Activation of Astrocytes &amp;lt;i&amp;gt;in Vitro&amp;lt;/i&amp;gt; by Macrophages Polarized with Keratin Biomaterial Treatment

Fearing, Bailey V.; Dyke, Mark Van

doi:10.4236/ojrm.2016.51001

Cited by 6 publications

(5 citation statements)

References 42 publications

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“…As SL decreased macrophage nitric oxide production in a sepsis model, we hypothesized that SLBEDA would shift M1 macrophages to an anti-inflammatory phenotype. Additionally, due to the crosstalk between macrophages and astrocytes, − we hypothesized that astrocytes would shift to a less reactive phenotype. We studied peritoneal macrophage (PMAC) and spinal cord astrocyte viability as well as PMAC polarization and astrocytic GFAP expression in response to varying concentrations of SLBEDA in vitro.…”

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confidence: 99%

Sophorolipid Butyl Ester Diacetate Does Not Affect Macrophage Polarization but Enhances Astrocytic Glial Fibrillary Acidic Protein Expression at Micromolar Concentrations in Vitro

Ziemba¹,

Gottipati

Totsingan³

et al. 2017

ACS Chem. Neurosci.

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Peritoneal macrophages (PMACs) and spinal cord astrocytes were exposed to varying concentrations of soluble sophorolipid butyl ester diacetate (SLBEDA) in vitro. Macrophages and astrocytes demonstrated no decrease in viability in response to SLBEDA. Studying pro-and antiinflammatory genes, PMACs did not show a shift toward a pro-inflammatory phenotype. However, at higher concentrations (3 and 30 μM), astrocytes showed an increase in their expression of glial acidic fibrillary protein. This novel category of compounds poses low risk to PMAC and astrocyte viability; however, the effect on PMAC polarization and astrocyte reactivity requires more elucidation. Graphical abstract Supporting InformationThe Supporting Information is available free of charge on the ACS Publications website at DOI: 10.1021/acschemneuro.6b00451. Additional methods and results for SLBEDA synthesis and characterization and plasticity of PMAC polarization test (PDF) Notes Any opinions, findings, and conclusions or recommendations expressed in this material are those of the author(s) and do not necessarily reflect the views of the National Science Foundation. The authors declare no competing financial interest. (SCI). 1 The mechanical insult accompanying injury produces hemorrhaging, ischemia, and edema that result in an expanding lesion. 2 After approximately 2 h, the injury progresses to a secondary injury phase characterized by inflammation. Neutrophils first infiltrate the injury site followed by the activation of microglia and the recruitment of blood monocytes that differentiate and respond to the environment by polarizing to a pro-inflammatory or an antiinflammatory phenotype. M1, pro-inflammatory, macrophages are prevalent during the first several days postinjury 3 but persist weeks postinjury. 2,4 These macrophages produce high levels of reactive oxygen species (ROS) and pro-inflammatory cytokines. 3 Ultimately, this M1 macrophage pro-inflammation is neurotoxic and results in axonal dieback 3,4 and causes neuronal and glial necrosis. 5 In addition to macrophages, astrocytes also play an important role post-SCI. Astrocytes are a heterogeneous population of glial cells present in the central nervous system (CNS) and are primarily responsible for the overall maintenance of homeostasis in the CNS. 6 Following SCI, astrocytes at and around the site of the injury are activated, leading to the formation of a glial scar which acts as a chemical and physical barrier to regenerating axons. 7 The activation/reactivity of astrocytes is characterized by an increase in migration/proliferation 8,9 along with an increase in the production of the intermediate filament glial fibrillary acidic protein (GFAP) 10 and extracellular chondroitin sulfate proteoglycans (CSPGs). 11 GFAP synthesis is a meaningful aspect of the developmental plan of astrocyte differentiation, and it is a part of the reactive response to several CNS injuries. 12 After the injury, astrocytes show a decrease in GFAP until 1 day postinjury (dpi) followed by a steady increas...

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confidence: 99%

Sophorolipid Butyl Ester Diacetate Does Not Affect Macrophage Polarization but Enhances Astrocytic Glial Fibrillary Acidic Protein Expression at Micromolar Concentrations in Vitro

Ziemba¹,

Gottipati

Totsingan³

et al. 2017

ACS Chem. Neurosci.

