Your search keyword '"focal adhesions"' showing total 151 results

1. Facilitation of mucosal healing by estrogen receptor β in ulcerative colitis through suppression of branched-chain amino acid transport and subsequent triggering of autophagy in colonic epithelial cells.

Author

Guo, Yilei, Zhu, Yanrong, Zhang, Jing, He, Yue, Zhao, Mianjiang, Lin, Haochang, Wei, Zhifeng, Xia, Yufeng, and Dai, Yue

Subjects

FOCAL adhesion kinase, AMINO acid transport, ULCERATIVE colitis, CELL migration, FOCAL adhesions

Abstract

Colonic mucosal healing is the ultimate goal of ulcerative colitis (UC) treatment, but it remains difficult to realize. Given the higher incidence of UC in males and the beneficial effect of estrogen on UC, we conducted this study to examine the therapeutic potential of estrogen receptor β (ER β), the primary ER subtype in colon, on mucosal healing in UC. Our study is the first to report that ER β activation degree was positively correlated with mucosal healing in patients with UC. Furthermore, ER β activation enhanced mucosal healing in mice with dextran sulfate sodium-induced and biopsy-induced colonic injuries. Mechanistically, ER β activation promoted autophagy of colonic epithelial cells by inhibiting branched-chain amino acid transport, leading to focal adhesion kinase (FAK) activation. Activated FAK promoted focal adhesion turnover and colonic epithelial cell migration, ultimately facilitating mucosal healing. ER β −/− colitis mice exhibited impaired mucosal healing compared to wild-type littermates, highlighting the crucial effect of ER β. Importantly, combination with ER β -agonist diarylpropionitrile enhanced the amelioration of 5-aminosalicylic acid, a standard UC treatment agent, against mouse colitis. These findings attest to the crucial role of ER β activation in colonic mucosal healing and may further inform the development of novel strategies for UC treatment. ER β activation promoted autophagy of colonic epithelial cells by inhibiting branched-chain amino acid transport, leading to FAK activation and epithelial cell migration to facilitate mucosal healing in colon. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2025

2. Time and space modulation of substrate curvature to regulate cell mechanical identity.

Author

Saporito, Stefania, Panzetta, Valeria, and Netti, Paolo Antonio

Subjects

FOCAL adhesions, HUMAN stem cells, FINITE element method, CELL physiology, CURVATURE, CELL adhesion

Abstract

Recently, a variety of microenvironmental biophysical stimuli have been proved to play a crucial role in regulating cell functions. Among them, morpho-physical cues, like curvature, are emerging as key regulators of cellular behavior. Changes in substrate curvature have been shown to impact the arrangement of Focal Adhesions (FAs), influencing the direction and intensity of cytoskeleton generated forces and resulting in an overall alteration of cell mechanical identity. In their native environment, cells encounter varying degrees of substrate curvature, and in specific organs, they are exposed to dynamic changes of curvature due to periodic tissue deformation. However, the mechanism by which cells perceive substrate curvature remains poorly understood. To this aim, a micro-pneumatic device was designed and implemented. This device enables the controlled application of substrate curvature, both statically and dynamically. Employing a combined experimental and simulative approach, human adipose-derived stem cells were exposed to controlled curvature intensity and frequency. During this exposure, measurements were taken on FAs extension and orientation, cytoskeleton organization and cellular/nuclear alignment. The data clearly indicated a significant influence of the substrate curvature on cell adhesion processes. These findings contribute to a better understanding of the mechanisms through which cells perceive and respond to substrate curvature signals. This work is our contribution to the comprehension of substrate curvature's function as a crucial regulator of cell adhesion at the scale of focal adhesions and cell mechanical identity. In recent years, a large body of knowledge is continuously growing providing comprehension of the role of various microenvironmental biophysical stimuli in regulating cell functions. Nevertheless, little is known about the role of substrate curvature, in particular, when cells are exposed to this stimulus in a dynamic manner. To address the role of substrate curvature on cellular behavior, a micro-pneumatic device was designed and implemented. This device enables the controlled application of substrate curvature, both statically and dynamically. The experiment data made it abundantly evident that the substrate curvature had a major impact on the mechanisms involved in cell adhesion. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

3. Focal adhesion and actin orientation regulated by cellular geometry determine stem cell differentiation via mechanotransduction.

Author

Wang, Xinlong, Yang, Yingjun, Wang, Yongtao, Lu, Chengyu, Hu, Xiaohong, Kawazoe, Naoki, Yang, Yingnan, and Chen, Guoping

Subjects

CELL adhesion, FOCAL adhesions, MECHANOTRANSDUCTION (Cytology), CELL differentiation, MESENCHYMAL stem cell differentiation, STEM cells

Abstract

Tuning cell adhesion geometry can affect cytoskeleton organization and the distribution of cytoskeleton forces, which play critical roles in controlling cell functions. To elucidate the geometrical relationship with cytoskeleton force distribution, it is necessary to control cell morphology. In this study, a series of dextral vortex micropatterns were prepared to precisely control cell morphology for investigating the influence of the curvature degree of adhesion curves on intracellular force distribution and stem cell differentiation at a sub-cellular level. Peripherial actin filaments of micropatterned cells were assembled along the adhesion curves and showed different orientations, filament thicknesses and densities. Focal adhesion and cytoskeleton force distribution were dependent on the curvature degree. Intracellular force distribution was also regulated by adhesion curves. The cytoskeleton and force distribution affected the osteogenic differentiation of mesenchymal stem cells through a YAP/TAZ-mediated mechanotransduction process. Thus, regulation of cell adhesion curvature, especially at cytoskeletal filament level, is critical for cell function manipulation. In this study, a series of dextral micro-vortexes were prepared and used for the culture of human mesenchymal stem cells (hMSCs) to precisely control adhesive curvatures (0°, 30°, 60°, and 90°). The single MSCs on the micropatterns had the same size and shape but showed distinct focal adhesion (FA) and cytoskeleton orientations. Cellular nanomechanics were observed to be correlated with the curvature degrees, subsequently influencing nuclear morphological features. As a consequence, the localization of the mechanotransduction sensor and activator-YAP/TAZ was affected, influencing osteogenic differentiation. The results revealed the pivotal role of adhesive curvatures in the manipulation of stem cell differentiation via the machanotransduction process, which has rarely been investigated. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

4. ITIH5 as a multifaceted player in pancreatic cancer suppression, impairing tyrosine kinase signaling, cell adhesion and migration.

Author

Kosinski, Jennifer, Sechi, Antonio, Hain, Johanna, Villwock, Sophia, Ha, Stefanie Anh, Hauschulz, Maximilian, Rose, Michael, Steib, Florian, Ortiz‐Brüchle, Nadina, Heij, Lara, Maas, Sanne L., van der Vorst, Emiel P. C., Knoesel, Thomas, Altendorf‐Hofmann, Annelore, Simon, Ronald, Sauter, Guido, Bednarsch, Jan, Jonigk, Danny, and Dahl, Edgar

Abstract

Inter‐alpha‐trypsin inhibitor heavy chain 5 (ITIH5) has been identified as a metastasis suppressor gene in pancreatic cancer. Here, we analyzed ITIH5 promoter methylation and protein expression in The Cancer Genome Atlas (TCGA) dataset and three tissue microarray cohorts (n = 618), respectively. Cellular effects, including cell migration, focal adhesion formation and protein tyrosine kinase activity, induced by forced ITIH5 expression in pancreatic cancer cell lines were studied in stable transfectants. ITIH5 promoter hypermethylation was associated with unfavorable prognosis, while immunohistochemistry demonstrated loss of ITIH5 in the metastatic setting and worsened overall survival. Gain‐of‐function models showed a significant reduction in migration capacity, but no alteration in proliferation. Focal adhesions in cells re‐expressing ITIH5 exhibited a smaller and more rounded phenotype, typical for slow‐moving cells. An impressive increase of acetylated alpha‐tubulin was observed in ITIH5‐positive cells, indicating more stable microtubules. In addition, we found significantly decreased activities of kinases related to focal adhesion. Our results indicate that loss of ITIH5 in pancreatic cancer profoundly affects its molecular profile: ITIH5 potentially interferes with a variety of oncogenic signaling pathways, including the PI3K/AKT pathway. This may lead to altered cell migration and focal adhesion formation. These cellular alterations may contribute to the metastasis‐inhibiting properties of ITIH5 in pancreatic cancer. [ABSTRACT FROM AUTHOR]

Published

2024

5. Integrative analysis of immune‐related signature profiles in eosinophilic chronic rhinosinusitis with nasal polyposis.

Author

Kan, Xuan, Guan, Ruidi, Hao, Jianwei, Zhao, Chunyuan, and Sun, Yanan

Subjects

NASAL polyps, SINUSITIS, FOCAL adhesions, HYPERTROPHIC cardiomyopathy, NASAL cavity, ADENOMATOUS polyps, EOSINOPHILIA

Abstract

Eosinophilic chronic rhinosinusitis with nasal polyps (ECRSwNP) is a subtype of chronic rhinosinusitis (CRS) that is associated with the nasal cavity and sinus polyps, elevated levels of eosinophils, and dysregulated immune responses to environmental triggers. The underlying cause of ECRSwNP is not well understood, and few studies have focused on the unique features of this subtype of CRS. Our study integrated proteomic and transcriptomic data with multi‐omic bioinformatics analyses. We collected nasal polyps from three ECRSwNP patients and three control patients and identified 360 differentially expressed (DE) proteins, including 119 upregulated and 241 downregulated proteins. Functional analyses revealed several significant associations with ECRSwNP, including focal adhesion, hypertrophic cardiomyopathy, and extracellular matrix (ECM)–receptor interactions. Additionally, a protein–protein interaction (PPI) network revealed seven hub proteins that may play crucial roles in the development of ECRSwNP. We also compared the proteomic data with publicly available transcriptomic data and identified a total of 1077 DE genes. Pathways enriched by the DE genes involved angiogenesis, positive regulation of cell motility, and immune responses. Furthermore, we investigated immune cell infiltration and identified biomarkers associated with eosinophil and M2 macrophage infiltration using CIBERSORT and Weighted Gene Correlation Network Analysis (WGCNA). Our results provide a more complete picture of the immune‐related mechanisms underlying ECRSwNP, which could contribute to the development of more precise treatment strategies for this condition. [ABSTRACT FROM AUTHOR]

