903 resultados para Incidence Matrix
Resumo:
Background Breast cancer in younger women has received increased attention in recent years. Although breast cancer is uncommon in young women, it is the most frequent cancer and the leading cause of cancer death for younger women in developed countries. For Switzerland, the United States and several European countries, declines in breast cancer incidence have been reported since around the year 2000, after decades of increase, among women aged 50 and older. On the other hand an increase in the incidence of breast cancer in younger women has been reported in recent years. Therefore, this study aims to evaluate time trends in breast cancer incidence in younger women in Switzerland. Methods Data on invasive breast cancer cases were obtained from the Swiss Cancer Registries of Basel, Fribourg, Geneva, Graubunden/Glarus, Jura, Neuchatel, St. Gallen-Appenzell, Ticino, Valais, Vaud and Zurich, covering the time period 1996 to 2009. Mid-year population estimates for the respective time period were supplied by the Swiss Federal Statistical Office. For females aged 20-49 years, annual age-standardized incidence rates (ASIRs) (European standard) per 100,000 person-years and corresponding 95%-confidence intervals (95% CI) were calculated. For females aged 20-39 and 40-49 years, ASIRs and incidence rate ratios (IRRs) were calculated by grouped time periods, consisting of 3-5 incidence years. IRRs and corresponding 95% CI were calculated using Poisson regression adjusting for age (reference period 1996-2000). Results ASIRs in females aged 20-49 increased gradually since 1996, being 57.36 per 100,000 person-years in 1996 (95% CI 52.54-62.51) and rising to 68.34 (95% CI 63.40-73.57) per 100,000 person-years in 2009. Comparing the time-period 2007-2009 and the reference period 1996-2000, IRRs show values of 1.17 (95% CI 1.04-1.31) for the age-group 20-39 years and 1.04 (95% CI 0.97-1.10) for the age-group 40-49 years. Conclusions Our findings confirm a slight increase in the incidence of invasive breast cancer in younger women in Switzerland during the period 1996-2009. An increase in breast cancer incidence in younger patients is an important public health problem. It warrants further investigations to identify specific risk factors of this population and to better understand the biology of this particular breast cancer.
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This paper analyzes whether standard covariance matrix tests work whendimensionality is large, and in particular larger than sample size. Inthe latter case, the singularity of the sample covariance matrix makeslikelihood ratio tests degenerate, but other tests based on quadraticforms of sample covariance matrix eigenvalues remain well-defined. Westudy the consistency property and limiting distribution of these testsas dimensionality and sample size go to infinity together, with theirratio converging to a finite non-zero limit. We find that the existingtest for sphericity is robust against high dimensionality, but not thetest for equality of the covariance matrix to a given matrix. For thelatter test, we develop a new correction to the existing test statisticthat makes it robust against high dimensionality.
