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Reimagining Cross-Functional Design in the Age of AI : A Preliminary Investigation
(2025-06-11) Kahn, Kenneth B.; Candi, Marina; Department of Business and Economics
Being cross-functional in design work can enable effective innovation, though the relevance of ‘being cross-functional’ and the related concept of ‘T-shaped’ individuals could potentially change in the age of artificial intelligence (AI). Reporting results of interviews with design managers, we explore what being cross-functional means for design, the benefits and challenges inherent in cross-functional design work, and AI’s possible impact on the nature of being cross-functional during design activities. Manager responses emphasized the importance of being cross-functional in design work. Noted challenges of cross-functional work include conflicting priorities, differing opinions, unclear roles, loss of design influence, multitasking pressure, and personality differences. Noted benefits include broader viewpoint, creativity versus practicality balance, healthy tension, diverse perspectives, early issue identification, and well-rounded solutions. Regarding the effects of AI, the transformation of cross-functional work by automating routine tasks and enabling deeper data-driven insights is foreseen, but there is disagreement on the degree of change. Some see a shift in the cognitive burden on individuals, allowing them to focus more on creative and integrative tasks, others not so much. All agree that AI tools offer significant opportunities for synthesizing information and managing mundane project management tasks. Managerial and research implications are suggested.
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Melatonin MT1 Receptor Expression in Luminal Invasive Ductal Breast Carcinoma in Postmenopausal Women
(2025-04) Pistiolis, Leda; Alawieh, Sahar; Halldórsdóttir, Þórhildur; Kovács, Anikó; Olofsson Bagge, Roger
Laboratory and animal studies indicate that melatonin exerts a negative impact on breast cancer progression and metastasis. These actions are both receptor-dependent and -independent. Of the two transmembrane melatonin receptors identified in humans, breast cancer expresses only MT1. The aim of this study was to investigate the expression of MT1 in hormone-receptor-positive, HER2-negative invasive ductal breast carcinoma in postmenopausal women and its possible correlations with clinicopathological parameters and survival. A total of 118 patients with luminal A/B primary breast cancer with or without axillary metastases were identified. The MT1 receptor expression was immunohistochemically assessed as a percentage of stained cells and a weighted index (WI) (percentage multiplied by staining intensity). Most tumor samples (84.7%) and metastasized lymph nodes (96%) stained positive for MT1, with varying intensity. No statistically significant correlations were found between the MT1 expression or the WI in the primary tumor and the patient and tumor characteristics, or the MT1 and WI in the metastasized lymph nodes. The survival analysis did not reveal a significant effect of MT1 expression or the WI on the risk of recurrence or survival.
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Impact of different chemical debridement agents on early cellular responses to titanium dental implants : A transcriptome-based in vitro study on peri-implant tissue regeneration
(2025-09) Wang, Qiang; Haugen, Håvard Jostein; Linke, Dirk; Lyngstadaas, Ståle Petter; Sigurjónsson, Ólafur Eysteinn; Ma, Qianli; Department of Engineering
Background: Poor peri-implant health leads to biofilm accumulation, peri-implantitis, and bone loss. Chemical debridement may help maintain peri-implant health, but its effects on peri-implant cells remain unclear. Methods: Five cleaning agents—hydrogen peroxide (H2O2), Poloxamer, H2O2 +Poloxamer, Perisolv, and Paroex—were applied on titanium (Ti) surfaces. Mouse pre-osteoblasts (MC3T3-E1), human gingival fibroblasts (HGF), and human bone marrow stromal cells (hBMSC) were cultured on agent-treated Ti surfaces for up to 120 minutes to assess morphology, cytotoxicity, adhesion, and proliferation. RNA sequencing was performed on hBMSC. Results: Except for Poloxamer, all treatments inhibited cellular spreading. Paroex increased cytotoxicity and inhibited proliferation. Perisolv impaired hBMSC adhesion and variably affected proliferation. H2O2, alone or with Poloxamer, elevated cytotoxicity and inhibited adhesion in hBMSCs but not MC3T3-E1 or HGF. In contrast, Poloxamer-treated Ti surfaces enhanced adhesion and proliferation across all cell types. RNA sequencing revealed that oxidant-based treatments (H2O2, H2O2 +Poloxamer, Perisolv) suppressed key genes for proliferation (HMGA2, JAG1, NOTCH1, YAP1, TBX3), anti-apoptosis (MCL1, BCL2L2), and adhesion (ITGA2, ITGB3, SPP1), while inhibiting MAPK, PI3K-Akt, and pluripotency pathways. Conclusion: Commercial agents like Perisolv and Paroex impair hBMSC function, with Paroex demonstrating significant cytotoxicity. H2O2 exhibits toxicity, particularly to hBMSCs. Poloxamer improves cell attachment and growth. Given these findings, careful selection of debridement agents is critical to balance cleaning efficacy and cytocompatibility. The adverse effects on hBMSCs necessitate prompt removal postapplication. Further research on biomaterials supporting tissue regeneration postdebridement is needed to restore peri-implant health.
