Your search keyword '"FGF"' showing total 3,041 results

1. Inflammatory Mediators Suppress FGFR2 Expression in Human Keratinocytes to Promote Inflammation.

Author

Ferrarese, Luca, Koch, Michael, Baumann, Artemis, Bento-Lopes, Liliana, Wüst, Daria, Berest, Ivan, Kopf, Manfred, and Werner, Sabine

Subjects

*HOMEOSTASIS, *ATOPIC dermatitis, *INFLAMMATORY mediators, *CONDITIONED response, *KERATINOCYTES, *FIBROBLAST growth factors

Abstract

Fibroblast growth factors (FGFs) are key orchestrators of development, tissue homeostasis and repair. FGF receptor (FGFR) deficiency in mouse keratinocytes causes an inflammatory skin phenotype with similarities to atopic dermatitis, but the human relevance is unclear. Therefore, we generated human keratinocytes with a CRISPR/Cas9-induced knockout of FGFR2. Loss of this receptor promoted the expression of interferon-stimulated genes and pro-inflammatory cytokines under homeostatic conditions and in particular in response to different inflammatory mediators. Expression of FGFR2 itself was strongly downregulated in cultured human keratinocytes exposed to various pro-inflammatory stimuli. This is relevant in vivo, because bioinformatics analysis of bulk and single-cell RNA-seq data showed strongly reduced expression of FGFR2 in lesional skin of atopic dermatitis patients, which likely aggravates the inflammatory phenotype. These results reveal a key function of FGFR2 in human keratinocytes in the suppression of inflammation and suggest a role of FGFR2 downregulation in the pathogenesis of atopic dermatitis and possibly other inflammatory diseases. [ABSTRACT FROM AUTHOR]

Published

2024

2. Cell type specification and diversity in subpallial organoids.

Author

Pavon, Narciso, Yubing Sun, and ChangHui Pak

Subjects

MEDIUM spiny neurons, GABAERGIC neurons, CELL differentiation, NEURAL development, FETAL development

Abstract

Neural organoids have emerged as valuable tools for studying the developing brain, sparking enthusiasm and driving their adoption in disease modeling, drug screening, and investigating fetal neural development. The increasing popularity of neural organoids as models has led to a wide range of methodologies aimed at continuous improvement and refinement. Consequently, research groups often improve and reconfigure protocols to create region-specific organoids, resulting in diverse phenotypes, including variations in morphology, gene expression, and cell populations. While these improvements are exciting, routine adoptions of such modifications and protocols in the research laboratories are often challenging due to the reiterative empirical testing necessary to validate the cell types generated. To address this challenge, we systematically compare the similarities and differences that exist across published protocols that generates subpallial-specific organoids to date. In this review, we focus specifically on exploring the production of major GABAergic neuronal subtypes, especially Medium Spiny Neurons (MSNs) and Interneurons (INs), from multiple subpallial organoid protocols. Importantly, we look to evaluate the cell type diversity and the molecular pathways manipulated to generate them, thus broadening our understanding of the existing subpallial organoids as well as assessing the in vitro applicability of specific patterning factors. Lastly, we discuss the current challenges and outlook on the improved patterning of region-specific neural organoids. Given the critical roles MSN and IN dysfunction play in neurological disorders, comprehending the GABAergic neurons generated by neural organoids will undoubtedly facilitate clinical translation. [ABSTRACT FROM AUTHOR]

Published

2024

3. A differentiation protocol for generating pancreatic delta cells from human pluripotent stem cells.

Author

Tongran Zhang, Nannan Wang, Zhiying Liao, Jingyi Chen, Hao Meng, Haopeng Lin, Tao Xu, Lihua Chen, Ling-Qiang Zhu, and Huisheng Liu

Subjects

PLURIPOTENT stem cells, HUMAN stem cells, STEM cells, ISLANDS of Langerhans, CELL differentiation

Abstract

In this protocol, we detail a seven-stage differentiation methodology for generating pancreatic delta cells (SC-delta cells) from human pluripotent stem cells (hPSCs). In the first step, definitive endoderm is generated by activin A and CHIR99021, followed by induction of primitive gut tube and posterior foregut by treatment with FGF7, SANT1, LDN193189, PdBU, and retinoic acid (RA). The subsequent endocrine generation and directed SC-delta cell induction is achieved by a combined treatment of the FGF7 with FGF2 during stage 4 and 5, together with RA, XXI, ALK5 inhibitor II, SANT1, Betacellulin and LDN193189. The planar cultivation is converted to a suspended system after stage 5, allowing cells to aggregate into delta cell-containing spheroids. The differentiation takes approximately 4-5 weeks for delta cell generation and an additional 1-2 weeks for cell expansion and evaluation. We believe that this amenable and simplified protocol can provide a stable source of SC-delta cells from efficient differentiation, facilitating further investigation of the physiological role of delta cells as well as refinement of islet cell therapeutic strategies. [ABSTRACT FROM AUTHOR]

Published

2024

4. The potential of fibroblast growth factor-21 and adiponectin as diagnostic biomarkers for type 2 diabetes mellitus: differential levels in response to treatments.

Author

Al-Qusous, Madleen Nabeel, Dwairi, Rami, and Hussein, Rasha Mohamed

Subjects

TYPE 2 diabetes, HYPOGLYCEMIC agents, DIABETES, BLOOD grouping & crossmatching, METFORMIN

Abstract

Background: Diabetes mellitus (DM) is a global epidemic disease affecting millions each year. Recent studies have suggested novel biomarkers that are linked to DM. This study aimed to measure the levels of fibroblast growth factor-21 (FGF-21) and adiponectin in the blood of patients with type 2 DM and to assess the variations in their levels in response to the type of treatments. The possible correlations with several biochemical parameters and the diagnostic potential of FGF-21 and adiponectin as biomarkers for DM were also investigated. Eighty subjects were classified into control, Type 2 DM patients who were treated with metformin, Type 2 DM patients who were treated with metformin + oral hypoglycemic agents (OHAs), and Type 2 DM patients who were treated with insulin + metformin + OHAs. Results: The metformin + OHAs group and the insulin + metformin + OHAs group had higher levels of FGF-21 when compared to the control group. The metformin + OHAs also had significantly higher adiponectin levels when compared to the control or metformin groups. The serum levels of FGF-21 in the diabetic subjects were negatively correlated with LDL, direct bilirubin, albumin, and insulin levels and positively correlated with the duration of DM. However, the serum levels of adiponectin in the diabetic subjects were negatively correlated with weight while positively correlated with potassium levels. Remarkably, FGF-21 and adiponectin were effective biomarkers for diagnosing DM with a specificity of 100% and 90% and sensitivity of 52.3% and 64.5%, respectively. Conclusion: These findings suggest that FGF-21 and adiponectin play crucial roles in DM diagnosis and prognosis and that their levels change depending on the treatment type. [ABSTRACT FROM AUTHOR]

Published

2024

5. VEGF-dependent testicular vascularisation involves MEK1/2 signalling and the essential angiogenesis factors, SOX7 and SOX17.

Author

Blücher, Rheannon O., Lim, Rachel S., Ritchie, Matthew E., and Western, Patrick S.

Subjects

*SERTOLI cells, *MITOGEN-activated protein kinases, *SOMATIC cells, *CELL migration, *BASAL lamina

Abstract

Background: Abnormalities of in utero testis development are strongly associated with reproductive health conditions, including male infertility and testis cancer. In mouse testes, SOX9 and FGF9 support Sertoli cell development, while VEGF signalling is essential for the establishment of vasculature. The mitogen-activated protein kinase (MAPK) pathway is a major signalling cascade, essential for cell proliferation, differentiation and activation of Sry during primary sex-determination, but little is known about its function during fetal testis morphogenesis. We explored potential functions of MAPK signalling immediately after the establishment of testis cords in embryonic day (E)12.5 Oct4-eGFP transgenic mouse testes cultured using a MEK1/2 inhibitor. Results: RNA sequencing in isolated gonadal somatic cells identified 116 and 114 differentially expressed genes after 24 and 72 h of MEK1/2 inhibition, respectively. Ingenuity Pathway Analysis revealed an association of MEK1/2 signalling with biological functions such as angiogenesis, vasculogenesis and cell migration. This included a failure to upregulate the master transcriptional regulators of vascular development, Sox7 and Sox17, VEGF receptor genes, the cell adhesion factor gene Cd31 and a range of other endothelial cell markers such as Cdh5 (encoding VE-cadherin) and gap junction genes Gja4 and Gja5. In contrast, only a small number of Sertoli cell enriched genes were affected. Immunofluorescent analyses of control testes revealed that the MEK1/2 downstream target, ERK1/2 was phosphorylated in endothelial cells and Sertoli cells. Inhibition of MEK1/2 eliminated pERK1/2 in fetal testes, and CD31, VE-cadherin, SOX7 and SOX17 and endothelial cells were lost. Consistent with a role for VEGF in driving endothelial cell development in the testis, inhibition of VEGFR also abrogated pERK1/2 and SOX7 and SOX17 expressing endothelial cells. Moreover, while Sertoli cell proliferation and localisation to the testis cord basement membrane was disrupted by inhibition of MEK1/2, it was unaffected by VEGFR inhibition. Instead, inhibition of FGF signalling compromised Sertoli cell proliferation and localisation to the testis cord basement membrane. Conclusions: Together, our data highlight an essential role for VEGF-dependent MEK1/2 signalling in promoting vasculature and indicate that FGF signalling through MEK1/2 regulates Sertoli cell organisation in the developing mouse testis. [ABSTRACT FROM AUTHOR]

Published

2024

6. An "R‐spondin code" for multimodal signaling ON‐OFF states.

Author

Niehrs, Christof, Seidl, Carina, and Lee, Hyeyoon

Subjects

*GROWTH factors, *MEMBRANE proteins, *STEM cell factor, *WNT signal transduction, *BINDING site assay

Abstract

R‐spondins (RSPOs) are a family of secreted proteins and stem cell growth factors that are potent co‐activators of Wnt signaling. Recently, RSPO2 and RSPO3 were shown to be multifunctional, not only amplifying Wnt‐ but also binding BMP‐ and FGF receptors to downregulate signaling. The common mechanism underlying these diverse functions is that RSPO2 and RSPO3 act as "endocytosers" that link transmembrane proteins to ZNRF3/RNF43 E3 ligases and trigger target internalization. Thus, RSPOs are natural protein targeting chimeras for cell surface proteins. Conducting data mining and cell surface binding assays we report additional candidate RSPO targets, including SMO, PTC1,2, LGI1, ROBO4, and PTPR(F/S). We propose that there is an "R‐spondin code" that imparts combinatorial signaling ON‐OFF states of multiple growth factors. This code involves the modular RSPO domains, notably distinct motifs in the divergent RSPO‐TSP1 domains to mediate target interaction and internalization. The RSPO code offers a novel framework for the understanding how diverse signaling pathways may be coordinately regulated in development and disease. [ABSTRACT FROM AUTHOR]