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“…However, in the case of macrophages, keratose coatings can promote monocyte differentiation toward anti-inflammatory "M2-type" macrophages over pro-inflammatory "M1-type" macrophages. 142 This is in contrast to collagen coatings, which promote equal monocyte differentiation into both M2 and M1 macrophages.…”

Section: ■ Hair Follicles As a Source Of Biomaterials For Regenerativ...mentioning

confidence: 97%

“…Inflammatory cytokines released by ‘M1-type’ macrophages can lead to excessive CSPG production by reactive astrocytes, hampering effective recovery. In an in vitro model for astrogliosis, media from monocytes grown on keratin films inhibited the process of astrogliosis 142. Thus, it opens up the possibility of controlling glial scarring by targeting and enhancing M2 macrophages, rather than astrocytes.…”

Section: Hair Follicles As a Source Of Biomaterials For Regenerative mentioning

confidence: 99%

“…In an in vitro model for astrogliosis, media from monocytes grown on keratin films inhibited the process of astrogliosis. 142 This opens up the possibility of controlling glial scarring by targeting and enhancing M2 macrophages rather than astrocytes. The idea of exploiting biased induction of differentiation is not new, and other studies have used biomaterials to create pro-regenerative microenvironments by biasing the recruitment of alternatively activated macrophages.…”

Section: ■ Hair Follicles As a Source Of Biomaterials For Regenerativ...mentioning

confidence: 99%

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The Hair Follicle: An Underutilized Source of Cells and Materials for Regenerative Medicine

Kiani

Almquist

2017

ACS Biomater. Sci. Eng.

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The hair follicle is one of only two structures within the adult body that selectively degenerates and regenerates, making it an intriguing organ to study and use for regenerative medicine. Hair follicles have been shown to influence wound healing, angiogenesis and neurogenesis, and harbor distinct populations of stem cells; this has led to cells from the follicle being used in clinical trials for tendinosis and chronic ulcers. In addition, keratin produced by the follicle in the form of a hair fiber provides an abundant source of biomaterials for regenerative medicine. In this review, we provide an overview of the structure of a hair follicle, explain the role of the follicle in regulating the microenvironment of skin and the impact on wound healing, explore individual cell types of interest for regenerative medicine, and cover several applications of keratin-based biomaterials.

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“…Fibroblasts serve as a connective tissue cell model and attach to the ECM, a non-cellular structure that contains fibrous proteins [79]. Focal adhesions create transmembrane communication channels that can activate cell proliferation [80,81], phenotypic changes [82,83], and cell signaling cascades [84]. Actin fibers are an indication of focal adhesion formation [81].…”

Section: Cellular Adhesion Immunochemistrymentioning

confidence: 99%

A comparative study of materials assembled from recombinant K31 and K81 and extracted human hair keratins

et al. 2020

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Natural biopolymers have found success in tissue engineering and regenerative medicine applications. Their intrinsic biocompatibility and biological activity make them well suited for biomaterials development. Specifically, keratin-based biomaterials have demonstrated utility in regenerative medicine applications including bone regeneration, wound healing, and nerve regeneration. However, studies of structure-function relationships in keratin biomaterials have been hindered by the lack of homogeneous preparations of materials extracted and isolated from natural sources such as wool and hair fibers. Here we present a side-by-side comparison of natural and recombinant human hair keratin proteins K31 and K81. When combined, the recombinant proteins (i.e. rhK31 and rhK81) assemble into characteristic intermediate filament-like fibers. Coatings made from natural and recombinant dimers were compared side-by-side and investigated for coating characteristics and cell adhesion. In comparison to control substrates, the recombinant keratin materials show a higher propensity for inducing involucrin and hence, maturation in terms of potential skin cell differentiation.

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Activation of Astrocytes <i>in Vitro</i> by Macrophages Polarized with Keratin Biomaterial Treatment

Cited by 6 publications

References 42 publications

Sophorolipid Butyl Ester Diacetate Does Not Affect Macrophage Polarization but Enhances Astrocytic Glial Fibrillary Acidic Protein Expression at Micromolar Concentrations in Vitro

Sophorolipid Butyl Ester Diacetate Does Not Affect Macrophage Polarization but Enhances Astrocytic Glial Fibrillary Acidic Protein Expression at Micromolar Concentrations in Vitro

The Hair Follicle: An Underutilized Source of Cells and Materials for Regenerative Medicine

A comparative study of materials assembled from recombinant K31 and K81 and extracted human hair keratins

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