Published

2023

6. Development of an integrin αv-based universal marker, capable of both prediction and direction of stem cell fate.

Author

Heo, Cheol Ho, Bak, Seon Young, Kim, Yonghan, Ok, Myoung-Ryul, and Kim, So Yeon

Subjects

MESENCHYMAL stem cells, CELL culture, INTEGRINS, STEM cells, CELL morphology, FOCAL adhesions

Abstract

Integrin-mediated focal adhesion (FA) and subsequent cytoskeletal reorganization influence cell morphology, migration, and ultimately cell fate. Previous studies have used various patterned surfaces with defined macroscopic cell shapes or nanoscopic FA distributions to explore how different substrates affect the fate of human bone marrow mesenchymal stem cells (BMSCs). However, there is currently no straightforward relationship between BMSC cell fates induced by patterned surfaces and FA distribution substrates. In this study, we conducted single-cell image analysis of integrin α v -mediated FA and cell morphological features of BMSCs during biochemically induced differentiation. This enabled the identification of distinct FA features that can discriminate between osteogenic and adipogenic differentiation, demonstrating that integrin α v -mediated focal adhesion (FA) can be used as a non-invasive biomarker for real time observation. Based on these results, we developed an organized microscale fibronectin (FN) patterned surface where the fate of BMSC could be precisely manipulated by these FA features. Notably, even in the absence of any biochemical inducers, such as those contained in the differentiation medium, BMSCs cultured on these FN patterned surfaces exhibited upregulation of differentiation markers comparable to BMSCs cultured using conventional differentiation methods. Therefore, the present study reveals the application of these FA features as universal markers not only for predicting differentiation status, but also for regulating cell fate by precisely controlling the FA features with a new cell culture platform. Although the effects of material physiochemical properties on cell morphology and subsequent cell fate decisions have been extensively studied, a simple yet intuitive correlation between cellular features and differentiation remains unavailable. We present a single cell image-based strategy for predicting and directing stem cell fate. By using a specific integrin isoform, integrin α v , we identified distinct geometric features that can be used as a marker for discriminating between osteogenic and adipogenic differentiation in real-time. From these data, new cell culture platforms capable of regulating cell fate by precisely controlling FA features and cell area can be developed. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

7. Living cells as a biological analog of optical tweezers – a non-invasive microrheology approach.

Author

Hardiman, William, Clark, Matt, Friel, Claire, Huett, Alan, Pérez-Cota, Fernando, Setchfield, Kerry, Wright, Amanda J., and Tassieri, Manlio

Subjects

OPTICAL tweezers, CYTOLOGY, CELLULAR mechanics, APPLIED mechanics, FOCAL adhesions, POLYMERSOMES, HEMORHEOLOGY

Abstract

[Display omitted] Microrheology, the study of fluids on micron length-scales, promises to reveal insights into cellular biology, including mechanical biomarkers of disease and the interplay between biomechanics and cellular function. Here a minimally-invasive passive microrheology technique is applied to individual living cells by chemically binding a bead to the surface of a cell, and observing the mean squared displacement of the bead at timescales ranging from milliseconds to 100s of seconds. Measurements are repeated over the course of hours, and presented alongside analysis to quantify changes in the cells' low-frequency elastic modulus, G 0 ′ , and the cell's dynamics over the time window ∼ 10 − 2 s to 10 s. An analogy to optical trapping allows verification of the invariant viscosity of HeLa S3 cells under control conditions and after cytoskeletal disruption. Stiffening of the cell is observed during cytoskeletal rearrangement in the control case, and cell softening when the actin cytoskeleton is disrupted by Latrunculin B. These data correlate with conventional understanding that integrin binding and recruitment triggers cytoskeletal rearrangement. This is, to our knowledge, the first time that cell stiffening has been measured during focal adhesion maturation, and the longest time over which such stiffening has been quantified by any means. Here, we present an approach for studying mechanical properties of live cells without applying external forces or inserting tracers. Regulation of cellular biomechanics is crucial to healthy cell function. For the first time in literature, we can non-invasively and passively quantify cell mechanics during interactions with functionalised surface. Our method can monitor the maturation of adhesion sites on the surface of individual live cells without disrupting the cell mechanics by applying forces to the cell. We observe a stiffening response in cells over tens of minutes after a bead chemically binds. This stiffening reduces the deformation rate of the cytoskeleton, although the internal force generation increases. Our method has potential for applications to study mechanics during cell-surface and cell-vesicle interactions. [ABSTRACT FROM AUTHOR]

Published

2023

8. Early committed polarization of intracellular tension in response to cell shape determines the osteogenic differentiation of mesenchymal stromal cells.

Author

Wu, Ming-Chung, Yu, Helen Wenshin, Chen, Yin-Quan, Ou, Meng-Hsin, Serrano, Ricardo, Huang, Guan-Lin, Wang, Yang-Kao, Lin, Kung-hui, Fan, Yu-Jui, Wu, Chi-Chang, del Álamo, Juan C., Chiou, Arthur, Chien, Shu, and Kuo, Jean-Cheng

Subjects

CELL morphology, STROMAL cells, NUCLEAR membranes, CELLULAR mechanics, FOCAL adhesions, CELL nuclei, ERYTHROCYTE deformability

Abstract

Within the heterogeneous tissue architecture, a comprehensive understanding of how cell shapes regulate cytoskeletal mechanics by adjusting focal adhesions (FAs) signals to correlate with the lineage commitment of mesenchymal stromal cells (MSCs) remains obscure. Here, via engineered extracellular matrices, we observed that the development of mature FAs, coupled with a symmetrical pattern of radial fiber bundles, appeared at the right-angle vertices in cells with square shape. While circular cells aligned the transverse fibers parallel to the cell edge, and moved them centripetally in a counter-clockwise direction, symmetrical bundles of radial fibers at the vertices of square cells disrupted the counter-clockwise swirling and bridged the transverse fibers to move centripetally. In square cells, the contractile force, generated by the myosin IIA-enriched transverse fibers, were concentrated and transmitted outwards along the symmetrical bundles of radial fibers, to the extracellular matrix through FAs, and thereby driving FA organization and maturation. The symmetrical radial fiber bundles concentrated the transverse fibers contractility inward to the linkage between the actin cytoskeleton and the nuclear envelope. The tauter cytoskeletal network adjusted the nuclear-actomyosin force balance to cause nuclear deformability and to increase nuclear translocation of the transcription co-activator YAP, which in turn modulated the switch in MSC commitment. Thus, FAs dynamically respond to geometric cues and remodel actin cytoskeletal network to re-distribute intracelluar tension towards the cell nucleus, and thereby controlling YAP mechanotransduction signaling in regulating MSC fate decision. We decipher how cellular mechanics is self-organized depending on extracellular geometric features to correlate with mesenchymal stromal cell lineage commitment. In response to geometry constrains on cell morphology, symmetrical radial fiber bundles are assembled and clustered depending on the maturation state of focal adhesions and bridge with the transverse fibers, and thereby establishing the dynamic cytoskeletal network. Contractile force, generated by the myosin-IIA-enriched transverse fibers, is transmitted and dynamically drives the retrograde movement of the actin cytoskeletal network, which appropriately adjusts the nuclear-actomyosin force balance and deforms the cell nucleus for YAP mechano-transduction signaling in regulating mesenchymal stromal cell fate decision. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

9. Identifying prognostic biomarkers and immune interactions in ovarian cancer associated with perfluorooctanoic acid exposure: Insights from comparative toxicogenomics and molecular docking studies.

Author

Li, Jianing, Bian, Xiaofeng, Zhang, Caixia, Chen, Yirong, Huang, Shijia, Zhao, Shuli, and Li, Yanchuan

Subjects

PERFLUOROOCTANOIC acid, POLLUTANTS, PROTEIN-protein interactions, MOLECULAR dynamics, FOCAL adhesions

Abstract

Perfluorooctanoic acid (PFOA) exposure has been implicated in various health issues. This study aims to identify common genes associated with PFOA exposure and ovarian cancer, elucidate their biological functions, and explore their prognostic significance. We identified common genes linked to PFOA exposure and ovarian cancer using the Comparative Toxicogenomics Database. Protein-protein interaction and functional enrichment analyses were performed via Metascape. A PFOA-related risk model was developed using TCGA data and LASSO regression. Survival and expression analyses were conducted, and a prognostic nomogram was created. Tumor immune microenvironment interactions were investigated using ESTIMATE and ssGSEA methods. Molecular docking studies assessed the binding affinities between PFOA and target proteins. Utilizing the Comparative Toxicogenomics Database, we identified 229 common genes linked to both PFOA exposure and ovarian cancer. A comprehensive protein-protein interaction (PPI) network analysis revealed distinct functional modules. Enrichment analysis indicated significant involvement of these genes in pathways like the PI3K-Akt signaling pathway and focal adhesion. Lasso regression identified seven key prognostic genes (ERBB2, CCNH, PDE2A, CXCL11, TIAM1, SLC9A1, and EPHA2), with survival analysis demonstrating that PFOA-related high risk group exhibited significantly worse overall survival. Expression analysis showed the dysregulation of key prognostic genes in tumor tissues, while immune correlation analysis indicated significant associations with the tumor microenvironment. Molecular docking and molecular dynamics simulations revealed strong binding affinities between PFOA and the PDE2A. Overall, this research contributes to a deeper understanding of the health risks associated with PFOA exposure and highlights the importance of continued monitoring and regulation of environmental pollutants to safeguard public health. [Display omitted] • Identified 229 common genes linked to PFOA exposure and ovarian cancer. • Seven prognostic genes revealed significant survival differences in high-risk groups. • Strong binding between PFOA and PDE2A suggests key interactions in cancer. [ABSTRACT FROM AUTHOR]

Published

2025

10. Roles of focal adhesion proteins in skeleton and diseases.

Author

Chen, Sheng, He, Tailin, Zhong, Yiming, Chen, Mingjue, Yao, Qing, Chen, Di, Shao, Zengwu, and Xiao, Guozhi