Published

2024

7. Tanycyte radial morphology and proliferation are influenced by fibroblast growth factor receptor 1 and high‐fat diet.

Author

Esteve, N. Alex, Rogers, Deborah J., Stagray, Jacob A., Mayeux, Holly, Nora, Glenae, Huval, Luke, and Smith, Karen Müller

Subjects

*FIBROBLAST growth factor receptors, *DENTATE gyrus, *WEIGHT gain, *GLUCOSE tolerance tests, *CEREBROSPINAL fluid, *HYPOTHALAMUS

Abstract

Fibroblast growth factor receptor 1 (FGFR1) is a widely expressed, membrane‐bound receptor that transduces extracellular signals from FGF ligands and cadherins, resulting in intracellular signals influencing cellular growth, proliferation, calcium, and transcription. FGF21 and FGF2 stimulate the proliferation of tanycytes, specialized radial astrocytes along the ventricle of the hypothalamus, and influence metabolism. Tanycytes are in a privileged position between the cerebrospinal fluid, the blood supply in the median eminence, and neurons within nuclei in the hypothalamus. The effect of FGFR1 signaling upon tanycyte morphology and metabolism was examined in adult mice with conditional deletion of the Fgfr1 gene using the Fgfr1flox/flox; Nestin‐Cre+ line. Loss of Fgfr1 resulted in shorter β tanycytes along the medial eminence. Control Fgfr1flox/flox littermates and Fgfr1flox/flox, Nestin‐Cre+ (Fgfr1 cKO) knockout mice were placed on a 1‐month long high‐fat diet (HFD) or a normal‐fat diet (NFD), to investigate differences in body homeostasis and tanycyte morphology under an obesity inducing diet. We found that FGFR1 is a vital contributor to tanycyte morphology and quantity and that it promotes stem cell maintenance in the hypothalamus and hippocampal dentate gyrus. The Fgfr1 cKO mice developed impaired tolerance to a glucose challenge test on a HFD without gaining more weight than control mice. The combination of HFD and loss of Fgfr1 gene resulted in altered β and α tanycyte morphology, and reduced stem cell numbers along the third ventricle of the hypothalamus and hippocampus. [ABSTRACT FROM AUTHOR]

Published

2024

8. FGF18 impairs blastocyst viability, DNA double-strand breaks and maternal recognition of pregnancy genes.

Author

Goetten, André Lucio Fontana, Barreta, Marcos Henrique, Pinto da Silva, Yago, Bertolin, Kalyne, Koch, Júlia, Rocha, Cecilia Constantino, Dias Gonçalves, Paulo Bayard, Price, Christopher Alan, Antoniazzi, Alfredo Quites, and Portela, Valerio Marques

Subjects

*DOUBLE-strand DNA breaks, *DNA repair, *BLASTOCYST, *GRANULOSA cells, *PREGNANCY, *DNA damage

Abstract

Embryonic mortality in cattle is high, reaching 10–40 % in vivo and 60–70 % in vitro. Death of embryos involves reduced expression of genes related to embryonic viability, inhibition of DNA repair and increased DNA damage. In follicular granulosa cells, FGF18 from the theca layer increases apoptosis and DNA damage, so we hypothesized that FGF18 may also affect the oocyte and contribute to early embryonic death. The aims of this study were to identify the effects of FGF18 on cumulus expansion, oocyte maturation and embryo development from cleavage to blastocyst stage using a conventional bovine in vitro embryo production system using ovaries of abattoir origin. Addition of FGF18 during in-vitro maturation did not affect FSH-induced cumulus expansion or rates of nuclear maturation. When FGF18 was present in the culture system, rates of cleavage were not affected however, blastocyst and expanded blastocyst development was substantially inhibited (P < 0.05), indicating a delay of blastulation. The number of phosphorylated histone H2AFX foci per nucleus, a marker of DNA damage, was higher in cleavage-stage embryos cultured with FGF18 than in those from control group (P < 0.05). Furthermore, FGF18 decreased accumulation of PTGS2 and IFNT2 mRNA in blastocysts. In conclusion, these novel findings suggest that FGF18 plays a role in the regulation of embryonic death during the early stages of development by impairing DNA double-strand break repair and expression of genes associated with embryo viability and maternal recognition of pregnancy during the progression from oocyte to expanded blastocysts. • FGF18 had no effect on cumulus expansion, oocyte nuclear maturation, or embryo development from cleavage stage. • FGF18 added during IVM increased DNA double-strand breaks in cleavage-stage embryos. • FGF18 impaired development to the blastocyst and expanded blastocyst stages. • FGF18 added during embryo culture reduced abundance of PTGS2 mRNA, an embryo viability marker, and mRNA encoding IFNT2, a protein responsible for maternal recognition of pregnancy. [ABSTRACT FROM AUTHOR]

Published

2024

9. The effects of Quercetin on wound healing in the human umbilical vein endothelial cells.

Author

Kartal, Bahar, Alimogullari, Ebru, Elçi, Pınar, Fatsa, Tugba, and Ören, Sema

Abstract

An injury that affects the integrity of the skin, either inside or externally, is called a wound. Damaged tissue is repaired by a set of cellular and molecular mechanisms known as wound healing. Quercetin, a naturally occurring flavonoid, may hasten the healing of wounds. The study's objective was to investigate any potential impacts of quercetin on the wound-healing process. Human umbilical vein endothelial cells (HUVECs) were treated to varying dose ranges of quercetin (5–320 nM) for 24 and 48 h. Cultured cells were evaluated by using the MTT analysis, wound scratch assay and vascular tube formation. Furthermore the gene expression of VEGF and FGF were evaluated by qRT-PCR to determine the effects of quercetin on angiogenezis and wound repair. Positive effects of quercetin on cellular viability were demonstrated by the MTT experiment. In HUVECs quercetin promoted tube formation, migration, and proliferation while also averting wound breakage. Moreover, quercetin increased the expression of the FGF and VEGF genes, which aid in the healing of wounds in HUVECs. Quercetin may be bioactive molecule that successfully speeds up wound healing by regulating the vasculogenezis and healing cells. [ABSTRACT FROM AUTHOR]

Published

2024

10. The potential of fibroblast growth factor-21 and adiponectin as diagnostic biomarkers for type 2 diabetes mellitus: differential levels in response to treatments

Author

Madleen Nabeel Al-Qusous, Rami Dwairi, and Rasha Mohamed Hussein

Subjects

Diabetes, Biomarker, FGF, ELISA, Adiponectin, Medicine (General), R5-920, Science

Abstract

Abstract Background Diabetes mellitus (DM) is a global epidemic disease affecting millions each year. Recent studies have suggested novel biomarkers that are linked to DM. This study aimed to measure the levels of fibroblast growth factor-21 (FGF-21) and adiponectin in the blood of patients with type 2 DM and to assess the variations in their levels in response to the type of treatments. The possible correlations with several biochemical parameters and the diagnostic potential of FGF-21 and adiponectin as biomarkers for DM were also investigated. Eighty subjects were classified into control, Type 2 DM patients who were treated with metformin, Type 2 DM patients who were treated with metformin + oral hypoglycemic agents (OHAs), and Type 2 DM patients who were treated with insulin + metformin + OHAs. Results The metformin + OHAs group and the insulin + metformin + OHAs group had higher levels of FGF-21 when compared to the control group. The metformin + OHAs also had significantly higher adiponectin levels when compared to the control or metformin groups. The serum levels of FGF-21 in the diabetic subjects were negatively correlated with LDL, direct bilirubin, albumin, and insulin levels and positively correlated with the duration of DM. However, the serum levels of adiponectin in the diabetic subjects were negatively correlated with weight while positively correlated with potassium levels. Remarkably, FGF-21 and adiponectin were effective biomarkers for diagnosing DM with a specificity of 100% and 90% and sensitivity of 52.3% and 64.5%, respectively. Conclusion These findings suggest that FGF-21 and adiponectin play crucial roles in DM diagnosis and prognosis and that their levels change depending on the treatment type.

Published

2024

11. Comprehensive analysis of transcription factors involved in odontoblast differentiation mechanism.

Author

Nakazato, Haruka, Onodera, Shoko, Aida, Natsuko, Furusawa, Masahiro, and Azuma, Toshifumi

Subjects

*FIBROBLAST growth factors, *NOTCH signaling pathway, *GENE expression, *TRANSCRIPTION factors, *NOTCH genes, *BLOOD coagulation factor IX

Abstract

Primary cultured odontoblasts rapidly lose their tissue-specific phenotype. To identify transcription factors (TF) that are important for the maintenance of the odontoblast phenotype, primary cultures of C57BL/6 J mouse dental mesenchymal cells (DMC) were isolated, and expression of TF and odontoblast marker genes in cells immediately after isolation and 2 days after culture were comprehensively evaluated and compared using RNA-sequencing (RNA-seq). The expression of odontoblast markers in mouse dental mesenchymal cells decreased rapidly after isolation. In addition, the expression of Hedgehog-related, Notch-related, and immediate- early gene (IEG)-related transcription factors significantly decreased. Forced expression of these genes in lentiviral vectors, together with fibroblast growth factor 4 (FGF4), fibroblast growth factor 9 (FGF9), and the Wnt pathway activator CHIR99021, significantly induced the expression of odontogenic marker genes. These results indicate, for the first time, that Notch signaling and early genes may be important for maintaining odontoblast cultures. Furthermore, simultaneous stimulation of FGF, Wnt, Hedgehog, Notch pathways, and IEG transcription factors cooperatively promoted the maintenance of the odontoblast phenotype. These results suggest that the Hedgehog and Notch signaling pathways may play an important role in maintaining odontoblast phenotypes, in addition to FGF and Wnt signaling. [ABSTRACT FROM AUTHOR]

Published

2024

12. Skeletal dysmorphology and mineralization defects in Fgf20 KO mice.

Author

Dlugosova, Sylvie, Spoutil, Frantisek, Madureira Trufen, Carlos Eduardo, Ogan, Betul Melike, Prochazkova, Michaela, Fedosieieva, Olha, Nickl, Petr, Novaliches, Goretti Aranaz, Sedlacek, Radislav, and Prochazka, Jan

