Nitric Oxide Stimulates Matrix Synthesis and Deposition by Adult Human Aortic Smooth Muscle Cells Within Three-Dimensional Cocultures

Simmers, Phillip; Gishto, Arsela; Vyavahare, Narendra R.; Kothapalli, Chandrasekhar R.

doi:10.1089/ten.tea.2014.0363

Cited by 24 publications

(29 citation statements)

References 81 publications

(93 reference statements)

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“…SDS/PAGE Western blot analysis was done for semi-quantitative detection of GSK-3β, βcatenin, DLL4, and notch-1 protein bands with their respective primary antibodies (Simmers, Gishto, Vyavahare, & Kothapalli, 2015). Similarly, samples for Notch1 pathway study include: control group, aza-treated group, γ-secretase inhibitor treated group, and aza + γ-secretase inhibitor treated group (aza exposure for 24 hr followed by its removal and addition of γ-secretase inhibitor).…”

Section: Western Blot For Protein Expressionmentioning

confidence: 99%

Three‐dimensional collagenous niche and azacytidine selectively promote time‐dependent cardiomyogenesis from human bone marrow‐derived MSC spheroids

Joshi

Mahajan

Kothapalli

2018

Biotech & Bioengineering

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Endogenous adult cardiac regenerative machinery is not capable of replacing the lost cells following myocardial infarction, often leading to permanent alterations in structure-function-mechanical properties. Regenerative therapies based on delivering autologous stem cells within an appropriate 3D milieu could meet such demand, by enabling homing and directed differentiation of the transplanted cells into lost specialized cell populations. Since type I collagen is the predominant cardiac tissue matrix protein, we here optimized the 3D niche which could promote time-dependent evolution of cardiomyogenesis from human bone marrow-derived mesenchymal stem cells (BM-MSC). 3D collagen gel physical and mechanical characteristics were assessed using SEM and AFM, respectively, while the standalone and combined effects of collagen concentration, culture duration, and 5-azacytidine (aza) dose on the phenotype and genotype of MSC spheroids were quantified using immunofluorescence labeling and RT-PCR analysis. Increasing collagen concentration led to a significant increase in Young's modulus (p < 0.01) but simultaneous decrease in the mean pore size, resulting in stiffer gels. Spheroid formation significantly modulated MSC differentiation and genotype, mostly due to better cell-cell interactions. Among the aza dosages tested, 10 μM appears to be optimal, while 3 mg/ml gels resulted in significantly lower cell viability compared to 1 or 2 mg/ml gels. Stiffer gels (2 and 3 mg/ml) and exposure to 10 μM aza upregulated early and late cardiac marker expressions in a time-dependent fashion. On the other hand, cell-cell signaling within the MSC spheroids seem to have a strong role in influencing mature cardiac markers expression, since neither aza nor gel stiffness seem to significantly improve their expression. Western blot analysis suggested that canonical Wnt/β-catenin signaling pathway might be primarily mediating the observed benefits of aza on cardiac differentiation of MSC spheroids. In conclusion, 2 mg/ml collagen and 10 μM aza appears to offer optimal 3D microenvironment in terms of cell viability and time-dependent evolution of cardiomyogenesis from human BM-MSCs, with significant applications in cardiac tissue engineering and stem cell transplantation for regenerating lost cardiac tissue.

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Section: Western Blot For Protein Expressionmentioning

confidence: 99%

Three‐dimensional collagenous niche and azacytidine selectively promote time‐dependent cardiomyogenesis from human bone marrow‐derived MSC spheroids

Joshi

Mahajan

Kothapalli

2018

Biotech & Bioengineering

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“…These approaches have involved biomaterials that utilize both chemical [40–42] and topographical modifications [43, 44] to regulate smooth muscle cells (SMCs) over-proliferation and enhance ECM synthesis as well as other innovative biomaterials that are impregnated with stem cells and/or utilize biomechanical stimulation to improve overall biocompatibility [41, 45]. …”

Section: Discussionmentioning

confidence: 99%

“…In a recent study, a collagen hydrogel construct doped with S-Nitrosoglutathione (GSNO) released exogenous nitric oxide in order to manipulate cell proliferation and matrix deposition by adult human aortic SMCs [40]. Growth factors such as transforming growth factor (TGF-β1) have also been conjugated to fibrin hydrogel vascular grafts and exposed to mechanical stimulation [41] to improve mechanical properties and ECM content.…”