Subjects

FOCAL adhesions, BONE fractures, FOCAL adhesion kinase, INTERVERTEBRAL disk, CELLULAR control mechanisms, PHOSPHATE metabolism

Abstract

The skeletal system, which contains bones, joints, tendons, ligaments and other elements, plays a wide variety of roles in body shaping, support and movement, protection of internal organs, production of blood cells and regulation of calcium and phosphate metabolism. The prevalence of skeletal diseases and disorders, such as osteoporosis and bone fracture, osteoarthritis, rheumatoid arthritis, and intervertebral disc degeneration, increases with age, causing pain and loss of mobility and creating a huge social and economic burden globally. Focal adhesions (FAs) are macromolecular assemblies that are composed of the extracellular matrix (ECM), integrins, intracellular cytoskeleton and other proteins, including kindlin, talin, vinculin, paxillin, pinch, Src, focal adhesion kinase (FAK) and integrin-linked protein kinase (ILK) and other proteins. FA acts as a mechanical linkage connecting the ECM and cytoskeleton and plays a key role in mediating cell–environment communications and modulates important processes, such as cell attachment, spreading, migration, differentiation and mechanotransduction, in different cells in skeletal system by impacting distinct outside-in and inside-out signaling pathways. This review aims to integrate the up-to-date knowledge of the roles of FA proteins in the health and disease of skeletal system and focuses on the specific molecular mechanisms and underlying therapeutic targets for skeletal diseases. Focal adhesion proteins sense changes of microenvironments, which allows cells to orchestrate the outside-in and inside-out signaling, and plays an important role in the health and diseases of skeletal system. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

11. Zyxin and actin structure confer anisotropic YAP mechanotransduction.

Author

Wen, Shin-Min, Wen, Wen-Cih, and Chao, Pen-hsiu Grace

Subjects

YAP signaling proteins, FOCAL adhesion kinase, MECHANOTRANSDUCTION (Cytology), ACTIN, FOCAL adhesions, HOMEOSTASIS

Abstract

Tissues and the embedded cells experience anisotropic deformations due to their functions and anatomical locations. The resident cells, such as tenocytes and muscle cells, are often restricted by their extracellular matrix and organize parallel to their major loading direction, yet most studies on cellular responses to strains use isotropic substrates without predetermined organizations. To understand how confined cells sense and respond to anisotropic loading, we combine cell patterning and uniaxial stretch to have precise geometric control. Dynamic stretch parallel to the long axis of the cell activates YAP nuclear translocation, but not when stretched in the perpendicular direction. Looking at the initial cytoskeleton response, parallel stretch leads to actin breakage and repair within the first minute, mediated by zyxin, the focal adhesion protein. In addition, this zyxin-mediated repair response is controlled by focal adhesion kinase (FAK) and leads to YAP signaling. As these factors are intimately involved in a wide range of mechanical regulation, our findings point to new roles of zyxin and YAP in anisotropic mechanotransduction, and may provide additional perspectives in cellular adaptive responses and tissue homeostasis. Structure and deformation of tissues control gene expression, migration, and proliferation of the resident cells. In an effort to understand the underlying mechanisms, we find that the transcription cofactor YAP respond to mechanical stretch in a direction-dependent manner. We demonstrate that parallel stretch induces actin cytoskeleton damage, focal adhesion kinase (FAK) activation, and zyxin relocation, which are involved in the anisotropic YAP signaling. Our findings provide additional perspectives in the interactions of tissue structure and cell mechanotransduction. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

12. Titanium nanotopography induces osteocyte lacunar-canalicular networks to strengthen osseointegration.

Author

He, Xindie, Yamada, Masahiro, Watanabe, Jun, Tiskratok, Watcharaphol, Ishibashi, Minoru, Kitaura, Hideki, Mizoguchi, Itaru, and Egusa, Hiroshi

Subjects

OSSEOINTEGRATION, TITANIUM, DENDRITES, FOCAL adhesions, DENTAL implants, BONE remodeling, HYDROXYL group

Abstract

Osteocyte network architecture is closely associated with bone turnover. The cellular mechanosensing system regulates osteocyte dendrite formation by enhancing focal adhesion. Therefore, titanium surface nanotopography might affect osteocyte network architecture and improve the peri-implant bone tissue quality, leading to strengthened osseointegration of bone-anchored implants. We aimed to investigate the effects of titanium nanosurfaces on the development of osteocyte lacunar-canalicular networks and osseointegration of dental implants. Alkaline etching created titanium nanosurfaces with anisotropically patterned dense nanospikes, superhydrophilicity, and hydroxyl groups. MLO-Y4 mouse osteocyte-like cells cultured on titanium nanosurfaces developed neuron-like dendrites with increased focal adhesion assembly and gap junctions. Maturation was promoted in osteocytes cultured on titanium nanosurfaces compared to cells cultured on machined or acid-etched micro-roughened titanium surfaces. Osteocytes cultured in type I three-dimensional collagen gels for seven days on nano-roughened titanium surfaces displayed well-developed interconnectivity with highly developed dendrites and gap junctions compared to the poor interconnectivity observed on the other titanium surfaces. Even if superhydrophilicity and hydroxyl groups were maintained, the loss of anisotropy-patterned nanospikes reduced expression of gap junction in osteocytes cultured on alkaline-etched titanium nanosurfaces. Four weeks after placing the titanium nanosurface implants in the upper jawbone of wild-type rats, osteocytes with numerous dendrites were found directly attached to the implant surface, forming well-developed lacunar-canalicular networks around the nano-roughened titanium implants. The osseointegration strength of the nano-roughened titanium implants was significantly higher than that of the micro-roughened titanium implants. These data indicate that titanium nanosurfaces promote osteocyte lacunar-canalicular network development via nanotopographical cues and strengthen osseointegration. The clinical stability of bone-anchoring implant devices is influenced by the bone quality. The osteocyte network potentially affects bone quality and is established by the three-dimensional (3D) connection of neuron-like dendrites of well-matured osteocytes within the bone matrix. No biomaterials are known to regulate formation of the osteocyte network. The present study provides the first demonstration that titanium nanosurfaces with nanospikes created by alkali-etching treatment enhance the 3D formation of osteocyte networks by promoting osteocyte dendrite formation and maturation by nanotopographic cues, leading to strengthened osseointegration of titanium implants. Osteocytes attached to the titanium nanosurfaces via numerous cellular projections. The success of osteocyte regulation by nanotechnology paves the way for development of epoch-making technologies to control bone quality. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

13. New Life Science Study Findings Have Been Reported from University of Yamanashi (Fructo-oligosaccharides Enhance the Expression of Genes Related To Focal Adhesion- and Inflammation-pathways In Small Intestinal Absorptive Caco-2 Cells).

Abstract

A recent study conducted at the University of Yamanashi in Japan explored the effects of fructo-oligosaccharides (FOS) on gene expression in human intestinal absorptive cells. The research found that FOS treatment enhanced the expression of genes related to focal adhesion and inflammation pathways in Caco-2 cells. This study was supported by the Ministry of Education, Culture, Sports, Science and Technology in Japan and has been peer-reviewed. For more information, the full report can be found in the Journal of Nutritional Science and Vitaminology. [Extracted from the article]

Published

2025

14. Insight into link between lysosomal activities and focal adhesions and implications for cancer research.

Abstract

The study explores the relationship between lysosomal exocytosis and focal adhesions in cancer cells, revealing the role of paucimannose glycans in cancer progression. Lysosomes, responsible for breaking down molecules, can also aid tumor progression through lysosomal exocytosis. Researchers suggest that targeting paucimannose glycans and lysosomal exocytosis mechanisms could lead to innovative cancer therapies. [Extracted from the article]

Published

2025

15. Researchers at Capital Medical University Report Research in Oral Health (LIPUS promotes osteogenic differentiation of rat BMSCs and osseointegration of dental implants by regulating ITGA11 and focal adhesion pathway).

Abstract

Researchers at Capital Medical University conducted a study on the effects of Low-Intensity Pulsed Ultrasound (LIPUS) on bone marrow mesenchymal stem cells (BMSCs) and dental implant osseointegration. The study found that LIPUS promoted osteogenic differentiation of BMSCs and improved implant osseointegration in rats by upregulating ITGA11 and activating the focal adhesion pathway. This research provides insights into potential clinical applications of LIPUS in oral health. For more information, the study is published in BMC Oral Health, and the lead researcher can be contacted at Beijing Stomatological Hospital, Capital Medical University. [Extracted from the article]

Published

2025

16. Three-year survey of oral hygiene conditions of Cambodian public primary school children.

Author

Yuria Asao, Yuko Iwamoto, Chieko Mitsuhata, Mariko Naito, and Katsuyuki Kozai

Subjects

ORAL hygiene, SCHOOL children, PRIMARY schools, FOCAL adhesions, DENTAL calculus

Abstract

Purpose: The purpose of this repeated cross-sectional study was to investigate the prevalence and severity of oral hygiene conditions in Cambodian primary school children. Methods: Oral examinations were conducted on 2,020 school children (1st-6th grade) at a public primary school in Siem Reap, Cambodia from 2013 to 2015, focusing on plaque adhesion, gingiva, and dental calculus deposition. Data analysis was performed on 1,998 children without any missing data, and the chi-square test was used to compare the variables. Results: The prevalence of dental plaque adhesion in 2013, 2014, and 2015 was 93.6%, 93.7%, and 85.1%, respectively. The prevalence of gingivitis in 2013, 2014, and 2015 was 93.1%, 92.1%, and 88.8%, respectively. The prevalence of dental calculus deposition in 2013, 2014, and 2015 was 55.1%, 19.3%, and 34.7%, respectively. Significant differences were observed in all variables each year (P < 0.001). Conclusion: The findings of this study suggest that oral hygiene conditions were poor in this population. [ABSTRACT FROM AUTHOR]

Published

2022

17. Nanoscale geometry determines mechanical biocompatibility of vertically aligned nanofibers.

Author

Rantataro, Samuel, Parkkinen, Ilmari, Pande, Ishan, Domanskyi, Andrii, Airavaara, Mikko, Peltola, Emilia, and Laurila, Tomi