Subjects

FIBROBLAST growth factors, COMPACT bone, BONE growth, CANCELLOUS bone, VOLUMETRIC analysis

Abstract

Introduction: Fibroblast growth factor 20 (Fgf20), a member of the Fgf9 subfamily, was identified as an important regulator of bone differentiation and homeostasis processes. However, the role of Fgf20 in bone physiology has not been approached yet. Here we present a comprehensive bone phenotype analysis of mice with functional ablation of Fgf20. Methods: The study conducts an extensive analysis of Fgf20 knockout mice compared to controls, incorporating microCT scanning, volumetric analysis, Fgf9 subfamily expression and stimulation experiment and histological evaluation. Results: The bone phenotype could be detected especially in the area of the lumbar and caudal part of the spine and in fingers. Regarding the spine, Fgf20-/- mice exhibited adhesions of the transverse process of the sixth lumbar vertebra to the pelvis as well as malformations in the distal part of their tails. Preaxial polydactyly and polysyndactyly in varying degrees of severity were also detected. High resolution microCT analysis of distal femurs and the fourth lumbar vertebra showed significant differences in structure and mineralization in both cortical and trabecular bone. These findings were histologically validated and may be associated with the expression of Fgf20 in chondrocytes and their progenitors. Moreover, histological sections demonstrated increased bone tissue formation, disruption of Fgf20-/- femur cartilage, and cellular-level alterations, particularly in osteoclasts. We also observed molar dysmorphology, including root taurodontism, and described variations in mineralization and dentin thickness. Discussion: Our analysis provides evidence that Fgf20, together with other members of the Fgf9 subfamily, plays a crucial regulatory role in skeletal development and bone homeostasis. [ABSTRACT FROM AUTHOR]

Published

2024

13. Quantitative and qualitative differences in the activation of a fibroblast growth factor receptor by different FGF ligands.

Author

Krzyscik, Mateusz A., Karl, Kelly, Dudeja, Pooja, Krejci, Pavel, and Hristova, Kalina

Subjects

*FIBROBLAST growth factor receptors, *PROTEIN-tyrosine kinases, *LIGANDS (Biochemistry), *SIGNALS & signaling

Abstract

The FGF system is the most complex of all receptor tyrosine kinase signaling networks with 18 FGF ligands and four FGFRs that deliver morphogenic signals to pattern most embryonic structures. Even when a single FGFR is expressed in the tissue, different FGFs can trigger dramatically different biological responses via this receptor. Here we show both quantitative and qualitative differences in the signaling of one of the FGF receptors, FGFR1c, in response to different FGFs. We provide an overview of the recent discovery that FGFs engage in biased signaling via FGFR1c. We discuss the concept of ligand bias, which represents qualitative differences in signaling as it is a measure of differential ligand preferences for different downstream responses. We show how FGF ligand bias manifests in functional data in cultured chondrocyte cells. We argue that FGF-ligand bias contributes substantially to FGF-driven developmental processes, along with known differences in FGF expression levels, FGF-FGFR binding coefficients and differences in FGF stability in vivo. [Display omitted] • We overview the recent discovery that FGFs engage in biased signaling via FGFR1c. • We discuss the concept of ligand bias, which represents qualitative differences in signaling. • We show how FGF ligand bias manifests in functional data. • We argue that FGF-ligand bias contributes to FGF-driven developmental processes. [ABSTRACT FROM AUTHOR]

Published

2024

14. Glycosylation of FGF/FGFR: An underrated sweet code regulating cellular signaling programs.

Author

Gędaj, Aleksandra, Gregorczyk, Paulina, Żukowska, Dominika, Chorążewska, Aleksandra, Ciura, Krzysztof, Kalka, Marta, Porębska, Natalia, and Opaliński, Łukasz

Subjects

*HOMEOSTASIS, *POST-translational modification, *CELL communication, *FIBROBLAST growth factors, *GLYCOSYLATION, *CELL physiology, *GALECTINS

Abstract

Fibroblast growth factors (FGFs) and their receptors (FGFRs) constitute plasma-membrane localized signaling hubs that transmit signals from the extracellular environment to the cell interior, governing pivotal cellular processes like motility, metabolism, differentiation, division and death. FGF/FGFR signaling is critical for human body development and homeostasis; dysregulation of FGF/FGFR units is observed in numerous developmental diseases and in about 10% of human cancers. Glycosylation is a highly abundant posttranslational modification that is critical for physiological and pathological functions of the cell. Glycosylation is also very common within FGF/FGFR signaling hubs. Vast majority of FGFs (15 out of 22 members) are N-glycosylated and few FGFs are O-glycosylated. Glycosylation is even more abundant within FGFRs; all FGFRs are heavily N-glycosylated in numerous positions within their extracellular domains. A growing number of studies points on the multiple roles of glycosylation in fine-tuning FGF/FGFR signaling. Glycosylation modifies secretion of FGFs, determines their stability and affects interaction with FGFRs and co-receptors. Glycosylation of FGFRs determines their intracellular sorting, constitutes autoinhibitory mechanism within FGFRs and adjusts FGF and co-receptor recognition. Sugar chains attached to FGFs and FGFRs constitute also a form of code that is differentially decrypted by extracellular lectins, galectins, which transform FGF/FGFR signaling at multiple levels. This review focuses on the identified functions of glycosylation within FGFs and FGFRs and discusses their relevance for the cell physiology in health and disease. [Display omitted] • FGF/FGFR signaling plays a pivotal role in establishing and maintaining the cell and organism homeostasis. • Vast majority of FGF proteins and all FGFRs are N-glycosylated. • N- and O-glycosylation of FGFs affects their secretion, stability and function. • N-glycosylation of FGFRs facilitates intracellular trafficking of FGFRs to the cell surface and regulates FGFRs interaction with FGFs and co-receptors. • N-glycosylation of FGFs and FGFRs constitutes a layer of information differentially read by galectins and transformed into specific modulatory activities. [ABSTRACT FROM AUTHOR]

Published

2024

15. Cell type specification and diversity in subpallial organoids

Author

Narciso Pavon, Yubing Sun, and ChangHui Pak

Subjects

brain region-specific organoids, neural organoids, shh, fgf, patterning, subpallium, Genetics, QH426-470

Abstract

Neural organoids have emerged as valuable tools for studying the developing brain, sparking enthusiasm and driving their adoption in disease modeling, drug screening, and investigating fetal neural development. The increasing popularity of neural organoids as models has led to a wide range of methodologies aimed at continuous improvement and refinement. Consequently, research groups often improve and reconfigure protocols to create region-specific organoids, resulting in diverse phenotypes, including variations in morphology, gene expression, and cell populations. While these improvements are exciting, routine adoptions of such modifications and protocols in the research laboratories are often challenging due to the reiterative empirical testing necessary to validate the cell types generated. To address this challenge, we systematically compare the similarities and differences that exist across published protocols that generates subpallial-specific organoids to date. In this review, we focus specifically on exploring the production of major GABAergic neuronal subtypes, especially Medium Spiny Neurons (MSNs) and Interneurons (INs), from multiple subpallial organoid protocols. Importantly, we look to evaluate the cell type diversity and the molecular pathways manipulated to generate them, thus broadening our understanding of the existing subpallial organoids as well as assessing the in vitro applicability of specific patterning factors. Lastly, we discuss the current challenges and outlook on the improved patterning of region-specific neural organoids. Given the critical roles MSN and IN dysfunction play in neurological disorders, comprehending the GABAergic neurons generated by neural organoids will undoubtedly facilitate clinical translation.

Published

2024

16. Molecular Pathways and Animal Models of Truncus Arteriosus

Author

Gill, Eleanor, Bamforth, Simon D., Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, Rickert-Sperling, Silke, editor, Kelly, Robert G., editor, and Haas, Nikolaus, editor

Published

2024

17. Xbra modulates the activity of linker region phosphorylated Smad1 during Xenopus development

Author

Santosh Kumar, Zobia Umair, Vijay Kumar, Ravi Shankar Goutam, Soochul Park, Unjoo Lee, and Jaebong Kim

Subjects

Xbra, Bmp4, Smad1, Smad4, Fgf, Erk, Medicine, Science

Abstract

Abstract The Bmp/Smad1 pathway plays a crucial role in developmental processes and tissue homeostasis. Mitogen-activated protein kinase (Mapk)/Erk mediated phosphorylation of Smad1 in the linker region leads to Smad1 degradation, cytoplasmic retention and inhibition of Bmp/Smad1 signaling. While Fgf/Erk pathway has been documented to inhibit Bmp/Smad1 signaling, several studies also suggests the cooperative interaction between these two pathways in different context. However, the precise role and molecular pathway of this collaborative interaction remain obscure. Here, we identified Xbra induced by Fgf/Erk signaling as a factor in a protective mechanism for Smad1. Xbra physically interacted with the linker region phosphorylated Smad1 to make Xbra/Smad1/Smad4 trimeric complex, leading to Smad1 nuclear localization and protecting it from ubiquitin-mediated proteasomal degradation. This interaction of Xbra/Smad1/Smad4 led to sustained nuclear localization of Smad1 and the upregulation of lateral mesoderm genes, while concurrently suppression of neural and blood forming genes. Taken together, the results suggests Xbra-dependent cooperative interplays between Fgf/Erk and Bmp/Smad1 signaling during lateral mesoderm specification in Xenopus embryos.