Section: Discussionmentioning

confidence: 99%

An in vivo study of a gold nanocomposite biomaterial for vascular repair

et al. 2015

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Currently vascular repairs are treated using synthetic or biologic patches, however these patches have an array of complications, including calcification, rupture, re-stenosis, and intimal hyperplasia. An active patch material composed of decellulzarized tissue conjugated to gold nanoparticles (AuNPs) was developed and the long term biocompatibility and cellular integration was investigated. Porcine abdominal aortic tissue was decellularized and conjugated with 100nm gold nanoparticles (AuNP). These patches were placed over a longitudinal arteriotomy of the thoracic aorta in six pigs. The animals were monitored for six months. Gross, histological, and immunohistochemical analyses of the patches were performed after euthanasia. Grossly there was minimal scar tissue with the patches still visible on the outer surface of the vessel. The inner lumen was smooth with a seamless transition from patch to native tissue. Histology demonstrated infiltration of host cells into the patch material. The immunohistochemical results demonstrated an endothelial cell layer forming over the patch within the vessel. Smooth muscle cells were repopulating the biomaterial in all animals. These results demonstrated that the AuNP biomaterial patch integrated well with the host tissue and did not failed over the six month implantation time.

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“…LOX activity in the cell matrix and in the pooled media was determined using a sensitive fluorescence-based assay (Amplex® Red Hydrogen Peroxide/Peroxidase assay kit, Molecular Probes) that uses the Amplex Red reagent (10-acetyl-3,7-dihydroxyphenoxazine) to detect H 2 O 2 . This assay is based on the principle that LOX amount is proportional to the released H 2 O 2 because LOX oxidatively deaminates alkyl monoamines and diamines (Palamakumbura & Trackman, 2002;Simmers, Gishto, Vyavahare, & Kothapalli, 2015). Absorbance was read at 560 nm, and a linear standard curve was derived to find H 2 O 2 /LOX in the samples.…”

Section: Lox Functional Activitymentioning

confidence: 99%

Synthesis and secretome release by human bone marrow mesenchymal stem cell spheroids within three‐dimensional collagen hydrogels: Integrating experiments and modelling

Joshi

Abnavi

Kothapalli

2019

J Tissue Eng Regen Med

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Myocardial infarction results in loss of cardiac cell types, inflammation, extracellular matrix (ECM) degradation, and fibrotic scar. Transplantation of bone marrow‐derived mesenchymal stem cells (BM‐MSCs) is being explored as they could differentiate into cardiomyocyte‐like cells, integrate into host tissue, and enhance resident cell activity. The ability of these cells to restore lost ECM, remodel the inflammatory scar tissue, and repair the injured myocardium remains unexplored. We here elucidated the synthesis and deposition of ECM (e.g., elastin, sulfated glycosaminoglycans, hyaluronan, collagen type III, laminin, fibrillin, lysyl oxidase, and nitric oxide synthases), matrix metalloproteinases (MMPs) and their inhibitors (TIMPs), and other secretome (cytokines, chemokines, and growth factors) in adult human BM‐MSC spheroid cultures within three‐dimensional collagen gels. The roles of species‐specific type I collagen and 5‐azacytadine were assessed over a 28‐day period. Results revealed that human collagen (but not rat‐derived) suppressed MSC proliferation and survival, and MSCs synthesized and released a variety of ECM proteins and secretome over the 28 days. Matrix deposition is at least an order of magnitude lower than their release levels at every time point, most possibly due to elevated MMP levels and interleukins with a concomitant decrease in TIMPs. Matrix synthesis over the 28‐day period was fitted to a competitive inhibition form of Michaelis–Menten kinetics, and the production and decay rates of ECM, MMPs, and TIMPs, along with the kinetic model parameters quantified. Such an integrated experimental and modelling approach would help elucidate the critical roles of various parameters (e.g., cell encapsulation and delivery vehicles) in stem cell‐based transplantation therapies.

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Nitric Oxide Stimulates Matrix Synthesis and Deposition by Adult Human Aortic Smooth Muscle Cells Within Three-Dimensional Cocultures

Cited by 24 publications

References 81 publications

Three‐dimensional collagenous niche and azacytidine selectively promote time‐dependent cardiomyogenesis from human bone marrow‐derived MSC spheroids

Three‐dimensional collagenous niche and azacytidine selectively promote time‐dependent cardiomyogenesis from human bone marrow‐derived MSC spheroids

An in vivo study of a gold nanocomposite biomaterial for vascular repair

Synthesis and secretome release by human bone marrow mesenchymal stem cell spheroids within three‐dimensional collagen hydrogels: Integrating experiments and modelling

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