Subjects

CARBON nanofibers, FOCAL adhesions, NANOFIBERS, ATOMIC force microscopy, MECHANICAL behavior of materials, HYDROGELS, SMART materials, BIOCOMPATIBILITY

Abstract

[Display omitted] Vertically aligned carbon nanofibers (VACNFs) are promising material candidates for neural biosensors due to their ability to detect neurotransmitters in physiological concentrations. However, the expected high rigidity of CNFs could induce mechanical mismatch with the brain tissue, eliciting formation of a glial scar around the electrode and thus loss of functionality. We have evaluated mechanical biocompatibility of VACNFs by growing nickel-catalyzed carbon nanofibers of different lengths and inter-fiber distances. Long nanofibers with large inter-fiber distance prevented maturation of focal adhesions, thus constraining cells from obtaining a highly spread morphology that is observed when astrocytes are being contacted with stiff materials commonly used in neural implants. A silicon nanopillar array with 500 nm inter-pillar distance was used to reveal that this inhibition of focal adhesion maturation occurs due to the surface nanoscale geometry, more precisely the inter-fiber distance. Live cell atomic force microscopy was used to confirm astrocytes being significantly softer on the long Ni-CNFs compared to other surfaces, including a soft gelatin hydrogel. We also observed hippocampal neurons to mature and form synaptic contacts when being cultured on both long and short carbon nanofibers, without having to use any adhesive proteins or a glial monoculture, indicating high cytocompatibility of the material also with neuronal population. In contrast, neurons cultured on a planar tetrahedral amorphous carbon sample showed immature neurites and indications of early-stage apoptosis. Our results demonstrate that mechanical biocompatibility of biomaterials is greatly affected by their nanoscale surface geometry, which provides means for controlling how the materials and their mechanical properties are perceived by the cells. Our research article shows, how nanoscale surface geometry determines mechanical biocompatibility of apparently stiff materials. Specifically, astrocytes were prevented from obtaining highly spread morphology when their adhesion site maturation was inhibited, showing similar morphology on nominally stiff vertically aligned carbon fiber (VACNF) substrates as when being cultured on ultrasoft surfaces. Furthermore, hippocampal neurons matured well and formed synapses on these carbon nanofibers, indicating high biocompatibility of the materials. Interestingly, the same VACNF materials that were used in this study have earlier also been proven to be capable for electrophysiological recordings and sensing neurotransmitters at physiological concentrations with ultra-high sensitivity and selectivity, thus providing a platform for future neural probes or smart culturing surfaces with superior sensing performance and biocompatibility. [ABSTRACT FROM AUTHOR]

Published

2022

18. Computer Aided Drug Discovery Utilization in Conservative Dentistry.

Author

Prahasti, Anastasia Elsa, Yuanita, Tamara, and Rahayu, Retno Pudji

Subjects

DRUG discovery, DRUG utilization, FOCAL adhesions, DRUG design, ABORTIFACIENTS, DENTISTRY, CARIOGENIC agents

Abstract

Computer aided drugs discovery or in silico design is bioinformatics’ contribution that supports pharmacy, medical and dentistry fields. It creates innovation in the search, design and optimization of new drug candidates. The method minimizes the use of animal models and in vitro assay laboratory work, which are very time and resources consuming processes. Even though it has big advantages, it has not been utilized frequently in conservative dentistry fields. Researches using CADD approaches in conservative dentistry shown in the reviews, used Structure-based design and Ligand-based design, both are two methods to predict compound-protein interaction. Utilized as genome identification of Streptococcus mutans, CADD can differ the genome from other bacteria and gives confirmation to polymerase chain reaction examination. CADD also beneficial to predict pharmacokinetics of drug candidates. This method exhibits great prediction in screening active compounds that have inhibition action in bacterial growth and adhesion on dental plaque. CADD approach has been used in conservative dentistry and showed great predictions to minimize numbers of trials in laboratory works. Expansion of application might boost drugs design projects in conservative dentistry. [ABSTRACT FROM AUTHOR]

Published

2022

19. Cell alignment modulated by surface nano-topography – Roles of cell-matrix and cell-cell interactions.

Author

Coyle, Stephen, Doss, Bryant, Huo, Yucheng, Singh, Hemang Raj, Quinn, David, Jimmy Hsia, K., and LeDuc, Philip R.

Subjects

CELL communication, SURFACE topography, CELL anatomy, FOCAL adhesions, TISSUES

Abstract

The propensity of cells to align in particular directions is relevant to a number of areas, including tissue engineering and biohybrid robotics. Cell alignment is modulated through various extracellular conditions including surface topographies, mechanical cues from cell-matrix interactions, and cell-cell interactions. Understanding of these conditions provides guidance for desirable cellular structure constructions. In this study, we examine the roles of surface topographies and cell-cell interactions in inducing cell alignment. We employed wavy surface topographies at the nanometer scale as a model extracellular environment for cell culture. The results show that, within a certain range of wavelengths and amplitudes of the surface topographies, cell alignment is dependent on cell confluency. This dependence on both topology and confluency suggests interplay between cell-cell and cell-matrix interactions in inducing cell alignment. Images of sparsely distributed and confluent cells also demonstrated clear differences in the structures of their focal adhesion complexes. To understand this effect, we introduced anti-N-cadherin to cell culture to inhibit cell-cell interactions. The results show that, when anti-N-cadherin was applied, cells on wavy surfaces required greater confluency to achieve the same alignment compared to that in the absence of anti-N-cadherin. The understanding of the cell alignment mechanisms will be important in numerous potential applications such as scaffold design, tissue repair, and development of biohybrid robotic systems. Cell alignment plays a critical role in numerous biological functions. Advances in tissue engineering utilizes cell alignment to restore, maintain, or even replace different types of biological tissues. The clinical impact that tissue engineering has made is facilitated by advancements in the understanding of interactions between scaffolds, biological factors, and cells. This work further elucidates the role of cell-cell interactions in promoting the organization of biological tissues. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

20. Targeting extracellular matrix glycation to attenuate fibroblast activation.

Author

Jang, Minjeong, Oh, Seung Won, Lee, Yunji, Kim, Jin Young, Ji, Eun Sun, and Kim, Pilnam

Subjects

EXTRACELLULAR matrix, FIBROBLASTS, INTEGRINS, ADVANCED glycation end-products, FOCAL adhesions, MATRIX effect, MYOFIBROBLASTS

Abstract

The extracellular matrix (ECM) of the tumor microenvironment undergoes constant remodeling that alters its biochemical and mechano-physical properties. Non-enzymatic glycation can induce the formation of advanced glycation end-products (AGEs), which may cause abnormal ECM turnover with excessively cross-linked collagen fibers. However, the subsequent effects of AGE-mediated matrix remodeling on the characteristics of stromal cells in tumor microenvironments remain unclear. Here, we demonstrate that AGEs accumulated in the ECM alter the fibroblast phenotype within a three-dimensional collagen matrix. Both the AGE interaction with its receptor (RAGE) and integrin-mediated mechanotransduction signaling were up-regulated in glycated collagen matrix, leading to fibroblast activation to acquire a cancer-associated fibroblast (CAF)-like phenotype. These effects were blocked with neutralizing antibodies against RAGE or the inhibition of focal adhesion (FA) signaling. An AGE cross-link breaker, phenyl-4,5-dimethylthiazolium bromide (ALT 711), also reduced the transformation of fibroblasts into the CAF-like phenotype because of its dual inhibitory role in the AGE-modified matrix. Apart from targeting the AGE–RAGE interaction directly, the decreased matrix stiffness attenuated fibroblast activation by inhibiting the downstream cellular response to matrix stiffness. Our results suggest that indirect/direct targeting of accumulated AGEs in the ECM has potential for targeting the tumor stroma to improve cancer therapy. Advanced glycated end-products (AGEs)-modified extracellular matrix (ECM) is closely associated with pathological states and is recognized as a critical factor that precedes tumorigenesis. While increased matrix stiffness is known to induce fibroblast activation, less is known about how both biochemical and mechano-physical changes in AGE-mediated matrix-remodeling cooperate to produce a myofibroblastic cancer-associated fibroblast (CAF)-like phenotype. For the first time, we found that both the AGE interaction with its receptor (RAGE) and integrin-mediated mechanotransduction were up-regulated in glycated collagen matrix, leading to fibroblast activation. We further demonstrated that an AGE cross-link breaker, ALT-711, reduced the CAF-like transformation because of its dual inhibitory role in the AGE-modified matrix. Our findings offer promising extracellular-reversion strategies targeting the non-enzymatic ECM glycation, to regulate fibroblast activation. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

21. Regulation of cell attachment, spreading, and migration by hydrogel substrates with independently tunable mesh size.

Author

Xia, Jing, Liu, Zong-Yuan, Han, Zheng-Yuan, Yuan, Yuan, Shao, Yue, Feng, Xi-Qiao, and Weitz, David A.

Subjects

CELLULAR control mechanisms, HYDROGELS, MECHANOTRANSDUCTION (Cytology), YAP signaling proteins, FOCAL adhesions, MELANOPSIN

Abstract

Hydrogels are widely used as substrates to investigate interactions between cells and their microenvironment as they mimic many attributes of the extracellular matrix. The stiffness of hydrogels is an important property that is known to regulate cell behavior. Beside stiffness, cells also respond to structural cues such as mesh size. However, since the mesh size of hydrogel is intrinsically coupled to its stiffness, its role in regulating cell behavior has never been independently investigated. Here, we report a hydrogel system whose mesh size and stiffness can be independently controlled. Cell behavior, including spreading, migration, and formation of focal adhesions is significantly altered on hydrogels with different mesh sizes but with the same stiffness. At the transcriptional level, hydrogel mesh size affects cellular mechanotransduction by regulating nuclear translocation of yes-associated protein. These findings demonstrate that the mesh size of a hydrogel plays an important role in cell-substrate interactions. Hydrogels are ideal platforms with which to investigate interactions between cells and their microenvironment as they mimic many physical properties of the extracellular matrix. However, the mesh size of hydrogels is intrinsically coupled to their stiffness, making it challenging to investigate the contribution of mesh size to cell behavior. In this work, we use hydrogel-on-glass substrates with defined thicknesses whose stiffness and mesh size can be independently tuned. We use these substrates to isolate the effects of mesh size on cell behavior, including attachment, spreading, migration, focal adhesion formation and YAP localization in the nucleus. Our results show that mesh size has significant, yet often overlooked, effects, on cell behavior, and contribute to a further understanding of cell-substrate interactions. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

22. Nanoimprinting for high-throughput replication of geometrically precise pillars in fused silica to regulate cell behavior.

