Using diabetes-prone NZO mice aged 7 weeks, fed a dietary regimen of carbohydrate restriction for different periods (young mice - 11 weeks, middle-aged mice - 32 weeks) followed by a carbohydrate intervention for 3 weeks, offered the opportunity to distinguish the effects of diet-induced metabolic stress in different ages on the functionality and integrity of pancreatic islets and their beta-cells (publication II, manuscript). Interestingly, while young NZO mice exhibited massive hyperglycemia in response to diet-induced metabolic stress accompanied by beta-cell dysfunction and apoptosis, middle-aged animals revealed only moderate hyperglycemia by the maintenance of functional beta-cells. The loss of functional beta-cell mass in islets of young mice was associated with reduced expression of PDX1 transcription factor, increased endocrine AGE formation and related redox stress as well as TXNIP-dependent induction of the mitochondrial death pathway. Although the amounts of secreted insulin and the proliferative potential were comparable in both age groups, islets of middle-aged mice exhibited sustained PDX1 expression, almost regular insulin secretory function, increased capacity for cell cycle progression as well as maintained redox potential. The results of the present thesis indicate a loss of functional beta-cell mass in young diabetes-prone NZO mice, occurring by redox imbalance and induction of apoptotic signaling pathways. In contrast, aging under physiological conditions in C57BL/6J mice and in combination with diet-induced metabolic stress in NZO mice does not appear to have adverse effects on the functionality and structural integrity of pancreatic islets and beta-cells, associated with adaptive responses on changing metabolic demands. However, considering the detrimental effects of aging, it has to be assumed that the compensatory potential of mice might be exhausted at a later point of time, finally leading to a loss of functional beta-cell mass and the onset and progression of type 2 diabetes. The polygenic, diabetes-prone NZO mouse is a suitable model for the investigation of human obesity-associated type 2 diabetes. However, mice at advanced age attenuated the diabetic phenotype or do not respond to the dietary stimuli. This might be explained by the middle age of mice, corresponding to the human age of about 38-40 years, in which the compensatory mechanisms of pancreatic islets and beta cells towards metabolic stress conditions are presumably more active. N2 - Das steigende Alter der Weltbevölkerung ist ein wesentlicher Faktor für die zunehmende Prävalenz bedeutsamer Pathologien und Krankheiten, wie dem Typ-2-Diabetes, der durch eine massive Insulinresistenz und eine Abnahme der funktionellen Beta-Zellmasse hervorgerufen wird und in hohem Maße mit einem verstärkten Auftreten von Fettleibigkeit assoziiert ist. Daher wurde in der vorliegenden Dissertation der Einfluss der Alterung unter physiologischen Bedingungen und in Kombination mit ernährungs-bedingtem, metabolischem Stress auf die Eigenschaften von Langerhans-Inseln und Beta-Zellen, mit dem Schwerpunkt auf Funktionalität und strukturelle Integrität, untersucht. Primär induziert durch Fehlernährung infolge des chronischen und übermäßigen Konsums von kalorienreichen Diäten, die große Mengen an Kohlenhydraten und Fetten enthalten, kann Adipositas, gefolgt von systemischen Entzündungen und peripherer Insulinresistenz, im Laufe des Lebens entstehen und metabolische Stresszustände auslösen. Daraus resultiert ein erhöhter Insulinbedarf, der eine adaptive Reaktion durch die Vergrößerung der Beta-Zellmasse infolge gesteigerter Proliferation auslöst. Längere Stressbedingungen führen hingegen zu Schäden an und Verlust von Beta-Zellen. Es wurde zudem gezeigt, dass das Altern die Funktionalität und Morphologie von Beta-Zellen, insbesondere durch proliferative Limitationen, beeinflusst. Die meisten Studien in Nagetieren wurden jedoch unter erhöhten Stressbedingungen für Beta-Zellen, beispielsweise durch die Fütterung von Hochfett-Diäten, durchgeführt. Deshalb wurde im ersten Teil der Arbeit (Publikation I) eine Charakterisierung von altersbedingten Veränderungen auf die Langerhans-Inseln und Beta-Zellen unter Verwendung von Plasmaproben und Pankreasgewebeschnitten von C57BL/6J-Wildtyp-Mäusen verschiedener Altersgruppen (2,5; 5; 10; 15 und 21 Monate), die mit einer Standarddiät gefüttert wurden, durchgeführt. Das Altern ging mit einem reduzierten, jedoch anhaltenden Proliferationspotential der Langerhans-Inseln sowie einer Induktion der zellulären Seneszenz einher. Dies war mit einem fortschreitenden Wachstum der Langerhans-Inseln verbunden, um eine Normoglykämie während der gesamten Lebensdauer aufrechtzuerhalten. Zudem wurden die Beta-Zell-Masse und die Funktionalität nicht beeinträchtigt, obwohl eine Bildung und Akkumulation von AGEs, die vorwiegend im Gefäßsystem der Langerhans-Inseln lokalisiert und von einer Induktion von oxidativem und nitrosativem (redox) Stress begleitet war, auftrat. Das Ernährungsverhalten während der gesamten Lebensspanne ist jedoch nicht auf eine ausgewogene Ernährung beschränkt. Dies unterstreicht die Bedeutung der Untersuchung von Fehlernährung durch die Einnahme energiereicher Diäten, wodurch metabolische Stresszustände induziert werden, die synergistisch mit dem Altern schädigende Effekte auf das endokrine Pankreas verstärken können. Verwendet wurden 7 Wochen alte, zur Entwicklung von Typ-2-Diabetes neigende NZO-Mäuse, die unterschiedlich langen