Published

2024

18. Skin advanced glycation end-products as indicators of the metabolic profile in diabetes mellitus: correlations with glycemic control, liver phenotypes and metabolic biomarkers

Author

Grigorios Christidis, Frederic Küppers, Senem Ceren Karatayli, Ersin Karatayli, Susanne N. Weber, Frank Lammert, and Marcin Krawczyk

Subjects

AGE, Diabetes, FGF, GDF15, Liver fibrosis, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Abstract Introduction The production of advanced glycation end-products (AGEs) is a key pathomechanism related to the complications of diabetes mellitus. The measurement of HbA1c as one of the AGEs is widely used in the clinic, but also other proteins undergo glycation in the course of diabetes. Here, we measure skin AGEs (SAGEs) in patients with diabetes type 1 (DM1) and type 2 (DM2) and correlate them with metabolic markers as well as non-invasively measured liver fibrosis and steatosis. Patients and methods In this cross-sectional study, a total of 64 patients with either DM1 or DM2 and 28 healthy controls were recruited. SAGEs were measured using autofluorescence (AGE Reader). Liver fibrosis and steatosis were quantified using transient elastography, which determines liver stiffness measurement (LSM) and controlled attenuation parameter (CAP). FGF19, FGF21 and GDF-15 were measured in blood samples using ELISA. Results SAGEs were elevated in both groups of patients with diabetes as compared to healthy controls (both p

Published

2024

19. Xbra modulates the activity of linker region phosphorylated Smad1 during Xenopus development.

Author

Kumar, Santosh, Umair, Zobia, Kumar, Vijay, Goutam, Ravi Shankar, Park, Soochul, Lee, Unjoo, and Kim, Jaebong

Subjects

*HOMEOSTASIS, *XENOPUS, *MESODERM, *MITOGEN-activated protein kinases

Abstract

The Bmp/Smad1 pathway plays a crucial role in developmental processes and tissue homeostasis. Mitogen-activated protein kinase (Mapk)/Erk mediated phosphorylation of Smad1 in the linker region leads to Smad1 degradation, cytoplasmic retention and inhibition of Bmp/Smad1 signaling. While Fgf/Erk pathway has been documented to inhibit Bmp/Smad1 signaling, several studies also suggests the cooperative interaction between these two pathways in different context. However, the precise role and molecular pathway of this collaborative interaction remain obscure. Here, we identified Xbra induced by Fgf/Erk signaling as a factor in a protective mechanism for Smad1. Xbra physically interacted with the linker region phosphorylated Smad1 to make Xbra/Smad1/Smad4 trimeric complex, leading to Smad1 nuclear localization and protecting it from ubiquitin-mediated proteasomal degradation. This interaction of Xbra/Smad1/Smad4 led to sustained nuclear localization of Smad1 and the upregulation of lateral mesoderm genes, while concurrently suppression of neural and blood forming genes. Taken together, the results suggests Xbra-dependent cooperative interplays between Fgf/Erk and Bmp/Smad1 signaling during lateral mesoderm specification in Xenopus embryos. [ABSTRACT FROM AUTHOR]

Published

2024

20. A dual‐omics approach on the effects of fibroblast growth factor‐2 (FGF‐2) on ventral tegmental area dopaminergic neurons in response to alcohol consumption in mice.

Author

Hose, Leonie, Langenhagen, Alina Katharina, Kefalakes, Ekaterini, Schweitzer, Theresa, Kubinski, Sabrina, Barak, Segev, Pich, Andreas, and Grothe, Claudia

Subjects

*DOPAMINERGIC neurons, *ALCOHOL drinking, *FIBROBLAST growth factor 2, *FIBROBLASTS, *ALCOHOLISM, *DNA fingerprinting, *PROTEOMICS

Abstract

Harmful alcohol consumption is a major socioeconomic burden to the health system, as it can be the cause of mortality of heavy alcohol drinkers. The dopaminergic (DAergic) system is thought to play an important role in the pathogenesis of alcohol drinking behaviour; however, its exact role remains elusive. Fibroblast growth factor 2 (FGF‐2), a neurotrophic factor, associated with both the DAergic system and alcohol consumption, may play an important role in DAergic neuroadaptations during alcohol abuse. Within this study, we aimed to clarify the role of endogenous FGF‐2 on the DAergic system and whether there is a possible link to alcohol consumption. We found that lack of FGF‐2 reduces the alcohol intake of mice. Transcriptome analysis of DAergic neurons revealed that FGF‐2 knockout (FGF‐2 KO) shifts the molecular fingerprint of midbrain dopaminergic (mDA) neurons to DA subtypes of the ventral tegmental area (VTA). In line with this, proteomic changes predominantly appear also in the VTA. Interestingly, these changes led to an altered regulation of the FGF‐2 signalling cascades and DAergic pathways in a region‐specific manner, which was only marginally affected by voluntary alcohol consumption. Thus, lack of FGF‐2 not only affects the gene expression but also the proteome of specific brain regions of mDA neurons. Our study provides new insights into the neuroadaptations of the DAergic system during alcohol abuse and, therefore, comprises novel targets for future pharmacological interventions. [ABSTRACT FROM AUTHOR]

Published

2024

21. FGF‐stimulated tendon cells embrace a chondrogenic fate with BMP7 in newt tissue culture.

Author

Sugiura, Nao and Agata, Kiyokazu

Subjects

*CARTILAGE regeneration, *ENDOCHONDRAL ossification, *TISSUE culture, *FIBROBLAST growth factors, *PLATELET-derived growth factor, *TENDONS, *ELBOW joint, *NEWTS

Abstract

Newts can regenerate functional elbow joints after amputation at the joint level. Previous studies have suggested the potential contribution of cells from residual tendon tissues to joint cartilage regeneration. A serum‐free tissue culture system for tendons was established to explore cell dynamics during joint regeneration. Culturing isolated tendons in this system, stimulated by regeneration‐related factors, such as fibroblast growth factor (FGF) and platelet‐derived growth factor, led to robust cell migration and proliferation. Moreover, cells proliferating in an FGF‐rich environment differentiated into Sox9‐positive chondrocytes upon BMP7 introduction. These findings suggest that FGF‐stimulated cells from tendons may aid in joint cartilage regeneration during functional elbow joint regeneration in newts. [ABSTRACT FROM AUTHOR]

Published

2024

22. Skin advanced glycation end-products as indicators of the metabolic profile in diabetes mellitus: correlations with glycemic control, liver phenotypes and metabolic biomarkers.

Author

Christidis, Grigorios, Küppers, Frederic, Karatayli, Senem Ceren, Karatayli, Ersin, Weber, Susanne N., Lammert, Frank, and Krawczyk, Marcin

Subjects

*CROSS-sectional method, *STATISTICAL correlation, *PEARSON correlation (Statistics), *FATTY liver, *GLYCOSYLATED hemoglobin, *DATA analysis, *T-test (Statistics), *RESEARCH funding, *GLYCEMIC control, *ENZYME-linked immunosorbent assay, *KRUSKAL-Wallis Test, *ULTRASONIC imaging, *DESCRIPTIVE statistics, *FIBROSIS, *ADVANCED glycation end-products, *ONE-way analysis of variance, *STATISTICS, *LIVER, *COMPARATIVE studies, *HEALTH outcome assessment, *DATA analysis software, *DIABETES, *PHENOTYPES, *BIOMARKERS, *NONPARAMETRIC statistics

Abstract

Introduction: The production of advanced glycation end-products (AGEs) is a key pathomechanism related to the complications of diabetes mellitus. The measurement of HbA1c as one of the AGEs is widely used in the clinic, but also other proteins undergo glycation in the course of diabetes. Here, we measure skin AGEs (SAGEs) in patients with diabetes type 1 (DM1) and type 2 (DM2) and correlate them with metabolic markers as well as non-invasively measured liver fibrosis and steatosis. Patients and methods: In this cross-sectional study, a total of 64 patients with either DM1 or DM2 and 28 healthy controls were recruited. SAGEs were measured using autofluorescence (AGE Reader). Liver fibrosis and steatosis were quantified using transient elastography, which determines liver stiffness measurement (LSM) and controlled attenuation parameter (CAP). FGF19, FGF21 and GDF-15 were measured in blood samples using ELISA. Results: SAGEs were elevated in both groups of patients with diabetes as compared to healthy controls (both p < 0.001) and were higher in patients with DM2 in comparison to DM1 (p = 0.006). SAGEs correlated positively with HbA1c (r = 0.404, p < 0.001), CAP (r = 0.260, p = 0.016) and LSM (r = 0.356, p < 0.001), and negatively with insulin growth factor binding protein 3 (p < 0.001). We also detected a positive correlation between GDF15 and SAGEs (r = 0.469, p < 0.001). Conclusions: SAGEs are significantly elevated in patients with both DM types 1 and 2 and correlate with metabolic markers, including HbA1c and GDF15. They might also help to detect patients with advanced liver injury in the setting of diabetes. [ABSTRACT FROM AUTHOR]

Published

2024

23. Skeletal dysmorphology and mineralization defects in Fgf20 KO mice

Author

Sylvie Dlugosova, Frantisek Spoutil, Carlos Eduardo Madureira Trufen, Betul Melike Ogan, Michaela Prochazkova, Olha Fedosieieva, Petr Nickl, Goretti Aranaz Novaliches, Radislav Sedlacek, and Jan Prochazka

Subjects

Fgf, mineralization, bone, chondrocytes, bone homeostasis, polydactylia, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

IntroductionFibroblast growth factor 20 (Fgf20), a member of the Fgf9 subfamily, was identified as an important regulator of bone differentiation and homeostasis processes. However, the role of Fgf20 in bone physiology has not been approached yet. Here we present a comprehensive bone phenotype analysis of mice with functional ablation of Fgf20.MethodsThe study conducts an extensive analysis of Fgf20 knockout mice compared to controls, incorporating microCT scanning, volumetric analysis, Fgf9 subfamily expression and stimulation experiment and histological evaluation.ResultsThe bone phenotype could be detected especially in the area of​ the lumbar and caudal part of the spine and in fingers. Regarding the spine, Fgf20-/- mice exhibited adhesions of the transverse process of the sixth lumbar vertebra to the pelvis as well as malformations in the distal part of their tails. Preaxial polydactyly and polysyndactyly in varying degrees of severity were also detected. High resolution microCT analysis of distal femurs and the fourth lumbar vertebra showed significant differences in structure and mineralization in both cortical and trabecular bone. These findings were histologically validated and may be associated with the expression of Fgf20 in chondrocytes and their progenitors. Moreover, histological sections demonstrated increased bone tissue formation, disruption of Fgf20-/- femur cartilage, and cellular-level alterations, particularly in osteoclasts. We also observed molar dysmorphology, including root taurodontism, and described variations in mineralization and dentin thickness.DiscussionOur analysis provides evidence that Fgf20, together with other members of the Fgf9 subfamily, plays a crucial regulatory role in skeletal development and bone homeostasis.