Author

Ganjian, Mahya, Modaresifar, Khashayar, Rompolas, Dionysios, Fratila-Apachitei, Lidy E., and Zadpoor, Amir A.

Subjects

FUSED silica, NANOIMPRINT lithography, SOFT lithography, FOCAL adhesions, ELECTRON beam lithography

Abstract

Developing high-throughput nanopatterning techniques that also allow for precise control over the dimensions of the fabricated features is essential for the study of cell-nanopattern interactions. Here, we developed a process that fulfills both of these criteria. Firstly, we used electron-beam lithography (EBL) to fabricate precisely controlled arrays of submicron pillars with varying values of interspacing on a large area of fused silica. Two types of etching procedures with two different systems were developed to etch the fused silica and create the final desired height. We then studied the interactions of preosteoblasts (MC3T3-E1) with these pillars. Varying interspacing was observed to significantly affect the morphological characteristics of the cell, the organization of actin fibers, and the formation of focal adhesions. The expression of osteopontin (OPN) significantly increased on the patterns, indicating the potential of the pillars for inducing osteogenic differentiation. The EBL pillars were thereafter used as master molds in two subsequent processing steps, namely soft lithography and thermal nanoimprint lithography for high-fidelity replication of the pillars on the substrates of interest. The molding parameters were optimized to maximize the fidelity of the generated patterns and minimize the wear and tear of the master mold. Comparing the replicated feature with those present on the original mold confirmed that the geometry and dimensions of the replicated pillars closely resemble those of the original ones. The method proposed in this study, therefore, enables the precise fabrication of submicron- and nanopatterns on a wide variety of materials that are relevant for systematic cell studies. Submicron pillars with specific dimensions on the bone implants have been proven to be effective in controlling cell behaviors. Nowadays, numerous methods have been proposed to produce bio-instructive submicron-topographies. However, most of these techniques are suffering from being low-throughput, low-precision, and expensive. Here, we developed a high-throughput nanopatterning technique that allows for control over the dimensions of the features for the study of cell-nanotopography interactions. Assessing the adaptation of preosteoblast cells showed the potential of the pillars for inducing osteogenic differentiation. Afterward, the pillars were used for high-fidelity replication of the bio-instructive features on the substrates of interest. The results show the advantages of nanoimprint lithography as a unique technique for the patterning of large areas of bio-instructive surfaces. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

23. Findings from Prince of Songkla University in Cervical Cancer Reported (Proteomic Analysis Reveals Cadherin, Actin, and Focal Adhesion Molecule-Mediated Formation of Cervical Cancer Spheroids).

Abstract

A recent study conducted at Prince of Songkla University in Thailand focused on the formation of cervical cancer spheroids, which are 3D assemblies of cancer cells used as models for studying cancer behavior. The research compared the proteomes of 3D and 2D cultures of cervical cancer cell lines, revealing differences in protein expression levels. The study found that certain proteins, including cadherin-binding, cytoskeleton, and adhesion proteins, play a crucial role in the formation of compact spheroids in cervical cancer cell lines. This research provides insights into the mechanisms underlying spheroid formation in cervical cancer. [Extracted from the article]

Published

2024

24. Data on Immunologic Receptors Discussed by Researchers at Xinxiang Medical University [Knockdown of Ano1 Decreases Tgf-(3-and Il-6-induced Adhesion and Migration of Cardiac Fibroblasts By Inhibiting the Expression of Integrin and Focal Adhesion...].

Abstract

Researchers at Xinxiang Medical University in the People's Republic of China have conducted a study on the role of ANO1, a calcium-activated chloride channel protein, in regulating cardiac fibroblasts (CFs) migration and adhesion under inflammatory conditions. The study found that knockdown of ANO1 decreased TGF-(3- and IL-6-induced adhesion and migration of CFs by inhibiting the expression of integrin and focal adhesion kinase. This research provides new insights into the mechanisms underlying CFs migration and adhesion, suggesting ANO1 as a potential therapeutic target for adverse fibrotic remodeling following myocardial infarction. [Extracted from the article]

Published

2024

25. University of California Researcher Describes Recent Advances in Ovarian Cancer (Nuclear Focal Adhesion Kinase Protects Against Cisplatin Stress in Ovarian Carcinoma).

Abstract

A recent study from the University of California highlights the role of nuclear focal adhesion kinase (FAK) in protecting against cisplatin stress in ovarian carcinoma. The research suggests that FAK expression, activity, and nuclear localization play a crucial role in limiting cisplatin cytotoxicity by regulating MKP1 levels and preventing non-canonical ERK/MAPK activation. This study sheds light on potential mechanisms of tumor chemotherapy resistance in high grade serous ovarian cancer (HGSOC) patients. [Extracted from the article]

Published

2024

26. New Ovarian Cancer Data Have Been Reported by Investigators at Kanagawa Cancer Center Research Institute [Tissue Factor Pathway Inhibitor-2 Inhibits Integrin (31 Activation and Focal Adhesion Formation and Suppresses Peritoneal Ovarian Cancer...].

Abstract

A recent study conducted at the Kanagawa Cancer Center Research Institute in Japan focused on the role of Tissue Factor Pathway Inhibitor-2 (TFPI2) in ovarian clear cell carcinoma (CCC) cells. The research found that TFPI2 inhibits cell proliferation, enhances focal adhesion formation, and suppresses peritoneal ovarian cancer dissemination in mice. This study sheds light on a potential novel function of TFPI2 in suppressing focal adhesion formation in CCC cells. For more information, the research article can be accessed through the DOI: https://doi.org/10.1016/j.bbrc.2024.150890. [Extracted from the article]

Published

2024

27. Research from Saarland University Medical Center Yields New Findings on Glioblastomas (Clotting promotes glioma growth and infiltration through activation of focal adhesion kinase).

Abstract

A recent study from Saarland University Medical Center in Germany explores the role of clotting in promoting the growth and infiltration of glioblastomas. The research highlights the accumulation of fibrin in tumor tissues, which enhances the growth of glioblastoma cells. By targeting focal adhesion kinase (FAK), researchers were able to inhibit tumor growth, suggesting a potential therapeutic strategy for glioblastoma treatment. The findings also correlate with genomic data indicating increased clotting activity in certain glioma subgroups with high integrin b1 and b3 expression, impacting patient survival rates. [Extracted from the article]

Published

2024

28. New Research on Osteosarcomas from Fudan University Shanghai Cancer Center Summarized (Prognostic signature and immunotherapeutic relevance of Focal adhesion signaling pathway-related genes in osteosarcoma).

Abstract

A recent study conducted by Fudan University Shanghai Cancer Center focused on osteosarcomas, the most common primary malignant bone tumor in children and adolescents. The research explored the prognostic features and immunotherapeutic relevance of focal adhesion pathway-related genes in osteosarcoma to develop new therapeutic options. The study identified three genes (ZYX, CAV1, and ITGA5) with a significant prognostic role and constructed a prognostic signature model associated with the focal adhesion signaling pathway. The findings suggest potential implications for personalized immunotherapy in treating osteosarcoma patients. [Extracted from the article]

Published

2024

29. Federal University Researchers Report Recent Findings in Apoptosis (Differential Gene Expression And Pathways Enrichment Analysis in Two Rna-seq Datasets of Jak2v617f Positive Cell Line, Treated With Ruxolitinib, Indicate Focal Adhesion Pathway...).

Abstract

Researchers from Federal University in Brazil conducted a study on the modulation of the Focal Adhesion pathway in JAK2 V617F-positive cells treated with the drug Ruxolitinib. The study aimed to understand the factors influencing the effectiveness of Ruxolitinib in reducing malignant clones and resistance in Myeloproliferative neoplasms (MPNs). Through RNAseq analysis of two datasets, researchers identified common differentially expressed genes (DEGs) related to the Focal Adhesion pathway, which plays a crucial role in cell viability, migration, and apoptosis. The findings suggest that further investigation into these genes could enhance the understanding of MPN treatment and prognosis. [Extracted from the article]

Published

2024

30. New Breast Cancer Study Findings Have Been Reported by Researchers at University of Nebraska-Kearney (Cytoarchitecture of Breast Cancer Cells Under Diabetic Conditions: Role of Regulatory Kinases-rho Kinase and Focal Adhesion Kinase).

Abstract

Researchers at the University of Nebraska-Kearney have conducted a study on the cytoarchitecture of breast cancer cells under diabetic conditions, focusing on the role of regulatory kinases Rho kinase and focal adhesion kinase. The study found that high-glucose conditions in diabetes can alter the structure of cancer cells, making them more aggressive and likely to spread. By blocking the ROCK or FAK proteins, these harmful changes can be lessened, potentially providing pathways to prevent such effects in diabetic breast cancer cells. This research sheds light on the impact of diabetes on breast cancer survival rates and metastasis, offering insights into potential targets for intervention. [Extracted from the article]

Published

2024

31. Recent Studies from Shahroud University of Medical Sciences Add New Data to Breast Cancer (Integrins linked kinase and focal adhesion kinase as the key signaling mediators of vascular mimicry in metastatic breast tumor cells).

Abstract

A recent study from Shahroud University of Medical Sciences explores the role of Integrins linked kinase (ILK) and focal adhesion kinase (FAK) in the formation of vascular mimicry (VM) in metastatic breast tumor cells. The research found that metastatic breast tumor cells have a higher potential for forming vascular-like structures, which is associated with elevated expression of ILK and FAK. These findings suggest that targeting ILK and FAK could be a potential strategy for combating metastasis in breast cancer. The study was published in BMC Research Notes and can be accessed for free online. [Extracted from the article]

Published

2024

32. Focal Adhesion Kinase (FAK) inhibition induces membrane accumulation of aquaporin2 (AQP2) through endocytosis inhibition and actin depolymerization in renal epithelial cells.

