Heterotopic Ossification : Clinical and Experimental Studies on Risk Factors, Etiology and Inhibition by Non-steroidal Anti-inflammatory Drugs

Persson, Per-Erik

January 2004

<p>In this thesis, occurrence of heterotopic ossification (HO) following total hip arthroplasty (THA) was studied. Preventive effects and complications with non-steroidal anti-inflammatory drugs (NSAIDs) were analyzed. Experimental investigations on bone formation were employed to gain insight to the mechanism of NSAIDs action on bone.</p><p>(I). Fifty-six patients with bilateral THAs were analyzed. We found a strong correlation between HO on the two sides. Incidence and grade of HO were higher in men than in women.</p><p>(II). Sixty-nine patients with bilateral THAs who had been treated with NSAIDs after one or both THAs were analyzed for HO. Widespread HO occurred in untreated THAs, but in none of the treated THAs.</p><p>(III). A consecutive series of THAs were analyzed for HO. No widespread HO occurred in patients treated with NSAIDs for 21 days. In contrast, widespread HO occurred in 23% of patients not treated.</p><p>(IV). A randomized, double-blind, prospective study on 144 patients was performed to determine the efficacy and minimum treatment time with Ibuprofen for prophylaxis of HO after THA. Treatment with Ibuprofen was effective for preventing HO and a treatment time of 8 days was sufficient.</p><p>(V). A ten-year follow-up examination was performed on the patients from study IV. Thirteen patients had been revised. All but one belonged to groups treated with Ibuprofen. However, the prosthetic survival time was not statistically different for patients treated with NSAIDs compared to the control group. Eighty-four more patients underwent radiographic examination10 years after THA. Nine loose prostheses were found. These were equally distributed between NSAIDs-treated and non-treated THAs. When combining complications (revisions and radiographic loosening) no significant effects could be verified.</p><p>(VI). Experimental induction of heterotopic new bone with demineralized allogeneic bone matrix (DABM) and with bone autografts, was used in rats to study effects of NSAIDs on new bone formation. Indomethacin inhibited net bone formation in DABMs and in orthotopic fractured bone. In contrast, a net mineral loss occurred in autografts, but neither mineral content nor ⁴⁵Ca incorporation was affected by Indomethacin treatment. The amount of bone formed per mg implanted DABM was linearly correlated to implant size.</p>

Surgery

Heterotopic ossification

Hip prosthesis

NSAIDs

Prophylaxis

Prosthesis loosening

Reoperation

Animal model

Bone formation

Kirurgi

Surgery

Kirurgi

Die rol van ruimte in Afrikaanse spookstories / deur Mariëtte van Graan

Van Graan, Mariëtte

January 2008

Thesis (M.A. (Afrikaans and Dutch))--North-West University, Potchefstroom Campus, 2008.

Ghost stories

Space

Fantasy

Horror

Gothic

Realism

Umheimlich (Freud)

Rhetorical space

Heterotopic space

Liminality

Liminal space

Liminal process

Heterotopic Ossification : Clinical and Experimental Studies on Risk Factors, Etiology and Inhibition by Non-steroidal Anti-inflammatory Drugs

