Early Natural History of Neotissue Formation in Tissue-Engineered Vascular Grafts in a Murine Model

Reinhardt, James W.; Ruíz-Rosado, Juan de Dios; Barker, Jenny C.; Lee, Yong‐Ung; Best, Cameron; Yi, Tai; Zeng, Qiang; Partida-Sánchez, Santiago; Shinoka, Toshiharu; Breuer, Christopher K.

doi:10.2217/rme-2018-0133

Cited by 24 publications

(32 citation statements)

References 44 publications

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“…Our prior work characterized proliferating cells within TEVGs and found two predominate populations, F4/80+ (macrophage specific) staining and COL1A1+ staining cells in accordance with classically described foreign body response. [ 4,35 ] Presently, we found that the degree of macrophage infiltration and ratio of PCNA+ cells in the graft at 14 d was independent of both seeding scheme and recipient genotype. This is in contrast to previous work showing TEVGs seeded with BM‐MNCs have decreased macrophage infiltration compared to unseeded TEVGs at 14 d postimplantation.…”

Section: Discussionmentioning

confidence: 74%

“…Both F4/80 and CD68 suffer from off‐target staining of leukocytes other than macrophages in addition to expression intensity differences in TEVGs at different time points. [ 4,36–38 ]…”

Section: Discussionmentioning

confidence: 99%

“…[ 1–3 ] In our murine models with small diameter TEVGs (<1 mm), occlusion occurs due to thrombosis, stenosis, or a dynamic interplay between the two. [ 4 ] Efforts to improve TEVG outcomes include incubation in a bioreactor, scaffold coatings, and cell seeding such as endothelial progenitor cells, fibroblasts, smooth muscle cells, and bone‐marrow derived mononuclear cells (BM‐MNCs). [ 5–10 ] Currently, our group utilizes a cell seeding approach with BM‐MNCs to mediate neotissue formation in situ.…”

Section: Introductionmentioning

confidence: 99%

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Tissue Engineered Vascular Graft Recipient Interleukin 10 Status Is Critical for Preventing Thrombosis

Mirhaidari

Barker

Zbinden

et al. 2020

Adv Healthcare Materials

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Tissue engineered vascular grafts (TEVGs) are a promising technology, but are hindered by occlusion. Seeding with bone‐marrow derived mononuclear cells (BM‐MNCs) mitigates occlusion, yet the precise mechanism remains unclear. Seeded cells disappear quickly and potentially mediate an anti‐inflammatory effect through paracrine signaling. Here, a series of reciprocal genetic TEVG implantations plus recombinant protein treatment is reported to investigate what role interleukin‐10, an anti‐inflammatory cytokine, plays from both host and seeded cells. TEVGs seeded with BM‐MNCs from wild‐type and IL‐10 KO mice, plus unseeded grafts, are implanted into wild‐type and IL‐10 KO mice. Wild‐type mice with unseeded grafts also receive recombinant IL‐10. Serial ultrasound evaluates occlusion and TEVGs are harvested at 14 d for immunohistochemical analysis. TEVGs in IL‐10 KO mice have significantly higher occlusion incidence compared to wild‐type mice attributed to acute (<3 d) thrombosis. Cell seeding rescues TEVGs in IL‐10 KO mice comparable to wild‐type patency. IL‐10 from the host and seeded cells do not significantly influence graft inflammation and macrophage phenotype, yet IL‐10 treatment shows interesting biologic effects including decreasing cell proliferation and increasing M2 macrophage polarization. IL‐10 from the host is critical for preventing TEVG thrombosis and seeded BM‐MNCs exert a significant anti‐thrombotic effect in IL‐10 KO mice.