Abstract

The article discusses how inhibiting Focal Adhesion Kinase (FAK) in renal epithelial cells leads to the accumulation of aquaporin2 (AQP2) in the cell membrane by inhibiting endocytosis and depolymerizing actin. This process is crucial for regulating water balance in the kidney. The study suggests that targeting FAK signaling could offer a new approach to treating water balance disorders related to AQP2 trafficking. The research is available as a preprint and has not yet undergone peer review. [Extracted from the article]

Published

2024

33. Study Results from Chosun University Broaden Understanding of Signal Transducing Adaptor Proteins (Effect of Rosmarinic Acid on the Focal Adhesions of MC3T3-E1 Preosteoblasts on Titanium Surface).

Abstract

A study conducted by researchers at Chosun University explores the effects of rosmarinic acid (RA) on the focal adhesions (FAs) and cell proliferation of MC3T3-E1 preosteoblasts on titanium surfaces. FAs play a crucial role in the initial stage of osseointegration between preosteoblasts and titanium, which is important for the success of dental implants. The study found that RA increased FAs, cell proliferation, and mitosis through specific signaling pathways. The researchers concluded that RA could be an effective substance for improving FAs and cell proliferation on titanium surfaces, which is essential for the clinical success of titanium-based dental implants. [Extracted from the article]

Published

2024

34. New Cancer Findings from Northeast Ohio Medical University Outlined (Focal Adhesion Kinase-mediated Interaction Between Tumor and Immune Cells In the Tumor Microenvironment: Implications for Cancer-associated Therapies and Tumor Progression).

Abstract

A recent study conducted by researchers at Northeast Ohio Medical University explores the role of focal adhesion kinase (FAK) in tumor growth, immunosuppression, metastasis, angiogenesis, and therapeutic resistance. The study suggests that targeting FAK alone or in combination with other agents could be a potential therapeutic strategy for cancer treatment. The researchers also highlight the importance of FAK in regulating the interaction between tumor and immune cells in the tumor microenvironment, which can influence tumor immune evasive mechanisms. This research has been peer-reviewed and provides valuable insights into cancer-associated therapies and tumor progression. [Extracted from the article]

Published

2024

35. Bioengineered miR-124-3p prodrug selectively alters the proteome of human carcinoma cells to control multiple cellular components and lung metastasis in vivo.

Author

Deng, Linglong, Petrek, Hannah, Tu, Mei-Juan, Batra, Neelu, Yu, Ai-Xi, and Yu, Ai-Ming

Subjects

CELL anatomy, CELL junctions, FOCAL adhesions, METASTASIS, CELL adhesion, PRODRUGS, METASTATIC breast cancer, CADHERINS, CELL communication

Abstract

With the understanding of microRNA (miRNA or miR) functions in tumor initiation, progression, and metastasis, efforts are underway to develop new miRNA-based therapies. Very recently, we demonstrated effectiveness of a novel humanized bioengineered miR-124-3p prodrug in controlling spontaneous lung metastasis in mouse models. This study was to investigate the molecular and cellular mechanisms by which miR-124-3p controls tumor metastasis. Proteomics study identified a set of proteins selectively and significantly downregulated by bioengineered miR-124-3p in A549 cells, which were assembled into multiple cellular components critical for metastatic potential. Among them, plectin (PLEC) was verified as a new direct target for miR-124-3p that links cytoskeleton components and junctions. In miR-124-3p-treated lung cancer and osteosarcoma cells, protein levels of vimentin, talin 1 (TLN1), integrin beta-1 (ITGB1), IQ motif containing GTPase activating protein 1 (IQGAP1), cadherin 2 or N-cadherin (CDH2), and junctional adhesion molecule A (F11R or JAMA or JAM1) decreased, causing remodeling of cytoskeletons and disruption of cell–cell junctions. Furthermore, miR-124-3p sharply suppressed the formation of focal adhesion plaques, leading to reduced cell adhesion capacity. Additionally, efficacy and safety of biologic miR-124-3p therapy was established in an aggressive experimental metastasis mouse model in vivo. These results connect miR-124-3p−PLEC signaling to other elements in the control of cytoskeleton, cell junctions, and adhesion essential for cancer cell invasion and extravasation towards metastasis, and support the promise of miR-124 therapy. The antimetastatic activity of bioengineered miR-124-3p is attributable to selective downregulation of proteins underlying multiple cellular components, including cytoskeleton, cell junctions, and focal adhesion, critical for invasion and extravasation. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

36. "Viscotaxis"- directed migration of mesenchymal stem cells in response to loss modulus gradient.

Author

Shirke, Pallavi Uday, Goswami, Hiya, Kumar, Vardhman, Shah, Darshan, Beri, Sarayu, Das, Siddhartha, Bellare, Jayesh, Mayor, Satyajit, Venkatesh, K.V., Seth, Jyoti R., and Majumder, Abhijit

Subjects

MESENCHYMAL stem cells, HUMAN stem cells, CELL morphology, CYTOLOGY, FOCAL adhesions

Abstract

Directed cell migration plays a crucial role in physiological and pathological conditions. One important mechanical cue, known to influence cell migration, is the gradient of substrate elastic modulus (E). However, the cellular microenvironment is viscoelastic and hence the elastic property alone is not sufficient to define its material characteristics. To bridge this gap, in this study, we investigated the influence of the gradient of viscous property of the substrate, as defined by loss modulus (G ″) on cell migration. We cultured human mesenchymal stem cells (hMSCs) on a collagen-coated polyacrylamide gel with constant storage modulus (G ′) but with a gradient in the loss modulus (G ″). We found hMSCs to migrate from high to low loss modulus. We have termed this form of directional cellular migration as "Viscotaxis". We hypothesize that the high loss modulus regime deforms more due to creep in the long timescale when subjected to cellular traction. Such differential deformation drives the observed Viscotaxis. To verify our hypothesis, we disrupted the actomyosin contractility with myosin inhibitor blebbistatin and ROCK inhibitor Y27632, and found the directional migration to disappear. Further, such time-dependent creep of the high loss material should lead to lower traction, shorter lifetime of the focal adhesions, and dynamic cell morphology, which was indeed found to be the case. Together, findings in this paper highlight the importance of considering the viscous modulus while preparing stiffness-based substrates for the field of tissue engineering. While the effect of substrate elastic modulus has been investigated extensively in the context of cell biology, the role of substrate viscoelasticity is poorly understood. This omission is surprising as our body is not elastic, but viscoelastic. Hence, the role of viscoelasticity needs to be investigated at depth in various cellular contexts. One such important context is cell migration. Cell migration is important in morphogenesis, immune response, wound healing, and cancer, to name a few. While it is known that cells migrate when presented with a substrate with a rigidity gradient, cellular behavior in response to viscoelastic gradient has never been investigated. The findings of this paper not only reveal a completely novel cellular taxis or directed migration, it also improves our understanding of cell mechanics significantly. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

37. Micro tensile tester measurement of biomechanical properties and adhesion force of microtubule-polymerization-inhibited cancer cells.

Author

Uesugi, Kaoru, Obata, Shota, and Nagayama, Kazuaki

Subjects

CANCER cells, CANCER cell culture, TUBULINS, ATOMIC force microscopes, FOCAL adhesions, DRUG efficacy, ANTINEOPLASTIC agents

Abstract

Both mechanical and adhesion properties of cancer cells are complex and reciprocally related to migration, invasion, and metastasis with large cell deformation. Therefore, we evaluated these properties for human cervical cancer cells (HeLa) simultaneously using our previously developed micro tensile tester system. For efficient evaluation, we developed image analysis software to modify the system. The software can analyze the tensile force in real time. The modified system can evaluate the tensile stiffness of cells to which a large deformation is applied, also evaluate the adhesion strength of cancer cells that adhered to a culture substrate and were cultured for several days with their adhesion maturation. We used the modified system to simultaneously evaluate the stiffness of the cancer cells to which a large deformation was applied and their adhesion strength. The obtained results revealed that the middle phase of tensile stiffness and adhesion force of the microtubule-depolymerized group treated with colchicine (an anti-cancer drug) (stiffness, 13.4 ± 7.5 nN/%; adhesion force, 460.6 ± 258.2 nN) were over two times larger than those of the control group (stiffness, 5.0 ± 3.5 nN/%; adhesion force, 168.2 ± 98.0 nN). Additionally, the same trend was confirmed with the detailed evaluation of cell surface stiffness using an atomic force microscope. Confocal fluorescence microscope observations showed that the stress fibers (SFs) of colchicine-treated cells were aligned in the same direction, and focal adhesions (FAs) of the cells developed around both ends of the SFs and aligned parallel to the developed direction of the SFs. There was a possibility that the microtubule depolymerization by the colchicine treatment induced the development of SFs and FAs and subsequently caused an increment of cell stiffness and adhesion force. From the above results, we concluded the modified system would be applicable to cancer detection and anti-cancer drug efficacy tests. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2024

38. Droplet microfluidics as a tool for production of bioactive calcium phosphate microparticles with controllable physicochemical properties.