Persson, Per-Erik

January 2004

In this thesis, occurrence of heterotopic ossification (HO) following total hip arthroplasty (THA) was studied. Preventive effects and complications with non-steroidal anti-inflammatory drugs (NSAIDs) were analyzed. Experimental investigations on bone formation were employed to gain insight to the mechanism of NSAIDs action on bone. (I). Fifty-six patients with bilateral THAs were analyzed. We found a strong correlation between HO on the two sides. Incidence and grade of HO were higher in men than in women. (II). Sixty-nine patients with bilateral THAs who had been treated with NSAIDs after one or both THAs were analyzed for HO. Widespread HO occurred in untreated THAs, but in none of the treated THAs. (III). A consecutive series of THAs were analyzed for HO. No widespread HO occurred in patients treated with NSAIDs for 21 days. In contrast, widespread HO occurred in 23% of patients not treated. (IV). A randomized, double-blind, prospective study on 144 patients was performed to determine the efficacy and minimum treatment time with Ibuprofen for prophylaxis of HO after THA. Treatment with Ibuprofen was effective for preventing HO and a treatment time of 8 days was sufficient. (V). A ten-year follow-up examination was performed on the patients from study IV. Thirteen patients had been revised. All but one belonged to groups treated with Ibuprofen. However, the prosthetic survival time was not statistically different for patients treated with NSAIDs compared to the control group. Eighty-four more patients underwent radiographic examination10 years after THA. Nine loose prostheses were found. These were equally distributed between NSAIDs-treated and non-treated THAs. When combining complications (revisions and radiographic loosening) no significant effects could be verified. (VI). Experimental induction of heterotopic new bone with demineralized allogeneic bone matrix (DABM) and with bone autografts, was used in rats to study effects of NSAIDs on new bone formation. Indomethacin inhibited net bone formation in DABMs and in orthotopic fractured bone. In contrast, a net mineral loss occurred in autografts, but neither mineral content nor 45Ca incorporation was affected by Indomethacin treatment. The amount of bone formed per mg implanted DABM was linearly correlated to implant size.

Surgery

Heterotopic ossification

Hip prosthesis

NSAIDs

Prophylaxis

Prosthesis loosening

Reoperation

Animal model

Bone formation

Kirurgi

Surgery

Kirurgi

Die rol van ruimte in Afrikaanse spookstories / deur Mariëtte van Graan

Van Graan, Mariëtte

January 2008

This study investigates the functions of space in the Afrikaans ghost story. The aim of this study is to form an overall understanding of the functions of space in the Afrikaans ghost story, and also to promp further investigations into this branch of Afrikaans literature. The study is mainly text-analytical, and is therefore practical rather than theoretical. Aspects of space in the texts are discussed with reference to several different theoretical frameworks, such as: genre-definition; space in prose; realism and reality; reader-oriented approaches; frame stories; Freud's concept of the unheimlich; rhethorical and heterotopical spaces; and different aspects of liminality. The spaces that are specifically discussed include the prototypical haunted house, the farm setting, the road or tunnel setting, die cemetery setting and the city setting. The conclusion reached in this study is that space performs four important functions in the Afrikaans ghost story. These functions are: space is a defining characteristic of the genre; space functions as a link between reality and the supernatural; space forms part of the cast of the genre; space is pre-eminently liminal. / Thesis (M.A. (Afrikaans and Dutch))--North-West University, Potchefstroom Campus, 2008.

Ghost stories

Space

Fantasy

Horror

Gothic

Realism

Umheimlich (Freud)

Rhetorical space

Heterotopic space

Liminality

Liminal space

Liminal process

Die rol van ruimte in Afrikaanse spookstories / deur Mariëtte van Graan

Van Graan, Mariëtte

January 2008

This study investigates the functions of space in the Afrikaans ghost story. The aim of this study is to form an overall understanding of the functions of space in the Afrikaans ghost story, and also to promp further investigations into this branch of Afrikaans literature. The study is mainly text-analytical, and is therefore practical rather than theoretical. Aspects of space in the texts are discussed with reference to several different theoretical frameworks, such as: genre-definition; space in prose; realism and reality; reader-oriented approaches; frame stories; Freud's concept of the unheimlich; rhethorical and heterotopical spaces; and different aspects of liminality. The spaces that are specifically discussed include the prototypical haunted house, the farm setting, the road or tunnel setting, die cemetery setting and the city setting. The conclusion reached in this study is that space performs four important functions in the Afrikaans ghost story. These functions are: space is a defining characteristic of the genre; space functions as a link between reality and the supernatural; space forms part of the cast of the genre; space is pre-eminently liminal. / Thesis (M.A. (Afrikaans and Dutch))--North-West University, Potchefstroom Campus, 2008.

