Comparison of the Application of Allogeneic Fibroblast and Autologous Mesh Grafting With the Conventional Method in the Treatment of Third-Degree Burns

Moravvej, Hamideh; Hormozi, Abdoljalil Kalantar; Hosseini, Seyed Nejat; Sorouri, Rahim; Mozafari, Nikoo; Ghazisaidi, Mohammad Reza; Rad, Mahnaz Mahmoudi; Moghimi, Mohammad Hossein; Sadeghi, Shahin Mohammad; Mirzadeh, Hamid

doi:10.1097/bcr.0b013e31825aeac1

Cited by 20 publications

(13 citation statements)

References 24 publications

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“…Previous studies have described contraction in mice as a common physiological phenomenon after skin grafting. Park et al (2014) compared the use of splinted versus non-splinted models and demonstrated that the wound generated in the skin of the animal tends to fully shrink and contract after 11 d in non-splinted models, whereas splinted models reduce the contraction rate to near 60 % after 11 d (Gebremeskel et al, 2018;Park et al, 2014). In the present study, the wound contraction percentage reached 61.7 % after 30 d, suggesting a reduction of the wound contraction that may improve re-epithelisation with the grafted tissue.…”

Section: Discussionmentioning

confidence: 99%

“…Numerous models of human skin, generated by tissue engineering, have been developed to date (Beaudoin Cloutier et al, 2017;Bhowmick et al, 2017;Forouzandeh et al, 2010;Hartmann-Fritsch et al, 2016;Klar et al, 2018;Larouche et al, 2016;Lloyd et al, 2015;Pensalfini et al, 2017;Reuter et al, 2017;Strong et al, 2017;Vig et al, 2017). However, few clinical trials have been conducted to test the biological security (phase I and II assays) of human skin models (Boa et al, 2013;Boyce et al, 2006;Boyce et al, 1999;Boyce et al, 2017;Germain et al, 2018;Moravvej et al, 2016;Yamada et al, 2012). Most of the clinically efficient skin models are organotypic structures, consisting of a dermal substitute of dermal fibroblasts immersed in biocompatible scaffolds and an epidermal layer of keratinocytes seeded on top of the stroma.…”

Section: Introductionmentioning

confidence: 99%

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Effective use of mesenchymal stem cells in human skin substitutes generated by tissue engineering

Martín-Piedra¹,

Alfonso²,

Zapater³

et al. 2019

eCM

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Mesenchymal stem cells (MSCs) can differentiate toward epithelial cells and may be used as an alternative source for generation of heterotypical artificial human skin substitutes, thus, enhancing their development and translation potential to the clinic. The present study aimed at comparing four types of heterotypical human bioengineered skin generated using MSCs as an alternative epithelial cell source. Adipose-tissue-derived stem cells (ADSCs), dental pulp stem cells (DPSCs), Wharton's jelly stem cells (WJSCs) and bone marrow stem cells (BMSCs) were used for epidermal regeneration on top of dermal skin substitutes. Heterotypic human skin substitutes were evaluated before and after implantation in immune-deficient athymic mice for 30 d. Histological and genetic studies were performed to evaluate extracellular matrix synthesis, epidermal differentiation and human leukocyte antigen (HLA) molecule expression. The four cell types differentiated into keratinocytes, as shown by the expression of cytokeratin 10 and filaggrin 30 d post-grafting; also, they induced dermal fibroblasts responsible for the synthesis of extracellular fibrillar and non-fibrillar components, in a similar way among each other. WJSCs and BMSCs showed higher expression of cytokeratin 10 and filaggrin, suggesting these cells were more prone to epidermal regeneration. The absence of HLA molecules, even when the epithelial layer was differentiated, supports the future clinical use of these substitutes-especially ADSCs, DPSCs and WJSCs-with low rejection risk. MSCs allowed the generation of bioengineered human skin substitutes with potential clinical usefulness. According to their epidermal differentiation potential and lack of HLA antigens, WJSCs should preferentially be used.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Effective use of mesenchymal stem cells in human skin substitutes generated by tissue engineering