Author

Galván-Chacón, Víctor P., Costa, Laura, Barata, David, and Habibovic, Pamela

Subjects

CALCIUM phosphate, MICROFLUIDICS, BONE substitutes, BIOACTIVE glasses, BONE grafting, FOCAL adhesions, BONE regeneration

Abstract

Affordable and therapeutically effective biomaterials are required for successful treatment of orthopaedic critical-size bone defects. Calcium phosphate (CaP) ceramics are widely used for bone repair and regeneration, however, further optimization of their properties and biological performance is still required. To improve the existing CaP bone graft substitutes, novel synthesis and production approaches are needed that provide a fine control over the chemical and physical properties and versatility in the delivery format. In this study, a microfluidic strategy for production of CaP microparticles with different sizes derived from highly monodisperse droplets is proposed for the controlled synthesis of bioactive CaP ceramics. Microfluidic droplets, that served as microreactors for CaP precipitation, allowed the production of different CaP phases, as well as strontium-substituted CaP. By varying the concentration of the precursor solution, microparticles with different porosity were obtained. The droplet microfluidic system allowed direct visualization and quantification of the reaction kinetics. Upon production and purification of the microparticles, the biocompatibility and bioactivity were tested in vitro using human mesenchymal stromal cells (hMSCs). Cell attachment was analysed by imaging of the cytoskeleton and focal adhesions Moreover, cell proliferation, metabolic activity, alkaline phosphatase activity and mRNA expression of a set of osteogenic markers were quantified. We demonstrated that droplet microfluidics is a functional technique for the synthesis of a range of bioactive CaP-based ceramics with controlled properties. Calcium phosphate (CaP) ceramics are widely applied synthetic biomaterials for repair and regeneration of damaged bone; yet, CaP bone graft substitutes require further improvement to fully replace natural bone grafts in challenging clinical situations. To this end, novel synthesis and production approaches are needed that provide a fine control over the chemical and physical properties. Here, we developed a microfluidic platform for production of CaP microparticles with different size, composition and porosity, derived from monodisperse droplets. We demonstrated that CaP microparticles produced using this platform supported growth and differentiation of human mesenchymal stromal cells. This platform is a useful tool for developing a variety of CaPs in a controlled manner to study their physicochemical properties in relation to their bioactivity. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2021

39. Advanced in silico validation framework for three-dimensional traction force microscopy and application to an in vitro model of sprouting angiogenesis.

Author

Barrasa-Fano, J., Shapeti, A., de Jong, J., Ranga, A., Sanz-Herrera, J.A., and Van Oosterwyck, H.

Subjects

FOCAL adhesions, GERMINATION, MICROSCOPY, SPROUTS, IMAGE processing

Abstract

[Display omitted] In the last decade, cellular forces in three-dimensional hydrogels that mimic the extracellular matrix have been calculated by means of Traction Force Microscopy (TFM). However, characterizing the accuracy limits of a traction recovery method is critical to avoid obscuring physiological information due to traction recovery errors. So far, 3D TFM algorithms have only been validated using simplified cell geometries, bypassing image processing steps or arbitrarily simulating focal adhesions. Moreover, it is still uncertain which of the two common traction recovery methods, i.e., forward and inverse, is more robust against the inherent challenges of 3D TFM. In this work, we established an advanced in silico validation framework that is applicable to any 3D TFM experimental setup and that can be used to correctly couple the experimental and computational aspects of 3D TFM. Advancements relate to the simultaneous incorporation of complex cell geometries, simulation of microscopy images of varying bead densities and different focal adhesion sizes and distributions. By measuring the traction recovery error with respect to ground truth solutions, we found that while highest traction recovery errors occur for cases with sparse and small focal adhesions, our implementation of the inverse method improves two-fold the accuracy with respect to the forward method (average error of 23% vs. 50%). This advantage was further supported by recovering cellular tractions around angiogenic sprouts in an in vitro model of angiogenesis. The inverse method recovered higher traction peaks and a clearer pulling pattern at the sprout protrusion tips than the forward method. Biomaterial performance is often studied by quantifying cell-matrix mechanical interactions by means of Traction Force Microscopy (TFM). However, 3D TFM algorithms are often validated in simplified scenarios, which do not allow to fully assess errors that could obscure physiological information. Here, we established an advanced in silico validation framework that mimics real TFM experimental conditions and that characterizes the expected errors of a 3D TFM workflow. We apply this framework to demonstrate the enhanced accuracy of a novel inverse traction recovery method that is illustrated in the context of an in vitro model of sprouting angiogenesis. Together, our study shows the importance of a proper traction recovery method to minimise errors and the need for an advanced framework to assess those errors. [ABSTRACT FROM AUTHOR]

Published

2021

40. Shell-adductor muscle attachment and Ca2+ transport in the bivalves Ostrea stentina and Anomia ephippium.

Author

Castro-Claros, Juan Diego, Checa, Antonio, Lucena, Cristina, Pearson, John R., and Salas, Carmen

Subjects

FOCAL adhesions, BIVALVES, EXTRACELLULAR matrix, MUSCLES, BIVALVE shells, MUSCLE cells

Abstract

Among bivalve muscles, the adductors are particularly important for animal survival because they control valve closure. Most studies have addressed the type and morphology of this muscle in bivalves but few have focused on the mechanism that anchors it to the shell myostracum layer. Moreover, the possible calcium transport mechanism through the adductor muscle cells to the myostracum shell layer, which is necessary for bivalve biomineralisation, has never been addressed. Our results indicate that the muscle cell-shell attachment is mediated by the outer mantle epithelial cell layer, here termed tendon cells. These cells are modified at the muscle scar zone by the presence of actin cytoskeletal bundles, which anchor cells to the extracellular matrix via focal adhesion (or focal contact) junctions at the basal side and to extrapallial matrix at the apical side, both rich in collagen. From apical focal adhesions, bundles of collagen-rich fibres cross the extrapallial space and penetrate the myostracum shell layer. The latter constitutes one of the strongest anchoring structures among invertebrates. Numerous vesicles protrude from the tendon cells into the extrapallial space. TEM-EDX analysis reveals the presence of Ca2+ inside some of these vesicles both in tendon cells and in the extrapallial space. This suggests a potential mechanism for calcium transport from cells to the myostracum. The interfaces between bivalve shells and muscular attachments are unique and of special interest as adhesive functional biomaterials, being one of the strongest invertebrate anchoring structures. We present an updated ultrastructural model of the adductor muscle-shell attachment. Muscle cells connect with the shell through epithelial 'tendon cells', which have a cytoskeleton of actin microfilaments that connect to the extracellular matrix via focal adhesions. Collagen-rich fibres arise from apical focal adhesions, cross the nanometric extrapallial space and penetrate the myostracum where they form an organic network. Calcium is present inside vesicles that are released into the extrapallial space. The lack of direct cellular control on secretion restricts the myostracal microstructure to prismatic aragonitic similar to its inorganic counterpart. Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published

2021

41. Julius Wolff Institute Researchers Report on Findings in Biology (Temporal regulation of BMP2 growth factor signaling in response to mechanical loading is linked to cytoskeletal and focal adhesion remodeling).

Abstract

A study conducted by researchers at the Julius Wolff Institute explores the relationship between mechanical loading and the signaling response to Bone Morphogenetic Proteins (BMP2) in bone development and regeneration. The study found that the intensity and duration of BMP2 signaling increased with increasing loading frequency, along with the number and size of focal adhesions. The researchers also discovered that interfering with cytoskeletal remodeling hindered focal adhesion remodeling, which plays a critical role in enhancing BMP2 responsiveness. This research has implications for the design of biomaterials that can locally enhance growth factor treatment at the site of injury. [Extracted from the article]

Published

2024

42. New Pancreatic Cancer Data Have Been Reported by Researchers at Pusan National University (Recycling machinery of integrin coupled with focal adhesion turnover via RAB11-UNC13D-FAK axis for migration of pancreatic cancer cells).

Abstract

Researchers at Pusan National University have reported new data on pancreatic cancer. The study focuses on the recycling of integrin, a protein involved in cell migration, and its role in the metastasis of pancreatic cancer. The researchers identified UNC13D as a prognostic factor for pancreatic cancer and found that it regulates the migration of cancer cells by coupling the recycling of endosomes with focal adhesion turnover. The study highlights the importance of UNC13D in promoting pancreatic cancer progression. [Extracted from the article]

Published

2024

43. Findings from Columbia University Provide New Insights into Science (Mdm2 requires Sprouty4 to regulate focal adhesion formation and metastasis independent of p53).

Abstract

A recent report from Columbia University highlights the multiple functions of the Mdm2 protein, which is known for its role in regulating the p53 tumor suppressor protein. The study found that Mdm2 can also regulate cell migration, invasion, cell spreading, and focal adhesion formation, independent of p53. The researchers discovered that Mdm2 downregulates the expression of Sprouty4, which is necessary for its effects on cell migration and metastasis. These findings provide new insights into the molecular mechanisms underlying metastasis and suggest that targeting Mdm2 and Sprouty4 could be a potential therapeutic strategy. [Extracted from the article]

Published

2024

44. Fudan University Researchers Reveal New Findings on Blood Transfusion (Acidic preconditioning induced intracellular acid adaptation to protect renal injury via dynamic phosphorylation of focal adhesion kinase-dependent activation of sodium...).

Abstract

New research from Fudan University explores the concept of acidic preconditioning (AP) and its potential protective effects on kidney injury. The study found that short-term, repetitive acidic stimulation can enhance a cell's ability to withstand subsequent adverse stress. In both in vitro and in vivo models, AP was shown to effectively mitigate hypoxia/reoxygenation (H/R) injury in kidney cells. The study also identified the involvement of the FAK/NOX4/NHE1 signaling pathway in maintaining intracellular pH homeostasis and promoting cytoskeletal remodeling. These findings provide evidence for the potential therapeutic application of AP in kidney injury. [Extracted from the article]

Published

2024

45. Research on Cell Membrane Described by a Researcher at University of California (Focal adhesion kinase signaling - tumor vulnerabilities and clinical opportunities).

Abstract

A recent research article titled "Focal adhesion kinase signaling - tumor vulnerabilities and clinical opportunities" discusses the role of focal adhesion kinase (FAK) in cell adhesion and its implications in cancer. FAK is a protein kinase that is activated by integrin receptor binding to extracellular matrix proteins. The article highlights the importance of FAK in cell motility, survival, and gene expression, as well as its association with tumor development and decreased survival in pancreatic and ovarian cancers. The researchers also discuss the potential of FAK inhibitors as a therapeutic strategy for targeting drug resistance in ovarian cancer. The article provides valuable insights into the mechanisms of FAK activation and signaling, as well as its potential as a target for combinatorial therapies. [Extracted from the article]

Published

2024

46. University of North Dakota Researcher Has Provided New Data on Hematopoietic Cell Growth Factors (Focal Adhesion Kinase and Colony Stimulating Factors: Intestinal Homeostasis and Innate Immunity Crosstalk).