Ghost stories

Space

Fantasy

Horror

Gothic

Realism

Umheimlich (Freud)

Rhetorical space

Heterotopic space

Liminality

Liminal space

Liminal process

Deciphering the role of the mononuclear phagocyte system in post-transplant airway fibrosis

Di Campli, Maria Pia

10 September 2020

Bronchiolitis obliterans syndrome (BOS), a form of chronic lung allograft dysfunction, represents a major cause of mortality after lung transplantation. This disease is associated with a progressive fibro-obliteration of small airways (known as obliterative bronchiolitis) which leads to respiratory impairment and graft failure. The mechanisms behind airway occlusion remain unclear, and no curative treatment is available at the moment. Myofibroblasts are considered central effectors in this fibrotic process, but their origin is controversial. They can arise either from donor cells (resident fibroblasts and epithelial cells) or recipient cells (bone marrow-derived cells).The purpose of this project was to identify the precursors of mesenchymal cells responsible for post-transplant airway fibro-obliteration. Lineage-tracing tools were used to track or deplete potential sources of myofibroblasts in the heterotopic tracheal transplantation model, which produces a surrogate of obliterans bronchiolitis. Confocal analysis showed that myofibroblasts in the allografts were mostly recipient-derived, even though immunosuppression with tacrolimus induced a mild increase of donor-derived myofibroblasts. Occasional epithelial-to-mesenchymal transition was detected, but only in tacrolimus-treated recipients. On the other hand, fate-mapping techniques demonstrated that myeloid cells gave rise to the majority of mesenchymal cells in occluded airways. Accordingly, specific ablation of Cx3cR1+ mononuclear phagocytes significantly decreased allografts fibrosis. In parallel, single-cell RNA-sequencing unveiled surprising similarities between myeloid-derived cells (i.e. fibrocytes and macrophages) from the allografts and both murine and human samples of pulmonary fibrosis. Finally, analysis of BOS lesions from transplanted patients allowed us to translate our results to a clinical level. Indeed, confocal microscopy revealed that myofibroblasts expressing the macrophage marker CD68 were increased in BOS explants when compared to controls, and their numbers seemed correlated with the intensity of fibrosis.Collectively, these findings indicate that recipient mononuclear phagocyte system constitutes a clinically relevant source of mesenchymal cells infiltrating the airways after allogeneic transplantation. Therefore, therapies targeting migration and differentiation of mononuclear phagocytes and fibrocytes could prevent fibrotic remodelling of small airways and improve long-term outcomes after lung transplantation. / La bronchiolite oblitérante (bronchiolitis obliterans syndrome, BOS), une forme de dysfonction chronique du greffon, représente une des majeures causes de mortalité après transplantation pulmonaire. Cette pathologie est associée à une oblitération progressive et irréversible des petites voies aériennes par de la fibrose, qui mène à une perte de fonction respiratoire jusqu’à la défaillance du greffon. Les mécanismes impliqués dans la fibroproliferation ne sont pas encore bien compris, et il n’existe pas de traitement efficace de la BOS à l’heure actuelle. Les myofibroblastes joueraient un rôle majeur dans le développement de la fibrose, mais leur origine reste controversée. Ils pourraient dériver des cellules du donneur (fibroblastes in situ ou cellules épithéliales) ou bien du receveur (à partir de la moelle osseuse). L’objectif de cette étude était d’identifier les précurseurs des cellules mésenchymateuses responsables de l’obstruction des voies aériennes après transplantation allogénique. Nous avons utilisé des techniques de lineage tracing pour identifier les sources potentielles de myofibroblastes dans un modèle de transplantation hétérotopique de trachée, lequel permet d’obtenir une maladie fibro-oblitérante du greffon qui simule histologiquement la bronchiolite oblitérante. Les analyses par microscopie confocale ont montré que les cellules du receveur constituent la source principale de myofibroblastes dans les allogreffons, malgré une faible augmentation de la proportion de cellules mésenchymateuses dérivées du donneur lors du traitement immunosuppresseur. En plus, une minime fraction de myofibroblastes d’origine épithéliales a également été détectée, mais seulement dans les greffons traités par tacrolimus. D’autre part, nous avons établi que la lignée myéloïde produit la plupart des cellules mésenchymateuses détectés dans les voies aériennes oblitérées. Par ailleurs, la délétion spécifique de phagocytes mononucléaires Cx3cR1+ était associée avec une diminution significative du nombre de myofibroblastes et de la fibrose endoluminale dans les allogreffons. En parallèle, l’utilisation des techniques de séquençage en single cell a permis de révéler des ressemblances inattendues entre des populations de cellules d’origine myéloïdes (macrophages et fibrocytes) retrouvés dans les greffons et celles impliqués dans le développement de la fibrose pulmonaire chez l’homme et la souris. In fine, l’analyse par microscopie confocale des lésions pulmonaires de patients atteints de BOS nous a permis de transposer en clinique nos résultats expérimentaux. En effet, nous avons observé que la fraction de myofibroblastes positifs pour le CD68, un marqueur typiquement exprimé par les macrophages, était significativement augmentée dans les greffons avec bronchiolite oblitérante par rapport aux contrôles. De plus, leur nombre était corrélé avec la sévérité de la fibrose. L’ensemble de ces résultats indique que le système phagocytaire mononuclée constitue une source significative de cellules mésenchymateuses et contribue à la fibro-oblitération des voies aériennes après transplantation. L’utilisation de thérapies ciblant la migration et la différenciation des phagocytes mononuclées et des fibrocytes pourrait bloquer la destruction du greffon pulmonaire et améliorer la survie à long terme des patients transplantés. / Doctorat en Sciences médicales (Médecine) / info:eu-repo/semantics/nonPublished

