Myogenic progenitors contribute to open but not closed fracture repair

Myogenic progenitors contribute to open but not closed fracture repair

<p>Abstract</p> <p>Background</p> <p>Bone repair is dependent on the presence of osteocompetent progenitors that are able to differentiate and generate new bone. Muscle is found in close association with orthopaedic injury, however its capacity to make a cellular contri...

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Main Authors: Liu Renjing, Birke Oliver, Morse Alyson, Peacock Lauren, Mikulec Kathy, Little David G, Schindeler Aaron
Format: Article
Language:English
Published: BMC 2011-12-01
Series:BMC Musculoskeletal Disorders
Online Access:http://www.biomedcentral.com/1471-2474/12/288
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spelling doaj-9165d7c7c9344366b74651dd01433b682020-11-24T21:39:30ZengBMCBMC Musculoskeletal Disorders1471-24742011-12-0112128810.1186/1471-2474-12-288Myogenic progenitors contribute to open but not closed fracture repairLiu RenjingBirke OliverMorse AlysonPeacock LaurenMikulec KathyLittle David GSchindeler Aaron<p>Abstract</p> <p>Background</p> <p>Bone repair is dependent on the presence of osteocompetent progenitors that are able to differentiate and generate new bone. Muscle is found in close association with orthopaedic injury, however its capacity to make a cellular contribution to bone repair remains ambiguous. We hypothesized that myogenic cells of the MyoD-lineage are able to contribute to bone repair.</p> <p>Methods</p> <p>We employed a <it>MyoD</it>-Cre<sup>+</sup>:Z/AP<sup>+ </sup>conditional reporter mouse in which all cells of the MyoD-lineage are permanently labeled with a <it>human alkaline phosphatase (hAP) </it>reporter. We tracked the contribution of MyoD-lineage cells in mouse models of tibial bone healing.</p> <p>Results</p> <p>In the absence of musculoskeletal trauma, MyoD-expressing cells are limited to skeletal muscle and the presence of reporter-positive cells in non-muscle tissues is negligible. In a closed tibial fracture model, there was no significant contribution of hAP<sup>+ </sup>cells to the healing callus. In contrast, open tibial fractures featuring periosteal stripping and muscle fenestration had up to 50% of hAP<sup>+ </sup>cells detected in the open fracture callus. At early stages of repair, many hAP<sup>+ </sup>cells exhibited a chondrocyte morphology, with lesser numbers of osteoblast-like hAP<sup>+ </sup>cells present at the later stages. Serial sections stained for hAP and type II and type I collagen showed that MyoD-lineage cells were surrounded by cartilaginous or bony matrix, suggestive of a functional role in the repair process. To exclude the prospect that osteoprogenitors spontaneously express MyoD during bone repair, we created a metaphyseal drill hole defect in the tibia. No hAP<sup>+ </sup>staining was observed in this model suggesting that the expression of MyoD is not a normal event for endogenous osteoprogenitors.</p> <p>Conclusions</p> <p>These data document for the first time that muscle cells can play a significant secondary role in bone repair and this knowledge may lead to important translational applications in orthopaedic surgery.</p> <p>Please see related article: <url>http://www.biomedcentral.com/1741-7015/9/136</url></p> http://www.biomedcentral.com/1471-2474/12/288
collection DOAJ
language English
format Article
sources DOAJ
author Liu Renjing
Birke Oliver
Morse Alyson
Peacock Lauren
Mikulec Kathy
Little David G
Schindeler Aaron
spellingShingle Liu Renjing
Birke Oliver
Morse Alyson
Peacock Lauren
Mikulec Kathy
Little David G
Schindeler Aaron
Myogenic progenitors contribute to open but not closed fracture repair
BMC Musculoskeletal Disorders
author_facet Liu Renjing
Birke Oliver
Morse Alyson
Peacock Lauren
Mikulec Kathy
Little David G
Schindeler Aaron
author_sort Liu Renjing
title Myogenic progenitors contribute to open but not closed fracture repair
title_short Myogenic progenitors contribute to open but not closed fracture repair
title_full Myogenic progenitors contribute to open but not closed fracture repair
title_fullStr Myogenic progenitors contribute to open but not closed fracture repair
title_full_unstemmed Myogenic progenitors contribute to open but not closed fracture repair
title_sort myogenic progenitors contribute to open but not closed fracture repair
publisher BMC
series BMC Musculoskeletal Disorders
issn 1471-2474
publishDate 2011-12-01
description <p>Abstract</p> <p>Background</p> <p>Bone repair is dependent on the presence of osteocompetent progenitors that are able to differentiate and generate new bone. Muscle is found in close association with orthopaedic injury, however its capacity to make a cellular contribution to bone repair remains ambiguous. We hypothesized that myogenic cells of the MyoD-lineage are able to contribute to bone repair.</p> <p>Methods</p> <p>We employed a <it>MyoD</it>-Cre<sup>+</sup>:Z/AP<sup>+ </sup>conditional reporter mouse in which all cells of the MyoD-lineage are permanently labeled with a <it>human alkaline phosphatase (hAP) </it>reporter. We tracked the contribution of MyoD-lineage cells in mouse models of tibial bone healing.</p> <p>Results</p> <p>In the absence of musculoskeletal trauma, MyoD-expressing cells are limited to skeletal muscle and the presence of reporter-positive cells in non-muscle tissues is negligible. In a closed tibial fracture model, there was no significant contribution of hAP<sup>+ </sup>cells to the healing callus. In contrast, open tibial fractures featuring periosteal stripping and muscle fenestration had up to 50% of hAP<sup>+ </sup>cells detected in the open fracture callus. At early stages of repair, many hAP<sup>+ </sup>cells exhibited a chondrocyte morphology, with lesser numbers of osteoblast-like hAP<sup>+ </sup>cells present at the later stages. Serial sections stained for hAP and type II and type I collagen showed that MyoD-lineage cells were surrounded by cartilaginous or bony matrix, suggestive of a functional role in the repair process. To exclude the prospect that osteoprogenitors spontaneously express MyoD during bone repair, we created a metaphyseal drill hole defect in the tibia. No hAP<sup>+ </sup>staining was observed in this model suggesting that the expression of MyoD is not a normal event for endogenous osteoprogenitors.</p> <p>Conclusions</p> <p>These data document for the first time that muscle cells can play a significant secondary role in bone repair and this knowledge may lead to important translational applications in orthopaedic surgery.</p> <p>Please see related article: <url>http://www.biomedcentral.com/1741-7015/9/136</url></p>
url http://www.biomedcentral.com/1471-2474/12/288
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