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Section: Discussionmentioning

confidence: 74%

“…Both F4/80 and CD68 suffer from off‐target staining of leukocytes other than macrophages in addition to expression intensity differences in TEVGs at different time points. [ 4,36–38 ]…”

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Tissue Engineered Vascular Graft Recipient Interleukin 10 Status Is Critical for Preventing Thrombosis

Mirhaidari

Barker

Zbinden

et al. 2020

Adv Healthcare Materials

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“…Previous studies have also observed contractile cells within the neointima of tissue engineered vessels. [43] Statistical regression analysis comparing the implanted scaffold parameters to the explanted neovessel characteristics demonstrated that the PGS coating decreased inflammation and increased collagen accumulation. The lower inflammation and macrophage density seen at explant (12 weeks), in comparison to other polymer-based vascular grafts at similar time, [22,23,44] likely reflected the near complete degradation of polymer by 12 weeks.…”

Section: Discussionmentioning

confidence: 99%

Effects of Braiding Parameters on Tissue Engineered Vascular Graft Development

Zbinden

Blum

Berman

et al. 2020

Adv Healthcare Materials

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Tissue engineered vascular grafts (TEVGs) using scaffolds fabricated from braided poly(glycolic acid) (PGA) fibers coated with poly(glycerol sebacate) (PGS) are developed. The approach relies on in vivo tissue engineering by which neotissue forms solely within the body after a scaffold has been implanted. Herein, the impact of altering scaffold braid design and scaffold coating on neotissue formation is investigated. Several combinations of braiding parameters are manufactured and evaluated in a Beige mouse model in the infrarenal abdominal aorta. Animals are followed with 4D ultrasound analysis, and 12 week explanted vessels are evaluated for biaxial mechanical properties as well as histological composition. Results show that scaffold parameters (i.e., braiding angle, braiding density, and presence of a PGS coating) have interdependent effects on the resulting graft performance, namely, alteration of these parameters influences levels of inflammation, extracellular matrix production, graft dilation, neovessel distensibility, and overall survival. Coupling carefully designed in vivo experimentation with regression analysis, critical relationships between the scaffold design and the resulting neotissue that enable induction of favorable cellular and extracellular composition in a controlled manner are uncovered. Such an approach provides a potential for fabricating scaffolds with a broad range of features and the potential to manufacture optimized TEVGs.

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“…Reinhardt and colleagues developed lyophilized vascular scaffolds from poly (glycolic acid) (PGA) and polycaprolactone-co-lactide (PCLA). Firstly, a solution of these polymers was inserted in a cylinder which was snap-frozen at −20°C for 20 min and then lyophilized for 24 h. The authors obtained highly porous scaffolds with an inner diameter of 0.91 mm and wall thickness of 300 μm ( 71 ). Wang and colleagues developed poly-L-lactic acid (PLLA), poly(L-lactide- co -caprolactone) (PLCL) and poly(lactic- co -glycolic acid) (PLGA) scaffolds by dual phase separation technique and lyophilization.…”

Section: Vte Techniquesmentioning

confidence: 99%

Vascular Tissue Engineering: Polymers and Methodologies for Small Caliber Vascular Grafts

Leal

Wakabayashi

Oyama

et al. 2021

Front. Cardiovasc. Med.

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Cardiovascular disease is the most common cause of death in the world. In severe cases, replacement or revascularization using vascular grafts are the treatment options. While several synthetic vascular grafts are clinically used with common approval for medium to large-caliber vessels, autologous vascular grafts are the only options clinically approved for small-caliber revascularizations. Autologous grafts have, however, some limitations in quantity and quality, and cause an invasiveness to patients when harvested. Therefore, the development of small-caliber synthetic vascular grafts (<5 mm) has been urged. Since small-caliber synthetic grafts made from the same materials as middle and large-caliber grafts have poor patency rates due to thrombus formation and intimal hyperplasia within the graft, newly innovative methodologies with vascular tissue engineering such as electrospinning, decellularization, lyophilization, and 3D printing, and novel polymers have been developed. This review article represents topics on the methodologies used in the development of scaffold-based vascular grafts and the polymers used in vitro and in vivo.

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Early Natural History of Neotissue Formation in Tissue-Engineered Vascular Grafts in a Murine Model

Cited by 24 publications

References 44 publications

Tissue Engineered Vascular Graft Recipient Interleukin 10 Status Is Critical for Preventing Thrombosis

Tissue Engineered Vascular Graft Recipient Interleukin 10 Status Is Critical for Preventing Thrombosis

Effects of Braiding Parameters on Tissue Engineered Vascular Graft Development

Vascular Tissue Engineering: Polymers and Methodologies for Small Caliber Vascular Grafts

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