Transplantation d'organes

Immunologie

Pneumologie

Chirurgie

Bronchiolitis obliterans syndrome

heterotopic tracheal transplantation

myofibroblasts

lineage-tracing

organ fibrosis

chronic lung allograft dysfunction

Neofunction of ACVR1 in fibrodysplasia ossificans progressiva / 進行性骨化性線維異形成症における変異ACVR1の新たな機能

Hino, Kyosuke

23 May 2016

京都大学 / 0048 / 新制・論文博士 / 博士(医学) / 乙第13031号 / 論医博第2113号 / 新制||医||1016(附属図書館) / 32989 / (主査)教授 妻木 範行, 教授 安達 泰治, 教授 開 祐司 / 学位規則第4条第2項該当 / Doctor of Medical Science / Kyoto University / DFAM

induced pluripotent stem cell (iPSC)

heterotopic ossification

bone morphogenetic protein (BMP)

transforming growth factor (TGF)

490

Ossification hétérotopique traumatique : altérations du microenvironnement des progéniteurs du muscle squelettique et induction du programme de différenciation ostéogénique / Traumatic heterotopic ossification: alterations of the microenvironment of skeletal muscle progenitor cells and induction of the osteogenic differentiation program

Drouin, Geneviève

January 2016

Résumé: Le muscle squelettique possède une excellente capacité à se regénérer notamment grâce à ses cellules progénitrices stromales (mrSC) et myogéniques (CPM). À la suite de certains traumas et pour des raisons encore méconnues, la qualité de sa régénération est compromise ce qui mène à l’apparition de structures aberrantes tel l’os mature, aussi appelée ossification hétérotopique (OH) post-traumatique. Notre laboratoire a montré dans un modèle murin que les mrSC sont pleinement impliquées dans cette pathologie. De plus, un facteur fortement ostéoinducteur, BMP9, ne cause l’OH que si, et seulement si, le muscle est endommagé. Ce modèle d’étude est unique puisqu’il présente les particularités physiopathologiques de l’OH post-traumatique, un dommage du muscle étant essentiel à la formation d’os. De plus, ce modèle a permis de mettre en évidence le rôle prédominant du microenvironnement des cellules progénitrices dans le développement de cette pathologie. Nous avons donc émis l’HYPOTHÈSE selon laquelle le microenvironnement du muscle endommagé contient des facteurs qui peuvent influencer le phénotype de ses cellules progénitrices stromales et myogéniques favorisant ainsi le développement de l’OH. Nos résultats montrent que l’état hypoxique d’un muscle sévèrement endommagé augmente la prolifération et la différenciation ostéogénique des mrSC. De plus, l’hypoxie induit spécifiquement l’expression de BMP9 par les mrSC. L’impact de BMP9 a également été évalué sur la différenciation des CPM. Les résultats montrent qu’à des concentrations physiologiques, BMP9 inhibe le potentiel myogénique des CPM en faveur d’une différenciation ostéogénique, et cela tant dans la lignée myoblastique murine C2C12 que chez les CPM primaires humaines. En résumé, le muscle endommagé développant l’OH possède un microenvironement spécifique responsable du débalancement de la capacité régénérative de ses progéniteurs. Nos travaux montrent que ce microenvironnement cause un retard de la myogenèse et une ostéogenèse où participeront non seulement les mrSC mais également les CPM. L’identification et la compréhension des mécanismes régulant ces facteurs s’avèrent clé pour offrir aux cliniciens des outils de diagnostic mais également des alternatives ou des approches complémentaires aux traitements prophylaxiques actuels. / Abstract: Skeletal muscle has an extraordinary ability to regenerate due to its resident stromal cells (mrSCs) and myogenic progenitor cells (MPCs). Following certain traumas, the quality of the regeneration of skeletal muscle can be compromised for unknown reasons, leading to the appearance of aberrant structures such as mature bone, a process called posttraumatic heterotopic ossification (HO). Our laboratory developed a mouse model to show that mrSCs are fully involved in this pathology. We also showed that BMP9, a highly osteoinductive factor, causes HO if and only if the muscle is damaged. This model is unique in that it