Published

2024

24. Injury-induced cooperation of InhibinβA and JunB is essential for cell proliferation in Xenopus tadpole tail regeneration

Author

Makoto Nakamura, Tatsuya Kyoda, Hitoshi Yoshida, Kimiko Takebayashi-Suzuki, Ryota Koike, Eri Takahashi, Yuka Moriyama, Marcin Wlizla, Marko E. Horb, and Atsushi Suzuki

Subjects

InhibinβA, JunB, FGF, Xenopus tail regeneration, Regenerative cell proliferation, Medicine, Science

Abstract

Abstract In animal species that have the capability of regenerating tissues and limbs, cell proliferation is enhanced after wound healing and is essential for the reconstruction of injured tissue. Although the ability to induce cell proliferation is a common feature of such species, the molecular mechanisms that regulate the transition from wound healing to regenerative cell proliferation remain unclear. Here, we show that upon injury, InhibinβA and JunB cooperatively function for this transition during Xenopus tadpole tail regeneration. We found that the expression of inhibin subunit beta A (inhba) and junB proto-oncogene (junb) is induced by injury-activated TGF-β/Smad and MEK/ERK signaling in regenerating tails. Similarly to junb knockout (KO) tadpoles, inhba KO tadpoles show a delay in tail regeneration, and inhba/junb double KO (DKO) tadpoles exhibit severe impairment of tail regeneration compared with either inhba KO or junb KO tadpoles. Importantly, this impairment is associated with a significant reduction of cell proliferation in regenerating tissue. Moreover, JunB regulates tail regeneration via FGF signaling, while InhibinβA likely acts through different mechanisms. These results demonstrate that the cooperation of injury-induced InhibinβA and JunB is critical for regenerative cell proliferation, which is necessary for re-outgrowth of regenerating Xenopus tadpole tails.

Published

2024

25. Diverse contribution of amniogenic somatopleural cells to cardiovascular development: With special reference to thyroid vasculature

Author

Haneda, Yuka, Miyagawa‐Tomita, Sachiko, Uchijima, Yasunobu, Iwase, Akiyasu, Asai, Rieko, Kohro, Takahide, Wada, Youichiro, and Kurihara, Hiroki

Subjects

Biochemistry and Cell Biology, Bioinformatics and Computational Biology, Evolutionary Biology, Biological Sciences, Cardiovascular, Heart Disease, Stem Cell Research, Underpinning research, 1.1 Normal biological development and functioning, amniogenic somatopleure, angiogenesis, cardiovascular development, FGF, quail-chick chimera, thyroid development, VEGF, Medical and Health Sciences, Developmental Biology, Biochemistry and cell biology, Bioinformatics and computational biology, Evolutionary biology

Abstract

BackgroundThe somatopleure serves as the primordium of the amnion, an extraembryonic membrane surrounding the embryo. Recently, we have reported that amniogenic somatopleural cells (ASCs) not only form the amnion but also migrate into the embryo and differentiate into cardiomyocytes and vascular endothelial cells. However, detailed differentiation processes and final distributions of these intra-embryonic ASCs (hereafter referred to as iASCs) remain largely unknown.ResultsBy quail-chick chimera analysis, we here show that iASCs differentiate into various cell types including cardiomyocytes, smooth muscle cells, cardiac interstitial cells, and vascular endothelial cells. In the pharyngeal region, they distribute selectively into the thyroid gland and differentiate into vascular endothelial cells to form intra-thyroid vasculature. Explant culture experiments indicated sequential requirement of fibroblast growth factor (FGF) and vascular endothelial growth factor (VEGF) signaling for endothelial differentiation of iASCs. Single-cell transcriptome analysis further revealed heterogeneity and the presence of hemangioblast-like cell population within ASCs, with a switch from FGF to VEGF receptor gene expression.ConclusionThe present study demonstrates novel roles of ASCss especially in heart and thyroid development. It will provide a novel clue for understanding the cardiovascular development of amniotes from embryological and evolutionary perspectives.

Published

2022

26. The MEK-ERK signaling pathway promotes maintenance of cardiac chamber identity.

Author

Yao Yao, Gupta, Deepam, and Yelon, Deborah

Subjects

*CELLULAR signal transduction, *GENE expression, *ATRIUMS (Architecture), *MAINTENANCE, *PROVOCATION (Behavior), *BRACHYDANIO

Abstract

Ventricular and atrial cardiac chambers have unique structural and contractile characteristics that underlie their distinct functions. The maintenance of chamber-specific features requires active reinforcement, even in differentiated cardiomyocytes. Previous studies in zebrafish have shown that sustained FGF signaling acts upstream of Nkx factors to maintain ventricular identity, but the rest of this maintenance pathway remains unclear. Here, we show that MEK1/2-ERK1/2 signaling acts downstream of FGF and upstream of Nkx factors to promote ventricular maintenance. Inhibition of MEK signaling, like inhibition of FGF signaling, results in ectopic atrial gene expression and reduced ventricular gene expression in ventricular cardiomyocytes. FGF and MEK signaling both influence ventricular maintenance over a similar timeframe, when phosphorylated ERK (pERK) is present in the myocardium. However, the role of FGF-MEK activity appears to be context-dependent: some ventricular regions are more sensitive than others to inhibition of FGF-MEK signaling. Additionally, in the atrium, although endogenous pERK does not induce ventricular traits, heightened MEK signaling can provoke ectopic ventricular gene expression. Together, our data reveal chamber-specific roles of MEK-ERK signaling in the maintenance of ventricular and atrial identities. [ABSTRACT FROM AUTHOR]

Published

2024

27. Injury-induced cooperation of InhibinβA and JunB is essential for cell proliferation in Xenopus tadpole tail regeneration.

Author

Nakamura, Makoto, Kyoda, Tatsuya, Yoshida, Hitoshi, Takebayashi-Suzuki, Kimiko, Koike, Ryota, Takahashi, Eri, Moriyama, Yuka, Wlizla, Marcin, Horb, Marko E., and Suzuki, Atsushi

Subjects

*CELL proliferation, *REGENERATION (Biology), *TADPOLES, *WOUND healing, *XENOPUS

Abstract

In animal species that have the capability of regenerating tissues and limbs, cell proliferation is enhanced after wound healing and is essential for the reconstruction of injured tissue. Although the ability to induce cell proliferation is a common feature of such species, the molecular mechanisms that regulate the transition from wound healing to regenerative cell proliferation remain unclear. Here, we show that upon injury, InhibinβA and JunB cooperatively function for this transition during Xenopus tadpole tail regeneration. We found that the expression of inhibin subunit beta A (inhba) and junB proto-oncogene (junb) is induced by injury-activated TGF-β/Smad and MEK/ERK signaling in regenerating tails. Similarly to junb knockout (KO) tadpoles, inhba KO tadpoles show a delay in tail regeneration, and inhba/junb double KO (DKO) tadpoles exhibit severe impairment of tail regeneration compared with either inhba KO or junb KO tadpoles. Importantly, this impairment is associated with a significant reduction of cell proliferation in regenerating tissue. Moreover, JunB regulates tail regeneration via FGF signaling, while InhibinβA likely acts through different mechanisms. These results demonstrate that the cooperation of injury-induced InhibinβA and JunB is critical for regenerative cell proliferation, which is necessary for re-outgrowth of regenerating Xenopus tadpole tails. [ABSTRACT FROM AUTHOR]

Published

2024

28. Conditional Ablation of Spred1 and Spred2 in the Eye Lens Negatively Impacts Its Development and Growth.

Author

Wazin, Fatima and Lovicu, Frank J.

Subjects

*CELL differentiation, *CELL anatomy, *EPITHELIAL cells, *MICROPHTHALMIA, *CELL proliferation, *CRYSTALLINE lens

Abstract

The development and growth of the eye depends on normal lens morphogenesis and its growth. This growth, in turn, is dependent on coordinated proliferation of the lens epithelial cells and their subsequent differentiation into fiber cells. These cellular processes are tightly regulated to maintain the precise cellular structure and size of the lens, critical for its transparency and refractive properties. Growth factor-mediated MAPK signaling driven by ERK1/2 has been reported as essential for regulating cellular processes of the lens, with ERK1/2 signaling tightly regulated by endogenous antagonists, including members of the Sprouty and related Spred families. Our previous studies have demonstrated the importance of both these inhibitory molecules in lens and eye development. In this study, we build on these findings to highlight the importance of Spreds in regulating early lens morphogenesis by modulating ERK1/2-mediated lens epithelial cell proliferation and fiber differentiation. Conditional loss of both Spred1 and Spred2 in early lens morphogenesis results in elevated ERK1/2 phosphorylation, hyperproliferation of lens epithelia, and an associated increase in the rate of fiber differentiation. This results in transient microphakia and microphthalmia, which disappears, owing potentially to compensatory Sprouty expression. Our data support an important temporal role for Spreds in the early stages of lens morphogenesis and highlight how negative regulation of ERK1/2 signaling is critical for maintaining lens proliferation and fiber differentiation in situ throughout life. [ABSTRACT FROM AUTHOR]

Published

2024

29. Fibroblast growth factor-induced lens fiber cell elongation is driven by the stepwise activity of Rho and Rac.

Author

Yuki Sugiyama, Reed, Daniel A., Herrmann, David, Lovicu, Frank J., Robinson, Michael L., Timpson, Paul, and Masai, Ichiro

Subjects

*FIBROBLAST growth factors, *FIBROBLASTS, *CRYSTALLINE lens, *FIBERS

Abstract

The spheroidal shape of the eye lens is crucial for precise light focusing onto the retina. This shape is determined by concentrically aligned, convexly elongated lens fiber cells along the anterior and posterior axis of the lens. Upon differentiation at the lens equator, the fiber cells increase in height as their apical and basal tips migrate towards the anterior and posterior poles, respectively. The forces driving this elongation and migration remain unclear. We found that, in the mouse lens, membrane protrusions or lamellipodia are observed only in the maturing fibers undergoing cell curve conversion, indicating that lamellipodium formation is not the primary driver of earlier fiber migration. We demonstrated that elevated levels of fibroblast growth factor (FGF) suppressed the extension of Racdependent protrusions, suggesting changes in the activity of FGF controlling Rac activity, switching to lamellipodium-driven migration. Inhibitors of ROCK, myosin and actin reduced the height of both early and later fibers, indicating that elongation of these fibers relies on actomyosin contractility. Consistent with this, active RhoA was detected throughout these fibers. Given that FGF promotes fiber elongation, we propose that it does so through regulation of Rho activity. [ABSTRACT FROM AUTHOR]

Published

2024

30. Assessing angiogenesis factors as prognostic biomarkers in breast cancer patients and their association with clinicopathological factors.