Abstract

A recent study conducted by researchers at the University of North Dakota explores the role of hematopoietic cell growth factors in intestinal homeostasis and innate immunity crosstalk. The study highlights the importance of focal adhesion kinase (FAK) in cell mobility and its potential as a target for pharmaceutical intervention in intestinal healing. Additionally, the research examines the connection between FAK and innate immunity, specifically macrophage/monocyte chemotaxis and intracellular signaling cascades. The study emphasizes the critical role of colony stimulating factors (CSFs) in maintaining homeostasis within the intestinal mucosa through crosstalk between macrophages and epithelial cells. Further investigation into these connections may provide valuable insights into the immune system's role in healing and inflammatory diseases of the gut. [Extracted from the article]

Published

2024

47. Roles of CCN2 as a mechano-sensing regulator of chondrocyte differentiation.

Author

Nishida, Takashi and Kubota, Satoshi

Subjects

STRAINS & stresses (Mechanics), G protein coupled receptors, CELL differentiation, FOCAL adhesions, ION channels, QUORUM sensing

Abstract

Cellular communication network factor 2 (CCN2) is a cysteine-rich secreted matricellular protein that regulates various cellular functions including cell differentiation. CCN2 is highly expressed under several types of mechanical stress, such as stretch, compression, and shear stress, in mesenchymal cells including chondrocytes, osteoblasts, and fibroblasts. In particular, CCN2 not only promotes cell proliferation and differentiation of various cells but also regulates the stability of mRNA of TRPV4, a mechanosensitive ion channel in chondrocytes. Of note, CCN2 behaves like a biomarker to sense suitable mechanical stress, because CCN2 expression is down-regulated when chondrocytes are subjected to excessive mechanical stress. These findings suggest that CCN2 is a mechano-sensing regulator. CCN2 expression is regulated by the activation of various mechano-sensing signaling pathways, e.g., mechanosensitive ion channels, integrin-focal adhesion-actin dynamics, Rho GTPase family members, Hippo-YAP signaling, and G protein-coupled receptors. This review summarizes the characterization of mechanoreceptors involved in CCN2 gene regulation and discusses the role of CCN2 as a mechano-sensing regulator of mesenchymal cell differentiation, with particular focus on chondrocytes. [ABSTRACT FROM AUTHOR]

Published

2020

48. Bio-surface coated titanium scaffolds with cancellous bone-like biomimetic structure for enhanced bone tissue regeneration.

Author

Zhang, Bingjun, Li, Jia, He, Lei, Huang, Hao, and Weng, Jie

Subjects

TISSUE scaffolds, OSSEOINTEGRATION, BONE regeneration, MESENCHYMAL stem cells, CELL receptors, FOCAL adhesions, BIOLOGICAL interfaces

Abstract

In view of the fact that titanium (Ti)-based implants still face the problem of loosening and failure of the implants caused by the slow biological response, the low osseointegration rate and the implant bacterial infection in clinical application, we designed a cancellous bone-like biomimetic Ti scaffold using the template accumulated by sugar spheres as a pore-forming agent. And based on a modified surface mineralization process and mussel-like adhesion mechanism, a silicon-doped calcium phosphate composite coating (Van-pBNPs/pep@pSiCaP) with Vancomycin (Van)-loaded polydopamine (pDA)-modified albumin nanoparticles (Van-pBNPs) and cell adhesion peptides (GFOGER) was constructed on the surface of Ti scaffold for mimicking the extracellular matrix (ECM) microenvironment of natural bone matrix to induce greater tissue regeneration. The in vitro study demonstrated that this porous Ti scaffold with functional bio-surface could distinctly facilitate cell early adhesion and spreading, and activate the expression of α2β1 integrin receptor on the cell membrane through promoting the formation of focal adhesions (FAs) in bone marrow stromal cells (BMSCs), thus mediating greater osteogenic cell differentiation. And it could also effectively inhibit the adhesion and growth of Staphylococcus epidermidis, exhibiting good antibacterial properties. Moreover, the Van-pBNPs/pep@pSiCaP-Ti scaffolds showed enhanced in vivo bone-forming ability due to the contributions of bioactive chemical components and the natural cancellous bone-like macrostructure. This work offers a promising structural and functional bio-inspired strategy for designing metal implants with desirable ability of osteoinduction synergistically with antibacterial efficacy for promoting bone regeneration and infection prevention simultaneously. This manuscript describes a new method for making porous Ti scaffolds with a natural cancellous bone-like structure. Besides, a functional bio-surface was constructed on the bionic structure, mimicking some of the functions of the collagen-rich organic matrix and inorganic CaP nanocrystallites of native ECM of bone in chemical components and biological activities. This interconnected inter-pore opening structure encouraged the migration of cells among open macro-pores within the scaffold. In addition, the functionalized surface not only improved early cell adhesion, spreading, stimulated greater osteogenic differentiation of bone-forming cells, but also endowed the scaffold with excellent antibacterial effect. The biomimetic metal implant with multiple biomedical functions designed in this study has a great clinical application potential. This study represents a feasible method for the preparation of biomimetic structure of metal implants and the improvement of their surface biological activity. Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published

2020

49. Focal adhesion displacement magnitude is a unifying feature of tensional homeostasis.

Author

Xu, Han, Donegan, Stephanie, Dreher, Jordan M., Stark, Alicia J., Canović, Elizabeth P., Stamenović, Dimitrije, and Smith, Michael L.

Subjects

FOCAL adhesions, VASCULAR smooth muscle, MUSCLE cells, EXTRACELLULAR matrix, ENDOTHELIAL cells

Abstract

Tensional homeostasis is widely recognized to exist at the length scales of organs and tissues, but the cellular length scale mechanism for tension regulation is not known. In this study, we explored whether tensional homeostasis emerges from the behavior of the individual focal adhesion (FA), which is the subcellular structure that transmits cell stress to the surrounding extracellular matrix. Past studies have suggested that cell contractility builds up until a certain displacement is achieved, and we thus hypothesized that tensional homeostasis may require a threshold level of substrate displacement. Micropattern traction microscopy was used to study a wide range of FA traction forces generated by bovine vascular smooth muscle cells and bovine aortic endothelial cells cultured on substrates of stiffness of 3.6, 6.7, 13.6, and 30 kPa. The most striking feature of FA dynamics observed here is that the substrate displacement resulting from FA traction forces is a unifying feature that determines FA tensional stability. Beyond approximately 1 μm of substrate displacement, FAs, regardless of cell type or substrate stiffness, exhibit a precipitous drop in temporal fluctuations of traction forces. These findings lead us to the conclusion that traction force dynamics collectively determine whether cells or cell ensembles develop tensional homeostasis, and this insight is necessary to fully understand how matrix stiffness impacts cellular behavior in healthy conditions and, more important, in pathological conditions such as cancer or vascular aging, where environmental stiffness is altered. Tensional homeostasis is widely recognized to exist at the length scales of organs and tissues, but the cellular length scale mechanism for tension regulation is not known. In this study, we explored whether tensional homeostasis emerges from the behavior of the individual focal adhesion (FA), which is the subcellular structure that transmits cell stress to the extracellular matrix. We utilized micropattern traction microscopy to measure time-lapses of FA forces in vascular smooth muscle cells and in endothelial cells. We discovered that the magnitude of the substrate displacement determines whether the FA has low temporal variability of traction forces. This finding is significant since it is the first known feature of tensional homeostasis that is broadly unifying across a range of environmental conditions and cell types. Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published

2020

50. Harnessing the perinuclear actin cap (pnAC) to influence nanocarrier trafficking and gene transfection efficiency in skeletal myoblasts using nanopillars.

Author

Chang, Ray, Yan, Qingfeng, Kingshott, Peter, Tsai, Wei-Bor, and Wang, Peng-Yuan

Subjects

GENE transfection, MYOBLASTS, CELL morphology, FOCAL adhesions, CELL nuclei, CELL suspensions

Abstract

Gene transfection is important in biotechnology and is used to modify cells intrinsically. It can be conducted in cell suspension or after cell adhesion, where the efficiency is dependent on many factors such as the type of nanocarrier used and cell division processes. Anchor-dependent cells are sensitive to the substrate they are attached to and adapt their behavior accordingly, including plasmid trafficking during gene transfection. Previously, it was shown in our group that the cytoskeleton is an essential factor in influencing gene transfection in skeletal myoblasts using nanogrooves as a substrate. In this study, the effect of the cytoskeleton on gene transfection efficiency of skeletal myoblasts was studied using various nanopillars and nanocarriers. Nanopillars with different diameters (200-1000 nm) and depths (200 or 400 nm) were fabricated using colloidal self-assembly and reactive ion etching. All surfaces were treated with oxygen plasma or polydopamine (PD) to further control cell morphology. Plasmid DNA was delivered into cells using jetPRIME or Lipofectamine 3000 nanocarriers. After screening hundreds of images, two distinguishable F-actin distributions were found, i.e., cells with or without a perinuclear actin cap (pnAC). Cells attached to nanopillars, especially the deep pillars, had a smaller spreading area, shorter F-actin, more 3D-like cell nuclei, and a lower percentage of pnAC, which lead to a higher gene transfection efficiency using jetPRIME. On the other hand, cells attached to the shallow nanopillars or flat surfaces had a larger spreading area, longer F-actin, more 2D-like cell nuclei, and a higher percentage of pnAC that facilitates gene transfection using Lipofectamine. The effects of cell density, cytoskeleton (cytoD), and focal adhesions (RGD) on gene transfection were also studied, and the results were consistent with our hypothesis that F-actin distribution is one of the critical factors in gene transfection. In conclusion, pnAC plays a vital role in the intracellular trafficking of nanocarrier/plasmid complexes and this study provides new insights into gene transfection in anchor-dependent cells. This study provides a new perspective in gene transfection using attached cells where perinuclear actin cap (pnAC) is an essential factor involved in transfection efficiency. A series of nanopillars were used to harness cell and cytoskeleton morphology. Two distinguishable cytoskeletal structures were found including cells with or without pnAC. 2D-like cells with pnAC facilitate gene delivery using liposome-based nanocarriers, while 3D-like cells without pnAC benefit gene delivery using cationic polymer-based nanocarriers. This study reveals the importance of the cytoskeleton during gene transfection that is beneficial in tissue transfection. Image, graphical abstract [ABSTRACT FROM AUTHOR]

Published

2020