recapitulates the pathophysiological features of post-traumatic HO in which muscle damage is essential for bone formation. The model was also used to show that the progenitor cell microenvironment plays a predominant role in the development of this pathology. Based on these results, we HYPOTHESIZED that the microenvironment of the damaged muscle contains factors that can influence the phenotype of its progenitor cell populations, thus promoting the development of HO. Our results showed that the hypoxic state of a severely damaged muscle increases the proliferation and osteogenic differentiation of mrSCs and also specifically induces the expression of BMP9 by mrSCs. The impact of BMP9 on the differentiation of MPCs was also evaluated. At physiological concentrations, BMP9 inhibited the myogenic differentiation potential of murine myoblast C2C12 cells and primary human MPCs, and triggered their differentiation into an osteogenic lineage. In summary, we showed that damaged muscle that develops HO has a specific microenvironment that is responsible for the loss of the regenerative capacity of progenitor cells, leading to a delay in myogenesis, and that mrSCs and MPCs are both involved in osteogenesis. The identification and understanding of the mechanisms regulating these key factors could provide clinicians with valuable diagnostic tools as well as alternative and/or complementary approaches to current prophylactic treatments.

Muscle squelettique

Ossification hétérotopique

Microenvironnement

Désordre régénératif

Cellules progénitrices

Hypoxie

BMP9

Différenciation cellulaire

Trauma

Skeletal muscle

Heterotopic ossification

Microenvironment

Regenerative disorder

Progenitor cells

Hypoxia

Cell differentiation

Kinase MSK1 et bronchiolite oblitérante / Kinase MSK1 and obliterative bronchiolitis

Nemska, Simona

11 September 2012

La bronchiolite oblitérante (BO) est la principale cause de décès à long terme après transplantation pulmonaire. La BO se manifeste par une diminution des capacités respiratoires liée à l’obstruction des petites voies aériennes par un tissu inflammatoire et fibroprolifératif. Dans cette thèse nous avons étudié l’hypothèse de l’implication de la kinase nucléaire MSK1 dans la BO. Nous avons utilisé la transplantation hétérotopique de trachée comme modèle murin de BO. La pertinence du choix de ce modèle a été confirmée par l’étude de la re-vascularisation fonctionnelle de la greffe après transplantation. Dans ce modèle nous avons montré une augmentation de l’expression et de l’activité de MSK1 pendant le développement de la BO. Le traitement des souris transplantées avec des inhibiteurs pharmacologiques de MSK1 a permis d’inhiber l’inflammation et la fibroprolifération, montrant le rôle de MSK1 dans la BO. Nous avons également mis en place un essai de criblage utilisant la technologie HTRF pour rechercher de nouveaux inhibiteurs de MSK1. Les résultats décrits dans cette thèse, montrent que la kinase MSK1 est une potentielle cible thérapeutique pour combattre la BO. / Obliterative bronchiolitis (OB) is the chronic rejection after lung transplantation and is the main cause for late death post-transplantation. OB is characterized by decrease of the pulmonary function caused by obstruction of the small airways by inflammatory and fibroproliferative tissue. We studied the hypothesis of the implication of the nuclear kinase MSK1 in the OB. The relevance of the model was demonstrated by showing the rapid functional re-vascularization of the graft. In this model the allograft, shows an increased MSK1 expression and activity. We therefore treated mice with pharmacological inhibitors of the MSK1 activity and we demonstrated an inhibition of the inflammation and the fibroproliferation during OB. We next set up an enzymatic assay using the heterogeneous time-resolved fluorescence, to proceed for a screening for new MSK1 inhibitors. In summary, this study proposed MSK1 as potential therapeutic target to combat OB.