kohlenhydratrestriktiven Fütterungsperioden (junge Mäuse - 11 Wochen, Mäuse mittleren Alters - 32 Wochen), gefolgt von einer 3-wöchigen Kohlenhydratintervention ausgesetzt waren. Dadurch konnten die Auswirkungen von ernährungsbedingtem metabolischem Stress auf die Funktionalität und Integrität von Langerhans-Inseln und deren Beta-Zellen in verschiedenen Altersstufen untersucht werden (Publikation II, Manuskript). Interessanterweise zeigten junge NZO-Mäuse eine massive Hyperglykämie als Reaktion auf den ernährungsbedingten, metabolischen Stress was von Beta-Zelldysfunktion und Apoptose begleitet war. Tiere mittleren Alters zeigten hingegen nur eine moderate Hyperglykämie durch den Erhalt funktioneller Beta-Zellen. Der Verlust funktioneller Beta-Zellmasse in jungen Mäusen war mit einer verminderten Expression des PDX1-Transkriptionsfaktors, einer erhöhten endokrinen AGE-Bildung und damit verbundenem Redox Stress sowie einer TXNIP-abhängigen Induktion des mitochondrialen Apoptosewegs verbunden. Obwohl die Mengen an sekretiertem Insulin sowie das Proliferationspotential in beiden Altersgruppen vergleichbar waren, zeigten die Langerhans-Inseln der Mäuse im mittleren Alter eine anhaltende PDX1-Expression, eine nahezu reguläre Insulinsekretionsfunktion, eine erhöhte Kapazität für das Fortschreiten des Zellzyklus sowie einen Erhalt des Redoxpotentials. Die Ergebnisse der vorliegenden Arbeit zeigen einen Verlust funktioneller Beta-Zellmasse bei jungen, diabetogenen NZO-Mäusen, der durch ein Redox-Ungleichgewicht und die Induktion apoptotischer Signalwege verursacht wurde. Im Gegensatz dazu scheint das Altern unter physiologischen Bedingungen bei C57BL/6J-Mäusen und in Kombination mit ernährungsbedingtem metabolischem Stress bei NZO-Mäusen keine nachteiligen Auswirkungen auf die Funktionalität und strukturelle Integrität von Langerhans und Beta-Zellen zu haben, was mit adaptiven Reaktionen auf wechselnde Stoffwechsel-anforderungen assoziiert war. In Anbetracht der negativen Auswirkungen der Alterung muss jedoch berücksichtigt werden, dass das Kompensationsverhalten von Mäusen zu einem späteren Zeitpunkt erschöpft sein könnte, was schließlich zu einem Verlust der funktionellen Beta-Zellmasse und dem Auftreten und Fortschreiten von Typ-2-Diabetes führt. Die polygene, zu Typ-2-Diabetes neigende NZO-Maus ist ein geeignetes Modell für die Untersuchung von mit Adipositas-assoziiertem Typ-2-Diabetes beim Menschen. Mäuse im fortgeschrittenen Alter zeigten jedoch einen verminderten diabetischen Phänotyp oder reagierten nicht auf die diätetischen Reize. Dies könnte durch das mittlere Alter der Mäuse erklärt werden, das dem menschlichen Alter von etwa 38 bis 40 Jahren entspricht, in dem die Kompensationsmechanismen von Langerhans-Inseln und Beta-Zellen gegenüber metabolischen Stressbedingungen möglicherweise aktiver sind. KW - Alterung KW - aging KW - Beta-Zelle KW - beta-cell KW - metabolischer Stress KW - metabolic stress Y1 - 2019 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-441099 ER - TY - GEN A1 - Heinzel, Stephan A1 - Rimpel, Jérôme A1 - Stelzel, Christine A1 - Rapp, Michael Armin T1 - Transfer Effects to a Multimodal Dual-Task after Working Memory Training and Associated Neural Correlates in Older Adults BT - A Pilot Study N2 - Working memory (WM) performance declines with age. However, several studies have shown that WM training may lead to performance increases not only in the trained task, but also in untrained cognitive transfer tasks. It has been suggested that transfer effects occur if training task and transfer task share specific processing components that are supposedly processed in the same brain areas. In the current study, we investigated whether single-task WM training and training-related alterations in neural activity might support performance in a dual-task setting, thus assessing transfer effects to higher-order control processes in the context of dual-task coordination. A sample of older adults (age 60–72) was assigned to either a training or control group. The training group participated in 12 sessions of an adaptive n-back training. At pre and post-measurement, a multimodal dual-task was performed in all participants to assess transfer effects. This task consisted of two simultaneous delayed match to sample WM tasks using two different stimulus modalities (visual and auditory) that were performed either in isolation (single-task) or in conjunction (dual-task). A subgroup also participated in functional magnetic resonance imaging (fMRI) during the performance of the n-back task before and after training. While no transfer to single-task performance was found, dual-task costs in both the visual modality (p < 0.05) and the auditory modality (p < 0.05) decreased at post-measurement in the training but not in the control group. In the fMRI subgroup of the training participants, neural activity changes in left dorsolateral prefrontal cortex (DLPFC) during one-back predicted post-training auditory dual-task costs, while neural activity changes in right DLPFC during three-back predicted visual dual-task costs. Results might indicate an improvement in central executive processing that could facilitate both WM and dual-task coordination. T3 - Zweitveröffentlichungen der Universität Potsdam : Humanwissenschaftliche Reihe - 343 KW - aging KW - cognitive training KW - dual-task KW - fMRI KW - modality KW - neuroimaging KW - transfer KW - working memory Y1 - 2017 U6 - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:kobv:517-opus4-401921 ER -