Martín-Piedra¹,

Alfonso²,

Zapater³

et al. 2019

eCM

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“…The use of amniotic membranes in wound healing is supported by its anti‐inflammatory, antiangiogenic and antifibrotic properties, which can induce keratinocyte proliferation, differentiation and re‐epithelialization through a variety of growth factors . Based on our previous studies, we used FAMS as a cover over the wounds. This resulted in complete closure of some wounds, which was evident by the presence of col VII on IFM after 2 weeks.…”

Section: Discussionmentioning

confidence: 99%

Cultured allogeneic fibroblast injection vs. fibroblasts cultured on amniotic membrane scaffold for dystrophic epidermolysis bullosa treatment

et al. 2018

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“…Skin substitutes are defined as a heterogeneous group of substances that aim to restore the skin barrier function, facilitate wound healing, prevent infections and manage pain. Most skin substitutes are acellular; however, in the last few years increasing attention has been paid to the development of cellular substitutes mainly manufactured using two types of cells: fibroblasts and keratinocytes . Moreover, recent researches also include new cell types such as melanocytes, mesenchymal stem cells (MSCs), epidermal stem cells, hair follicle stem cells and even cell‐based products such as platelet‐rich‐plasma (PRP) …”

Section: Introductionmentioning

confidence: 99%

“…Most skin substitutes are acellular; however, in the last few years increasing attention has been paid to the development of cellular substitutes mainly manufactured using two types of cells: fibroblasts and keratinocytes. [4][5][6] Moreover, recent researches also include new cell types such as melanocytes, 7 mesenchymal stem cells (MSCs), 8 epidermal stem cells, 9 hair follicle stem cells 10 and even cell-based products such as platelet-rich-plasma (PRP). [11][12][13] New approaches for skin TE are focused on combining novel natural or synthetic materials and living cells in several biomedical and pharmaceutical applications.…”

Section: Introductionmentioning

confidence: 99%

Therapeutic strategies for skin regeneration based on biomedical substitutes

Chocarro‐Wrona

López‐Ruiz

Perán

et al. 2019

Acad Dermatol Venereol

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Regenerative medicine and tissue engineering (TE) have experienced significant advances in the development of in vitro engineered skin substitutes, either for replacement of lost tissue in skin injuries or for the generation of in vitro human skin models to research. However, currently available skin substitutes present different limitations such as expensive costs, abnormal skin microstructure and engraftment failure. Given these limitations, new technologies, based on advanced therapies and regenerative medicine, have been applied to develop skin substitutes with several pharmaceutical applications that include injectable cell suspensions, cell‐spray devices, sheets or 3Dscaffolds for skin tissue regeneration and others. Clinical practice for skin injuries has evolved to incorporate these innovative applications to facilitate wound healing, improve the barrier function of the skin, prevent infections, manage pain and even to ameliorate long‐term aesthetic results. In this article, we review current commercially available skin substitutes for clinical use, as well as the latest advances in biomedical and pharmaceutical applications used to design advanced therapies and medical products for wound healing and skin regeneration. We highlight the current progress in clinical trials for wound healing as well as the new technologies that are being developed and hold the potential to generate skin substitutes such as 3D bioprinting‐based strategies.

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Comparison of the Application of Allogeneic Fibroblast and Autologous Mesh Grafting With the Conventional Method in the Treatment of Third-Degree Burns

Cited by 20 publications

References 24 publications

Effective use of mesenchymal stem cells in human skin substitutes generated by tissue engineering

Effective use of mesenchymal stem cells in human skin substitutes generated by tissue engineering

Cultured allogeneic fibroblast injection vs. fibroblasts cultured on amniotic membrane scaffold for dystrophic epidermolysis bullosa treatment

Therapeutic strategies for skin regeneration based on biomedical substitutes

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