Author

Abbasi-Dokht, Tannaz, Malek, Farhad, Nafissi, Nahid, Mohammadlou, Maryam, Sheikh, Maryam, Akbari, Sedigheh, Zargaran, Mohammad Hossein, and Baharlou, Rasoul

Subjects

*PROGNOSIS, *TRANSFORMING growth factors-beta, *VASCULAR endothelial growth factors, *EPIDERMAL growth factor, *BREAST cancer, *GROWTH factors

Abstract

Angiogenesis is fundamental for tumor growth and metastasis across many solid malignancies. Considerable interest has focused on the molecular regulation of tumor angiogenesis as a means to predict disease outcomes and guide therapeutic decisions. In the present study, we investigated the prognostic value of transforming growth factor beta (TGF-β), epidermal growth factor (EGF), fibroblast growth factor (FGF), delta-like ligand 4 (DLL4), and vascular endothelial growth factor (VEGF) in the serum of 120 women diagnosed with breast cancer using ELISA as well as examined their associations with clinical parameters and the outcome of the disease. Our results demonstrated that the serum concentration of TGF-β and EGF were remarkably higher in patients with higher tumor size, end stages of the disease, and positive lymph node involvement compared to patients with lower tumor size, early stages of the disease, and negative lymph node involvement. In addition, we found a significant correlation between the serum concentration of VEGF and the level of EGF, FGF, and DLL4 in patients with breast cancer. Furthermore, both univariate and multivariate analyses showed that TGF-β and EGF can be used as end-stage predictors. Based on our findings, increasing the level of angiogenesis factors is significantly associated with higher tumor size and late stages of the disease in patients with breast cancer. Moreover, measuring the level of angiogenesis factors could lead to better prediction of disease outcomes and choosing the best treatments for patients. [ABSTRACT FROM AUTHOR]

Published

2024

31. Molecular Targeting of the Fibroblast Growth Factor Receptor Pathway across Various Cancers.

Author

Shan, Khine S., Dalal, Shivani, Thaw Dar, Nyein Nyein, McLish, Omani, Salzberg, Matthew, and Pico, Brian A.

Subjects

*FIBROBLAST growth factors, *MONOCLONAL antibodies, *ANTIBODY-drug conjugates, *TRANSITIONAL cell carcinoma, *CELLULAR control mechanisms

Abstract

Fibroblast growth factor receptors (FGFRs) are a family of receptor tyrosine kinases that are involved in the regulation of cell proliferation, survival, and development. FGFR alterations including amplifications, fusions, rearrangements, and mutations can result in the downstream activation of tyrosine kinases, leading to tumor development. Targeting these FGFR alterations has shown to be effective in treating cholangiocarcinoma, urothelial carcinoma, and myeloid/lymphoid neoplasms, and there are currently four FGFR inhibitors approved by the Food and Drug Administration (FDA). There have been developments in multiple agents targeting the FGFR pathway, including selective FGFR inhibitors, ligand traps, monoclonal antibodies, and antibody–drug conjugates. However, most of these agents have variable and low responses, with some intolerable toxicities and acquired resistances. This review will summarize previous clinical experiences and current developments in agents targeting the FGFR pathway, and will also discuss future directions for FGFR-targeting agents. [ABSTRACT FROM AUTHOR]

Published

2024

32. Integrated single-cell multiomics uncovers foundational regulatory mechanisms of lens development and pathology.

Author

Tangeman, Jared A., Rebull, Sofia M., Grajales-Esquivel, Erika, Weaver, Jacob M., Bendezu-Sayas, Stacy, Robinson, Michael L., Lachke, Salil A., and Del Rio-Tsonis, Katia

Subjects

*MULTIOMICS, *CELL determination, *CELL differentiation, *EPITHELIAL cells, *TRANSCRIPTION factors

Abstract

Ocular lens development entails epithelial to fiber cell differentiation, defects in which cause congenital cataracts. We report the first singlecell multiomic atlas of lens development, leveraging snRNA-seq, snATAC-seq and CUT&RUN-seq to discover previously unreported mechanisms of cell fate determination and cataract-linked regulatory networks. A comprehensive profile of cis- and trans-regulatory interactions, including for the cataract-linked transcription factor MAF, is established across a temporal trajectory of fiber cell differentiation. Furthermore, we identify an epigenetic paradigm of cellular differentiation, defined by progressive loss of the H3K27 methylation writer Polycomb repressive complex 2 (PRC2). PRC2 localizes to heterochromatin domains across master-regulator transcription factor gene bodies, suggesting it safeguards epithelial cell fate. Moreover, we demonstrate that FGF hyper-stimulation in vivo leads to MAF network activation and the emergence of novel lens cell states. Collectively, these data depict a comprehensive portrait of lens fiber cell differentiation, while defining regulatory effectors of cell identity and cataract formation. [ABSTRACT FROM AUTHOR]

Published

2024

33. Diverse contribution of amniogenic somatopleural cells to cardiovascular development: With special reference to thyroid vasculature.

Author

Haneda, Yuka, Miyagawa‐Tomita, Sachiko, Uchijima, Yasunobu, Iwase, Akiyasu, Asai, Rieko, Kohro, Takahide, Wada, Youichiro, and Kurihara, Hiroki

Subjects

CARDIOVASCULAR development, VASCULAR endothelial cells, VASCULAR endothelial growth factors, FIBROBLAST growth factors, CARDIOVASCULAR system

Abstract

Background: The somatopleure serves as the primordium of the amnion, an extraembryonic membrane surrounding the embryo. Recently, we have reported that amniogenic somatopleural cells (ASCs) not only form the amnion but also migrate into the embryo and differentiate into cardiomyocytes and vascular endothelial cells. However, detailed differentiation processes and final distributions of these intra‐embryonic ASCs (hereafter referred to as iASCs) remain largely unknown. Results: By quail‐chick chimera analysis, we here show that iASCs differentiate into various cell types including cardiomyocytes, smooth muscle cells, cardiac interstitial cells, and vascular endothelial cells. In the pharyngeal region, they distribute selectively into the thyroid gland and differentiate into vascular endothelial cells to form intra‐thyroid vasculature. Explant culture experiments indicated sequential requirement of fibroblast growth factor (FGF) and vascular endothelial growth factor (VEGF) signaling for endothelial differentiation of iASCs. Single‐cell transcriptome analysis further revealed heterogeneity and the presence of hemangioblast‐like cell population within ASCs, with a switch from FGF to VEGF receptor gene expression. Conclusion: The present study demonstrates novel roles of ASCss especially in heart and thyroid development. It will provide a novel clue for understanding the cardiovascular development of amniotes from embryological and evolutionary perspectives. Key Findings: Here, we show that amniogenic somatopleure cells (ASCs) differentiate into various cell types constituting the cardiovascular system, with some populations having a molecular background similar to that of hemangioblasts. Among them, those contributing to the thyroid vascular network were suggested to differentiate into vascular endothelial cells with FGF‐specification and VEGF‐induced maturation. This study will provide a novel clue for understanding the cardiovascular development of amniotes from embryological and evolutionary perspectives. [ABSTRACT FROM AUTHOR]

Published

2024

34. Fibroblast growth factor signaling in axons: from development to disease

Author

Diogo Tomé, Marta S. Dias, Joana Correia, and Ramiro D. Almeida

Subjects

FGF, Signaling pathways, Axons, Presynaptic terminal, Axonal injury, Neuronal disorders, Medicine, Cytology, QH573-671

Abstract

Abstract The fibroblast growth factor (FGF) family regulates various and important aspects of nervous system development, ranging from the well-established roles in neuronal patterning to more recent and exciting functions in axonal growth and synaptogenesis. In addition, FGFs play a critical role in axonal regeneration, particularly after spinal cord injury, confirming their versatile nature in the nervous system. Due to their widespread involvement in neural development, the FGF system also underlies several human neurological disorders. While particular attention has been given to FGFs in a whole-cell context, their effects at the axonal level are in most cases undervalued. Here we discuss the endeavor of the FGF system in axons, we delve into this neuronal subcompartment to provide an original view of this multipurpose family of growth factors in nervous system (dys)function. Video Abstract

Published

2023

35. The Promises of Pancreatic Progenitor Proliferation and Differentiation

Author

Kimura, Azuma, Osafune, Kenji, Piemonti, Lorenzo, editor, Odorico, Jon, editor, Kieffer, Timothy J ., editor, Sordi, Valeria, editor, and de Koning, Eelco, editor

Published

2023

36. Signaling Pathways Regulating Cartilage Formation

Author

Ramzan, Faiza, Salim, Asmat, Khan, Irfan, Baghaban Eslaminejad, Mohamadreza, editor, and Hosseini, Samaneh, editor

Published

2023

37. Specification and Plasticity of Mammalian Cochlear Hair Cell Progenitors

Author

McGovern, Melissa M., Groves, Andrew K., Coffin, Allison B., Series Editor, Sisneros, Joseph, Series Editor, Avraham, Karen, Editorial Board Member, Popper, Arthur N., Founding Editor, Bass, Andrew, Editorial Board Member, Fay, Richard R., Founding Editor, Cunningham, Lisa, Editorial Board Member, Fritzsch, Bernd, Editorial Board Member, Groves, Andrew, Editorial Board Member, Hertzano, Ronna, Editorial Board Member, Le Prell, Colleen, Editorial Board Member, Litovsky, Ruth, Editorial Board Member, Manis, Paul, Editorial Board Member, Manley, Geoffrey, Editorial Board Member, Moore, Brian, Editorial Board Member, Simmons, Andrea, Editorial Board Member, Yost, William, Editorial Board Member, Warchol, Mark E., editor, and Stone, Jennifer S., editor

Published

2023

38. Muscle-tendon cross talk during muscle wasting

Author

Avey, Alec M and Baar, Keith

Subjects

Regenerative Medicine, Aging, Biotechnology, Underpinning research, 1.1 Normal biological development and functioning, Aetiology, 2.1 Biological and endogenous factors, Musculoskeletal, Animals, Biomechanical Phenomena, Exosomes, Fibroblast Growth Factors, Gene Expression Regulation, Humans, MicroRNAs, Muscle Cells, Muscle, Skeletal, Muscular Atrophy, Myostatin, Osteonectin, Signal Transduction, Tendons, cachexia, FGF, myostatin, sarcopenia, SPARC, Biochemistry and Cell Biology, Physiology, Medical Physiology

Abstract

In organisms from flies to mammals, the initial formation of a functional tendon is completely dependent on chemical signals from muscles (myokines). However, how myokines affect the maturation, maintenance, and regeneration of tendons as a function of age is completely unstudied. Here we discuss the role of four myokines-fibroblast growth factors (FGF), myostatin, the secreted protein acidic and rich in cysteine (SPARC) miR-29-in tendon development and hypothesize a role for these factors in the progressive changes in tendon structure and function as a result of muscle wasting (disuse, aging, and disease). Because of the close relationship between mechanical loading and muscle and tendon regulation, disentangling muscle-tendon cross talk from simple mechanical loading is experimentally quite difficult. Therefore, we propose an experimental framework that hopefully will be useful in demonstrating muscle-tendon cross talk in vivo. Though understudied, the promise of a better understanding of muscle-tendon cross talk is the development of new interventions that will improve tendon development, regeneration, and function throughout the lifespan.

