Comparison of autologous full-thickness gingiva and skin substitutes for wound healing

Abraham P Vriens; Taco Waaijman; Henk M van den Hoogenband; Edith M de Boer; Rik J Scheper; Susan Gibbs

doi:10.3727/096368908787236521

Comparison of autologous full-thickness gingiva and skin substitutes for wound healing

Abraham P Vriens
, Taco Waaijman
, Henk M van den Hoogenband
, Edith M de Boer
, Rik J Scheper
, Susan Gibbs

Department of Dermatology, VU University Medical Centre, O/2 Building, De Boelelaan 1108, 1081 HZ Amsterdam, The Netherlands.

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Ideally tissue-engineered products should maintain the characteristics of the original tissue. For example, skin represents orthokeratinized epithelium and oral gingiva represents parakeratinized epithelium. The aim of this study was to develop an autologous full-thickness gingiva substitute suitable for clinical applications and to compare it with our autologous full-thickness skin substitute that is routinely used for healing chronic wounds. Autologous full-thickness skin and gingiva substitutes were constructed under identical culture conditions from 3-mm punch biopsies isolated from the upper leg or gingiva tissue, respectively. Both consisted of reconstructed epithelia on acellular dermis repopulated with fibroblasts. To compare the characteristics of the original and reconstructed tissue, differential morphological observations and expression of differentiation markers (keratins 6, 10, and 17 and stratum corneum precursors involucrin, loricrin, and SKALP) were determined. Skin and gingiva substitutes were transplanted onto therapy-resistant leg ulcers or tooth extraction sites in order to determine their effects on wound healing. The tissue-engineered constructs maintained many of the differential histological and immunohistochemical characteristics of the original tissues from which they were derived. The skin substitute was orthokeratinized, and the gingiva substitute was parakeratinized. Transplantation of skin (n = 19) and gingiva substitutes (n = 3) resulted in accelerated wound healing with no adverse effects. As identical culture systems were used to generate both the skin and gingiva substitutes, the differences observed in tissue (immuno)histology can be attributed to intrinsic properties of the tissues rather than to environmental factors (e.g., air or saliva). This study emphasizes the importance of closely matching donor sites with the area to be transplanted. Our results represent a large step forward in the area of clinical applications in oral tissue engineering, which have until now greatly lagged behind skin tissue engineering.

Original language	English
Pages (from-to)	1199-209
Number of pages	11
Journal	Cell transplantation
Volume	17
Issue number	10-11
DOIs	https://doi.org/10.3727/096368908787236521
Publication status	Published - 2008

Keywords

Cells, Cultured
Gingiva/metabolism
Gingival Diseases/metabolism
Humans
Keratins/metabolism
Ki-67 Antigen/metabolism
Leg Ulcer/metabolism
Organ Size
Organ Specificity
Pilot Projects
Salvage Therapy
Skin, Artificial
Tissue Distribution
Tooth Extraction/methods
Transplantation, Autologous
Wound Healing/physiology

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10.3727/096368908787236521

Cite this

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title = "Comparison of autologous full-thickness gingiva and skin substitutes for wound healing",

abstract = "Ideally tissue-engineered products should maintain the characteristics of the original tissue. For example, skin represents orthokeratinized epithelium and oral gingiva represents parakeratinized epithelium. The aim of this study was to develop an autologous full-thickness gingiva substitute suitable for clinical applications and to compare it with our autologous full-thickness skin substitute that is routinely used for healing chronic wounds. Autologous full-thickness skin and gingiva substitutes were constructed under identical culture conditions from 3-mm punch biopsies isolated from the upper leg or gingiva tissue, respectively. Both consisted of reconstructed epithelia on acellular dermis repopulated with fibroblasts. To compare the characteristics of the original and reconstructed tissue, differential morphological observations and expression of differentiation markers (keratins 6, 10, and 17 and stratum corneum precursors involucrin, loricrin, and SKALP) were determined. Skin and gingiva substitutes were transplanted onto therapy-resistant leg ulcers or tooth extraction sites in order to determine their effects on wound healing. The tissue-engineered constructs maintained many of the differential histological and immunohistochemical characteristics of the original tissues from which they were derived. The skin substitute was orthokeratinized, and the gingiva substitute was parakeratinized. Transplantation of skin (n = 19) and gingiva substitutes (n = 3) resulted in accelerated wound healing with no adverse effects. As identical culture systems were used to generate both the skin and gingiva substitutes, the differences observed in tissue (immuno)histology can be attributed to intrinsic properties of the tissues rather than to environmental factors (e.g., air or saliva). This study emphasizes the importance of closely matching donor sites with the area to be transplanted. Our results represent a large step forward in the area of clinical applications in oral tissue engineering, which have until now greatly lagged behind skin tissue engineering.",

keywords = "Cells, Cultured, Gingiva/metabolism, Gingival Diseases/metabolism, Humans, Keratins/metabolism, Ki-67 Antigen/metabolism, Leg Ulcer/metabolism, Organ Size, Organ Specificity, Pilot Projects, Salvage Therapy, Skin, Artificial, Tissue Distribution, Tooth Extraction/methods, Transplantation, Autologous, Wound Healing/physiology",

author = "Vriens, \{Abraham P\} and Taco Waaijman and \{van den Hoogenband\}, \{Henk M\} and \{de Boer\}, \{Edith M\} and Scheper, \{Rik J\} and Susan Gibbs",

year = "2008",

doi = "10.3727/096368908787236521",

language = "English",

volume = "17",

pages = "1199--209",

journal = "Cell transplantation",

issn = "0963-6897",

publisher = "Cognizant Communication Corporation",

number = "10-11",

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TY - JOUR

T1 - Comparison of autologous full-thickness gingiva and skin substitutes for wound healing