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Phase slips extracted from derivatives of EEG data provide a deeper insight into the formation of cortical phase transitions
(2025-02-25) Ramon, Ceon; Gargiulo, Paolo; Department of Engineering
The phase slips are generally extracted from the EEG using Hilbert transforms but could also be extracted from the derivatives of EEG, providing additional information about the formation of cortical phase transitions. We examined this from the 30 s long, 256-channel resting state, eyes open EEG data of a 30-year-old male subject. The phase slip rates, PSR1 from EEG, PSR2 from the first-order derivative of EEG, and PSR3 from the second-order derivative of EEG, respectively, were extracted. The study was performed in the alpha (7-12 Hz) band only. The spatiotemporal plots of the EEG and phase slip rates over a 3.0 s period with a 0.5 s resolution were made with a montage layout of the 256 electrode positions. The spatiotemporal patterns of EEG and its derivatives exhibited shifting activity from posterior visual areas to the central and frontal regions over the 3.0 s period. The PSR1, PSR2, and PSR3 activity areas were different from the EEG and were distributed in larger areas as compared with the EEG and its derivatives. Also, the PSR2 and PSR3 activity areas and magnitudes were significantly different as compared with the PSR1 alone. This was also confirmed (p < 0.01) by the one-way ANOVA analysis of the means of PSR1, PSR2, and PSR3. These results show that PSR2 and PSR3 carry additional information that could potentially be biomarkers for studying the rate of formation of phase slips and the related cortical activity from the derivatives of EEG data.
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Missense variants in FRS3 affect body mass index in populations of diverse ancestries
(2025-03-25) DBDS Genomic Consortium; Jónsdóttir, Andrea Björg; Ægisdóttir, Hildur Margrét; Arnar, Davíð Ottó; Bjarnason, Ragnar Grímur; Halldórsson, Gísli Hreinn; Jónsdóttir, Ingileif; Melsted, Páll; Stefánsdóttir, Lilja; Steingrímsdóttir, Þóra; Teitsdóttir, Unnur Diljá; Þorsteinsdóttir, Unnur; Ulfarsson, Magnus O; Víkingsson, Arnór; Walters, Guðmundur Bragi; Helgason, Agnar Freyr; Halldórsson, Bjarni Vilhjálmur; Stefánsson, Kári
Obesity is associated with adverse effects on health and quality of life. Improved understanding of its underlying pathophysiology is essential for developing counteractive measures. To search for sequence variants with large effects on BMI, we perform a multi-ancestry meta-analysis of 13 genome-wide association studies on BMI, including data derived from 1,534,555 individuals of European ancestry, 339,657 of Asian ancestry, and 130,968 of African ancestry. We identify an intergenic 262,760 base pair deletion at the MC4R locus that associates with 4.11 kg/m2 higher BMI per allele, likely through downregulation of MC4R. Moreover, a rare FRS3 missense variant, p.Glu115Lys, only found in individuals from Finland, associates with 1.09 kg/m2 lower BMI per allele. We also detect three other low-frequency FRS3 missense variants that associate with BMI with smaller effects and are enriched in different ancestries. We characterize FRS3 as a BMI-associated gene, encoding an adaptor protein known to act downstream of BDNF and TrkB, which regulate appetite, food intake, and energy expenditure through unknown signaling pathways. The work presented here contributes to the biological foundation of obesity by providing a convincing downstream component of the BDNF-TrkB pathway, which could potentially be targeted for obesity treatment.

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