Published

2021

39. Comparison between compression tested and simulated Mg-6.3Gd bone scaffolds produced by binder based additive manufacturing technique

Author

Martin Wolff, Mohammad Marvi-Mashhadi, Eshwara Nidadavolu, Henrik Lüneburg, Thomas Ebel, and Regine Willumeit-Römer

Subjects

Magnesium, Mg-6.3Gd, Additive manufacturing, Simulation, FGF, Biodegradable, Mining engineering. Metallurgy, TN1-997

Abstract

In this study, a binder based 3D-printing technology viz. Fused Granular Fabrication (FGF) technique was used to produce interconnected and open porous Mg-6.3Gd bone scaffolds for compression test analyses. The consolidation of the green parts (as printed scaffolds) was performed using solvent debinding in cyclohexane and subsequent conventional sintering in argon atmosphere. Compression tests were performed on as sintered parts. Additionally, a simulation strategy was developed for modeling the compression behavior of the sintered parts, utilizing the data from the experimental results. The experimental compression test results and the simulation strategy for the compression behavior of the 3D-printed scaffolds demonstrated good agreement.

Published

2023

40. Fgf22 and Fgfr2b are required for neurogenesis and gliogenesis in the zebrafish forebrain.

Author

Miyake, Ayumi, Ohmori, Takatoshi, and Murakawa, Yuka

Subjects

*PROSENCEPHALON, *FIBROBLAST growth factors, *OLIGODENDROGLIA, *BRACHYDANIO, *GABAERGIC neurons, *NEUROGENESIS, *DEVELOPMENTAL neurobiology

Abstract

Fibroblast growth factors (Fgfs) play crucial roles in various developmental processes including brain development. We previously identified Fgf22 in zebrafish and found that fgf22 is involved in midbrain patterning during embryogenesis. Here, we investigated the role of Fgf22 in the formation of the zebrafish forebrain. We found that fgf22 was essential for determining the ventral properties of the telencephalon and diencephalon but not for cell proliferation. In addition, the knockdown of fgf22 inhibited the generation of glutamatergic neurons, γ–aminobutyric acid (GABA)ergic interneurons and astrocytes. Recently, Fgf signaling has received much attention because of its importance in the pathogenesis of multiple sclerosis, in which oligodendrocytes and myelin are destroyed. However, the effects of each Fgf on oligodendrocytes remain largely unknown. Therefore, we also investigated the role of Fgf22 in oligodendrocyte development and explored whether there is a difference between Fgf22 and other Fgfs. Knockdown of fgf22 promoted the generation of oligodendrocytes. Conversely, overexpression of fgf22 inhibited the generation of oligodendrocytes. Furthermore, the forebrain phenotypes of fgfr2b knockdown zebrafish were remarkably similar to those of fgf22 knockdown zebrafish. This establishes the Fgf22-Fgfr2b axis as a key ligand‒receptor partnership in neurogenesis and gliogenesis in the forebrain. Our results indicate that Fgf22 has a unique function in suppressing oligodendrocyte differentiation through Fgfr2b without affecting cell proliferation. • In the forebrain, Fgf22 had no effect on cell proliferation. • Fgf22 is involved in the development of glutamatergic and GABAergic neurons. • Fgf22 has a unique function in suppressing oligodendrocyte (OL) differentiation. • The Fgf22-Fgfr2b partnership is important for the inhibition of OL differentiation. [ABSTRACT FROM AUTHOR]

Published

2023

41. Fibroblast growth factor signaling in axons: from development to disease.

Author

Tomé, Diogo, Dias, Marta S., Correia, Joana, and Almeida, Ramiro D.

Subjects

*FIBROBLAST growth factors, *AXONS, *NERVOUS system, *NEUROLOGICAL disorders, *SPINAL cord injuries, *GROWTH factors

Abstract

The fibroblast growth factor (FGF) family regulates various and important aspects of nervous system development, ranging from the well-established roles in neuronal patterning to more recent and exciting functions in axonal growth and synaptogenesis. In addition, FGFs play a critical role in axonal regeneration, particularly after spinal cord injury, confirming their versatile nature in the nervous system. Due to their widespread involvement in neural development, the FGF system also underlies several human neurological disorders. While particular attention has been given to FGFs in a whole-cell context, their effects at the axonal level are in most cases undervalued. Here we discuss the endeavor of the FGF system in axons, we delve into this neuronal subcompartment to provide an original view of this multipurpose family of growth factors in nervous system (dys)function. AweD8hz_Jb9Xnmt7MCVsuU Video Abstract [ABSTRACT FROM AUTHOR]

Published

2023

42. Transformation of Pluripotency States during Morphogenesis of Mouse and Human Epiblast.

Author

Abdyev, V. K., Alpeeva, E. V., Kalistratova, E. N., Vorotelyak, E. A., and Vasiliev, A. V.

Subjects

*EPIBLAST, *GASTRULATION, *GERM cell differentiation, *MORPHOGENESIS, *PLURIPOTENT stem cells, *CELL transformation

Abstract

The pluripotent status of a cell in vivo is spatio-temporally regulated within embryogenesis and is determined by the processes of self-renewal, endless proliferation, and differentiation into all cell types of the body. Initially, the concept of pluripotency status was proposed for characterization of teratocarcinoma cells, and then this concept was applied to the embryonic cells of the preimplantation mouse embryo. Mouse and human pluripotent stem cells (PSCs) are formed during the preimplantation period and are present in the embryo until the beginning of gastrulation. The differentiation of the inner cell mass of the blastocyst (ICM) into a hypoblast and an epiblast, which develops into the embryo itself, is one of the main events in early mammalian development. Continuous and dynamic transformation of pluripotency states in development coincides with the morphogenetic processes that are involved in the formation and maturation of the epiblast. Thus, blastocyst ICM cells differ in epigenetic and transcription patterns from their daughter cells forming the peri/postimplantation epiblast. With the onset of gastrulation movements, the maturation of epiblast cells ends with their differentiation into cells of three germ layers. This review considers the historical aspects of the study of cell pluripotency, various sources of PSCs, and mechanisms and signaling pathways that support self-renewal and pluripotency in PSCs cultures. In addition, the authors summarize and conceptualize data on morphogenetic processes that are involved in the formation of naive ICM cells in vivo and the subsequent maturation of mouse and human epiblast cells associated with the transformation of their pluripotency states. [ABSTRACT FROM AUTHOR]

Published

2023

43. Glare countering and exploiting via dual stream network for nighttime vehicle detection

Author

Du, Pengshu, Wang, Xiao, Zheng, Qi, Wang, Xi, Li, WeiGang, and Xu, Xin

Published

2024

44. Galectins use N-glycans of FGFs to capture growth factors at the cell surface and fine-tune their signaling

Author

Aleksandra Gedaj, Dominika Zukowska, Natalia Porebska, Marta Pozniak, Mateusz Krzyscik, Aleksandra Czyrek, Daniel Krowarsch, Malgorzata Zakrzewska, Jacek Otlewski, and Lukasz Opalinski

Subjects

FGF, Galectins, N-glycosylation, Multivalency, Signaling, Extracellular matrix, Medicine, Cytology, QH573-671

Abstract

Abstract Fibroblast growth factors (FGFs) and their receptors (FGFRs) constitute complex signaling hubs that are crucial for the development and homeostasis of the human body. Most of FGFs are released by cells using the conventional secretory pathway and are N-glycosylated, yet the role of FGFs glycosylation is largely unknown. Here, we identify N-glycans of FGFs as binding sites for a specific set of extracellular lectins, galectins − 1, -3, -7 and − 8. We demonstrate that galectins attract N-glycosylated FGF4 to the cell surface, forming a reservoir of the growth factor in the extracellular matrix. Furthermore, we show that distinct galectins differentially modulate FGF4 signaling and FGF4-dependent cellular processes. Using engineered variants of galectins with altered valency we demonstrate that multivalency of galectins is critical for the adjustment of FGF4 activity. Summarizing, our data reveal a novel regulatory module within FGF signaling, in which the glyco-code in FGFs provides previously unanticipated information differentially deciphered by multivalent galectins, affecting signal transduction and cell physiology. Video Abstract

Published

2023

45. FGF-trapping hampers cancer stem-like cells in uveal melanoma

Author

Alessandra Loda, Stefano Calza, Arianna Giacomini, Cosetta Ravelli, Adwaid Manu Krishna Chandran, Chiara Tobia, Giovanna Tabellini, Silvia Parolini, Francesco Semeraro, Roberto Ronca, and Sara Rezzola

Subjects

Uveal melanoma, Cancer stem-like cells, FGF, FGF inhibitor, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282, Cytology, QH573-671

Abstract

Abstract Background Cancer stem-like cells (CSCs) are a subpopulation of tumor cells responsible for tumor initiation, metastasis, chemoresistance, and relapse. Recently, CSCs have been identified in Uveal Melanoma (UM), which represents the most common primary tumor of the eye. UM is highly resistant to systemic chemotherapy and effective therapies aimed at improving overall survival of patients are eagerly required. Methods Herein, taking advantage from a pan Fibroblast Growth Factor (FGF)-trap molecule, we singled out and analyzed a UM-CSC subset with marked stem-like properties. A hierarchical clustering of gene expression data publicly available on The Cancer Genome Atlas (TCGA) was performed to identify patients’ clusters. Results By disrupting the FGF/FGF receptor (FGFR)-mediated signaling, we unmasked an FGF-sensitive UM population characterized by increased expression of numerous stemness-related transcription factors, enhanced aldehyde dehydrogenase (ALDH) activity, and tumor-sphere formation capacity. Moreover, FGF inhibition deeply affected UM-CSC survival in vivo in a chorioallantoic membrane (CAM) tumor graft assay, resulting in the reduction of tumor growth. At clinical level, hierarchical clustering of TCGA gene expression data revealed a strong correlation between FGFs/FGFRs and stemness-related genes, allowing the identification of three distinct clusters characterized by different clinical outcomes. Conclusions Our findings support the evidence that the FGF/FGFR axis represents a master regulator of cancer stemness in primary UM tumors and point to anti-FGF treatments as a novel therapeutic strategy to hit the CSC component in UM.