AU - Vriens, Abraham P

AU - Waaijman, Taco

AU - van den Hoogenband, Henk M

AU - de Boer, Edith M

AU - Scheper, Rik J

AU - Gibbs, Susan

PY - 2008

Y1 - 2008

N2 - Ideally tissue-engineered products should maintain the characteristics of the original tissue. For example, skin represents orthokeratinized epithelium and oral gingiva represents parakeratinized epithelium. The aim of this study was to develop an autologous full-thickness gingiva substitute suitable for clinical applications and to compare it with our autologous full-thickness skin substitute that is routinely used for healing chronic wounds. Autologous full-thickness skin and gingiva substitutes were constructed under identical culture conditions from 3-mm punch biopsies isolated from the upper leg or gingiva tissue, respectively. Both consisted of reconstructed epithelia on acellular dermis repopulated with fibroblasts. To compare the characteristics of the original and reconstructed tissue, differential morphological observations and expression of differentiation markers (keratins 6, 10, and 17 and stratum corneum precursors involucrin, loricrin, and SKALP) were determined. Skin and gingiva substitutes were transplanted onto therapy-resistant leg ulcers or tooth extraction sites in order to determine their effects on wound healing. The tissue-engineered constructs maintained many of the differential histological and immunohistochemical characteristics of the original tissues from which they were derived. The skin substitute was orthokeratinized, and the gingiva substitute was parakeratinized. Transplantation of skin (n = 19) and gingiva substitutes (n = 3) resulted in accelerated wound healing with no adverse effects. As identical culture systems were used to generate both the skin and gingiva substitutes, the differences observed in tissue (immuno)histology can be attributed to intrinsic properties of the tissues rather than to environmental factors (e.g., air or saliva). This study emphasizes the importance of closely matching donor sites with the area to be transplanted. Our results represent a large step forward in the area of clinical applications in oral tissue engineering, which have until now greatly lagged behind skin tissue engineering.

AB - Ideally tissue-engineered products should maintain the characteristics of the original tissue. For example, skin represents orthokeratinized epithelium and oral gingiva represents parakeratinized epithelium. The aim of this study was to develop an autologous full-thickness gingiva substitute suitable for clinical applications and to compare it with our autologous full-thickness skin substitute that is routinely used for healing chronic wounds. Autologous full-thickness skin and gingiva substitutes were constructed under identical culture conditions from 3-mm punch biopsies isolated from the upper leg or gingiva tissue, respectively. Both consisted of reconstructed epithelia on acellular dermis repopulated with fibroblasts. To compare the characteristics of the original and reconstructed tissue, differential morphological observations and expression of differentiation markers (keratins 6, 10, and 17 and stratum corneum precursors involucrin, loricrin, and SKALP) were determined. Skin and gingiva substitutes were transplanted onto therapy-resistant leg ulcers or tooth extraction sites in order to determine their effects on wound healing. The tissue-engineered constructs maintained many of the differential histological and immunohistochemical characteristics of the original tissues from which they were derived. The skin substitute was orthokeratinized, and the gingiva substitute was parakeratinized. Transplantation of skin (n = 19) and gingiva substitutes (n = 3) resulted in accelerated wound healing with no adverse effects. As identical culture systems were used to generate both the skin and gingiva substitutes, the differences observed in tissue (immuno)histology can be attributed to intrinsic properties of the tissues rather than to environmental factors (e.g., air or saliva). This study emphasizes the importance of closely matching donor sites with the area to be transplanted. Our results represent a large step forward in the area of clinical applications in oral tissue engineering, which have until now greatly lagged behind skin tissue engineering.

KW - Cells, Cultured

KW - Gingiva/metabolism

KW - Gingival Diseases/metabolism

KW - Humans

KW - Keratins/metabolism

KW - Ki-67 Antigen/metabolism

KW - Leg Ulcer/metabolism

KW - Organ Size

KW - Organ Specificity

KW - Pilot Projects

KW - Salvage Therapy

KW - Skin, Artificial

KW - Tissue Distribution

KW - Tooth Extraction/methods

KW - Transplantation, Autologous

KW - Wound Healing/physiology

U2 - 10.3727/096368908787236521

DO - 10.3727/096368908787236521

M3 - Article

C2 - 19181214

SN - 0963-6897

VL - 17

SP - 1199

EP - 1209

JO - Cell transplantation

JF - Cell transplantation

IS - 10-11

ER -

Comparison of autologous full-thickness gingiva and skin substitutes for wound healing

Abstract

Keywords

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