Transplantation pulmonaire

Bronchiolite oblitérante

Kinase MSK1

Vascularisation

Criblage

Inhibiteurs

Obliterative bronchiolitis

MSK1 kinase

Heterotopic tracheal transplantation

Vascularization

Screening

Inhibitors

571.96

617.95

Efeito da radioterapia na profilaxia da ossificação heterotópica em pacientes com lesão medular traumática / The effect of radiotherapy on the prophylaxis of heterotopic ossification in patients with spinal cord injury

Castro, Anita Weigand de

12 January 2009

O objetivo deste trabalho foi estudar o efeito da radioterapia na profilaxia da ossificação heterotópica (OH) em pacientes com lesão medular traumática. Foram estudados 19 pacientes (15 homens e quatro mulheres), média de idade de 30,4 ± 10,8 anos (19 a 58 anos), com lesão medular traumática. A causa mais freqüente da lesão medular foi acidente de trânsito (42,1%), seguida por queda (26,3%), ferimento por projétil de arma de fogo (21%), mergulho (5,3%) e queda de objeto sobre as costas (5,3%). Dez pacientes eram tetraplégicos (52,6%) e nove (47,4%) eram paraplégicos. Apresentavam lesão medular completa (Frankel A) 14 pacientes (73,7%) e cinco pacientes (25,3%) tinham lesão incompleta (Frankel B). Todos os pacientes incluídos no estudo realizaram cintilografia óssea inicial até um mês após o traumatismo raquimedular e apresentaram diagnóstico negativo para OH. Os pacientes foram divididos em dois grupos: nove pacientes receberam radioterapia em dose única de 8 Gy nos quadris (Grupo Estudo) e 10 pacientes compuseram o Grupo Controle. Após seis meses de seguimento clínico e radiológico, um paciente do Grupo Estudo (11%) e cinco pacientes do Grupo Controle (50%) apresentaram OH. A distribuição da freqüência do desenvolvimento da OH nos dois grupos não mostrou diferença estatística significante, apesar da menor incidência de OH no grupo submetido à radioterapia (Grupo Estudo). Concluiu-se que, com o número de pacientes estudados, não foi possível comprovar a eficácia da radioterapia na prevenção da ossificação heterotópica, ainda que haja uma forte tendência para a correlação estatística / The goal of this study was to evaluate the effect of radiotherapy on the prophylaxis of heterotopic ossification (HO) after spinal cord injury (SCI). Nineteen SCI patients were studied (15 men and four women). The mean age was 30.4 ± 10.8 years (range 19 to 58 years). The most frequent causes of lesion were traffic accident (42.1%), fall (26.3%), shot gun (21%), diving (5.3%) and objects falling on the vertebral column (5.3%). Ten patients were tetraplegics (52.6%) and nine were paraplegics. Fourteen patients (73.7%) had complete lesion (Frankel A) and five had incomplete lesion (Frankel B). All patients realized initial scintigraphy until one month after SCI and showed negative results for HO. The patients were randomized in two groups: nine patients received single dose irradiation with 8 Gy on the hips (Study Group) and 10 patients were the Control Group. After six months of clinical and radiological follow up, one patient of the Study Group (11%) and five patients of Control Group (50%) showed HO. The frequency distribution of the development of HO in both groups showed no significant statistical difference, although there was lower incidence of HO in the radiotherapy group. We concluded that, with the number of patients studied, it was no possible to prove the efficacy of radiotherapy to prevent HO, although had a strong tendency for the statistical correlation

Paraplegia/complicações

Paraplegia/complications

Quadriplegia/complicações

Quadriplegia/complications

Radioterapia

Radiotherapy

Spinal cord injury/complications