Published

2023

46. Subcellular hot spots of GPCR signaling promote vascular inflammation

Author

Birch, Cierra A, Molinar-Inglis, Olivia, and Trejo, JoAnn

Subjects

Medical Biochemistry and Metabolomics, Biomedical and Clinical Sciences, Clinical Sciences, 2.1 Biological and endogenous factors, Arrestins, B-cell lymphoma protein 10, COVID-19, Endosomes, Endothelial, G protein-coupled receptor, GPCR, JAK-STAT, Janus kinase, JAK, MALT1, NFκB, adherens junctions, AJ, angiotensin II type 1 receptor, AT1, angiotensin converting enzyme-2, ACE2, caspase recruitment domain-containing protein, CARMA, coronavirus disease of 2019, COVID-19, fibroblast-growth-factor, FGF, inhibitor of NFκB kinase, IKK, mitogen-activated protein kinase, MAPK, mucosa-associated lymphoid tissue lymphoma translocation protein 1, neural precursor cell expressed developmentally downregulated protein 4, NEDD4, nuclear factor kappa-light-chain-enhancer of activated B cells, NFκB, p38 MAPK, platelet activating factor, PAF, protease-activated receptor-1, PAR1, severe acute respiratory syndrome coronavirus 2, SARS-CoV-2, signal transducer and activator of transcription, STAT, transforming growth factor-α-activated kinase binding protein-1, TAB1, Clinical sciences, Medical biochemistry and metabolomics

Abstract

G-coupled protein receptors (GPCRs) comprise the largest class of druggable targets. Signaling by GPCRs is initiated from subcellular hot spots including the plasma membrane, signalosomes, and endosomes to contribute to vascular inflammation. GPCR-G protein signaling at the plasma membrane causes endothelial barrier disruption and also cross-talks with growth factor receptors to promote proinflammatory signaling. A second surge of GPCR signaling is initiated by cytoplasmic NFκB activation mediated by β-arrestins and CARMA-BCL10-MALT1 signalosomes. Once internalized, ubiquitinated GPCRs initiate signaling from endosomes via assembly of the transforming growth factor-β-activated kinase binding protein-1 (TAB1)-TAB2-p38 MAPK complex to promote vascular inflammation. Understanding the complexities of GPCR signaling is critical for development of new strategies to treat vascular inflammation such as that associated with COVID-19.

Published

2021

47. FGFR signalling in human cervical cancer cell lines

Author

Mahmood, Hibe-Tun-Noor Afshan, Chioni, Athina-Myrto, Walker, Tony, Polycarpou, Elena, and Grose, Richard

Subjects

cervical cancer, FGF, FGFR, FGFR signalling, HPV, drug resistance

Abstract

Fibroblast Growth Factors (FGFs) play a vital role in development and tissue regeneration. There are at least 23 distinct members of the FGF family that bind to at least four tyrosine kinase receptors known as FGF Receptors (FGFRs). FGF/FGFR signalling plays an important role in variety of processes and is tightly regulated. However, some cancer cells hijack the control of FGFR pathway, causing deregulation of FGFR signalling. FGF and their receptors, such as FGFR1 and 2, have been involved in susceptibility of breast cancer and progression as well as in a number of other cancers. Cervical cancer (CC) is one of the most commonly diagnosed cancers in women worldwide. One of the main causative agents of CC is the human papillomavirus (HPV). However, not all females infected with HPV develop CC demonstrating that other factors might be important. Although some studies have emphasised the possible involvement of FGFR signalling in CC, the aetiology and the molecular mechanisms related to CC and FGFR signalling remain poorly understood. The main aim of this study was to investigate FGFR signalling in cervical cancer cell lines (HeLa, SiHa and CaSki cell lines; CCCLs). A detailed understanding of the mechanism correlated to CC will make possible to use specific FGFR inhibitors that are currently in clinical trial, for CC treatment either on its own or in conjunction with the existing treatment, in order to increase success rates. In addition, FGFR signalling could be of early prognostic value. In order to examine gene and protein expression of FGFRs and associated ligands in CCCLs, PCR and immunocytochemistry were performed. Downstream extracellular signal-regulated protein kinase (ERK) signalling in CCCLs was investigated using Western blotting. Functional FGFR studies carried out through cell proliferation, migration and apoptosis assays. The above experiments were performed using stimulated and unstimulated CC cells in the presence and absence of FGFR inhibitors PD173074 and SU5402. RNAi mediated FGFR1 and FGFR2 knockdown was also performed to further assess function. The human CCCLs expressed FGFR1, FGFR2, FGFR4, FGF2, FGF4 and FGF7 mRNA and protein, with 'b' and 'c' isoforms of FGFR1 and FGFR2 confirmed using gene expression analysis. The FGFR1 and FGFR2 protein in CCCLs was localised within the nucleus with a distinct speckled arrangement. Importantly, ELISA revealed that all CCCLs secreted FGF2 ligand only, but not FGF4 and FGF7 suggesting that FGFR was activated in a paracrine manner. Activation of the ERK pathway occurred in response to FGF2, 4 and 7 exposures in all three CCCLs and the activation was eradicated in the presence of PD173074 or SU5402 inhibitor, suggesting that the effect is specific to FGFR signalling. Functional studies revealed that FGFR signalling enhanced cell proliferation and migration. Furthermore, knockdown of FGFR1 and FGFR2 by RNA interference or blockade using PD173074 inhibited cell proliferation, cell migration and also promoted the apoptosis CC cells. Drug resistant CCCLs (HeLa, CaSki and SiHa) were established following long-term exposure to PD17307. Collectively, this work supports an association between CC progression and FGFR signalling, laying the foundations for developing FGFR inhibitors for CC therapy. The drug resistant CCCLs will be valuable for further investigations into the mechanisms involved in acquired drug resistance.

Published

2020

48. Programmed ageing: decline of stem cell renewal, immunosenescence, and Alzheimer's disease.

Author

Lathe, Richard and St. Clair, David

Subjects

*IMMUNOSENESCENCE, *ALZHEIMER'S disease, *CELL proliferation, *SOMATOMEDIN, *STEM cells, *FIBROBLAST growth factors

Abstract

The characteristic maximum lifespan varies enormously across animal species from a few hours to hundreds of years. This argues that maximum lifespan, and the ageing process that itself dictates lifespan, are to a large extent genetically determined. Although controversial, this is supported by firm evidence that semelparous species display evolutionarily programmed ageing in response to reproductive and environmental cues. Parabiosis experiments reveal that ageing is orchestrated systemically through the circulation, accompanied by programmed changes in hormone levels across a lifetime. This implies that, like the circadian and circannual clocks, there is a master 'clock of age' (circavital clock) located in the limbic brain of mammals that modulates systemic changes in growth factor and hormone secretion over the lifespan, as well as systemic alterations in gene expression as revealed by genomic methylation analysis. Studies on accelerated ageing in mice, as well as human longevity genes, converge on evolutionarily conserved fibroblast growth factors (FGFs) and their receptors, including KLOTHO, as well as insulin‐like growth factors (IGFs) and steroid hormones, as key players mediating the systemic effects of ageing. Age‐related changes in these and multiple other factors are inferred to cause a progressive decline in tissue maintenance through failure of stem cell replenishment. This most severely affects the immune system, which requires constant renewal from bone marrow stem cells. Age‐related immune decline increases risk of infection whereas lifespan can be extended in germfree animals. This and other evidence suggests that infection is the major cause of death in higher organisms. Immune decline is also associated with age‐related diseases. Taking the example of Alzheimer's disease (AD), we assess the evidence that AD is caused by immunosenescence and infection. The signature protein of AD brain, Aβ, is now known to be an antimicrobial peptide, and Aβ deposits in AD brain may be a response to infection rather than a cause of disease. Because some cognitively normal elderly individuals show extensive neuropathology, we argue that the location of the pathology is crucial – specifically, lesions to limbic brain are likely to accentuate immunosenescence, and could thus underlie a vicious cycle of accelerated immune decline and microbial proliferation that culminates in AD. This general model may extend to other age‐related diseases, and we propose a general paradigm of organismal senescence in which declining stem cell proliferation leads to programmed immunosenescence and mortality. [ABSTRACT FROM AUTHOR]

Published

2023

49. Comparison between compression tested and simulated Mg-6.3Gd bone scaffolds produced by binder based additive manufacturing technique.

Author

Wolff, Martin, Marvi-Mashhadi, Mohammad, Nidadavolu, Eshwara, Lüneburg, Henrik, Ebel, Thomas, and Willumeit-Römer, Regine

Subjects

POLYCAPROLACTONE, CYCLOHEXANE, ARGON, POROSITY

Abstract

• Worldwide 1st time binder based 3D-printed (FGF) biodegradable Mg-based (MgGd-alloy) bone scaffolds. • Obtaining an as printed interconnected open porosity for cell ingrownth and vascularisation. • Mechanical behavior of experimental test and simulation shows good agreement. In this study, a binder based 3D-printing technology viz. Fused Granular Fabrication (FGF) technique was used to produce interconnected and open porous Mg-6.3Gd bone scaffolds for compression test analyses. The consolidation of the green parts (as printed scaffolds) was performed using solvent debinding in cyclohexane and subsequent conventional sintering in argon atmosphere. Compression tests were performed on as sintered parts. Additionally, a simulation strategy was developed for modeling the compression behavior of the sintered parts, utilizing the data from the experimental results. The experimental compression test results and the simulation strategy for the compression behavior of the 3D-printed scaffolds demonstrated good agreement. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2023

50. Devo-Aging: Intersections Between Development and Aging.

Author

Silva-García, Carlos Giovanni

Subjects

DEVELOPMENTAL biology, AGING, EMBRYOLOGY, CELLULAR signal transduction, AGE factors in disease, CONTINUITY

Abstract

There are two fundamental questions in developmental biology. How does a single fertilized cell give rise to a whole body? and how does this body later produce progeny? Synchronization of these embryonic and postembryonic developments ensures continuity of life from one generation to the next. An enormous amount of work has been done to unravel the molecular mechanisms behind these processes, but more recently, modern developmental biology has been expanded to study development in wider contexts, including regeneration, environment, disease, and even aging. However, we have just started to understand how the mechanisms that govern development also regulate aging. This review discusses examples of signaling pathways involved in development to elucidate how their regulation influences healthspan and lifespan. Therefore, a better knowledge of developmental signaling pathways stresses the possibility of using them as innovative biomarkers and targets for aging and age-related diseases. [ABSTRACT FROM AUTHOR]

Published

2023