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1.1. La greffe de rein La greffe d'organes a révolutionné la médecine. De tout le temps elle a suscité les fantasmes et les rêves : la pratique est ancestrale ; elle remonte au 3ème siècle lorsque Saint Côme et Saint Damien réalisent pour la première fois une greffe de jambe de Maure sur un patient. Il faudra néanmoins attendre le 20ème siècle pour voir la transplantation se réaliser plus concrètement avec succès et se généraliser. A Vienne, en 1902, le Dr. Ulmann (1861-1937) pratique la toute première autogreffe de rein sur un chien. Il replace le rein de l'animal au niveau du cou, pratiquant une anastomose vasculaire. Depuis, les tentatives se multiplient et peu après le Dr. Von Decastello, pratique la première transplantation chien-chien. Par la suite, en associa- tion avec le Dr. Ulmann la première greffe entre un chien et une chèvre aura lieu, avec un certain succès. En effet, elle a permis à l'animal receveur de produire de l'urine. L'avancée majeure durant ce début de siècle fut le développement d'une nouvelle technique de suture vasculaire par le Dr. Carrel, qui obtiendra le prix Nobel en 1912. Son élève, le Dr. Jaboulay (1860-1913) a réalisé plusieurs tentatives de xénogreffes rénales. Il pratiquera en 1906 les deux premières xénogreffes en utilisant un cochon et une chèvre comme donneurs. Le greffon fut respectivement placé au niveau de la cuisse et du bras des patients. La fonction rénale durera une heure. En 1909 Ernest Unger (1875-1938) transplanta un rein de fox-terrier sur un boxer, avec une production d'urine pendant 14 jours. Durant la même année le Dr. Unger a pratiqué une xénogreffe en transplantant un rein de nouveau né sur un babouin, cette intervention se terminant par la mort de l'animal. Un autre essai de greffe singe à humain, pratiqué sur une femme mourant de défaillance rénale, a fait comprendre à Unger qu'il y a des barrières biologiques dans la transplantation, mais que la greffe rénale est techniquement faisable. En 1914, J.B. Murphy découvre l'importance de la rate et de la moelle osseuse dans la réponse immune. En 1933 et 1949 en Ukraine, les premières allogreffes humaines de reins sont pratiquées par le chirurgien soviétique Yu Yu Voronoy. Malheureuse- ment aucune fonction rénale des greffons n'a été observée. Après une période de « stagnation scientifique » générale qui durera à peu près 10 ans, l'intérêt pour la transplantation refait surface dans les années 1950. Deux équipes de chirurgien se forment : une à Boston et l'autre à Paris. De nombreux cas d'allogreffes humaines sans immunosuppression sont documentés de 1950 à 1953. Malheureusement chaque opération aboutit à un échec, ceci dû aux phénomènes du rejet. M. Simonsen et WJ. Dempster découvrent qu'un mécanisme immun est à la base du rejet. Ils établissent aussi que la position pelvienne était meilleure que la position plus superficielle. Grâce aux découvertes dans le domaine du rejet et les nombreux progrès techniques, une allogreffe entre vrais jumeaux est pratiquée à Boston en 1954. L'opération est un succès total et permet de contrer toutes les hypothèses négatives avancées par certains groupes de travail. Depuis 1948, de nombreux travaux dans le domaine de l'immunosuppression ont été entrepris. La découverte de l'action immunosuppressive de la cortisone permet son instauration dans le traitement anti-rejet, malheureusement avec peu de succès. En effet, l'irradiation totale reste la méthode de choix jusqu'en 1962, date de l'apparition de l'Azaothioprine (Imuran®). La découverte de l'Azaothioprine, permet d'avancer de nouvelles hypothèses concernant le rejet : en évitant le rejet post-opératoire aigu, une protection et une adaptation au receveur pourraient être modulées par l'immunosuppression. Dans les années 1960, l'apparition des immunosuppresseurs de synthèse permet de développer de nouvelles lignes de traitement. Le Dr.Starzl et ses collègues, découvrent l'efficacité d'un traitement combiné de Prednisone et d'Azathioprine qui devient alors le standard d'immunosuppression post greffe durant cette période. Les années 60 et 70 sont des années d'optimisme. La prise en charge des patients s'améliore, le développement de la dialyse permet de maintenir en vie les patients avant la greffe, les techniques de conservation des organes s'améliorent, la transplantation élargit son domaine d'action avec la première greffe de coeur en 1968. Le typage tissulaire permet de déterminer le type d'HLA et la compatibilité entre le re- ceveur et le donneur afin de minimiser les risques de rejet aigu. Les années 1970 se caractérisent par deux amélioration majeures : celle du typage HLA-DR et l'apparition des inhibiteurs de la calcineurine (Cyclosporine A). Ce dernier restera l'agent de premier choix jusqu'aux alentours des années 1990 où apparaissaient de nouveaux immunosuppresseurs, tels que les inhibiteurs mTOR (siroli- mus) et les inhibiteurs de l'inosine monophosphate déshydrogénase (mycophénolate mofétil), par exemple. En conclusion, la transplantation rénale a été une des premières transplantations d'organes solides pratiquées sur l'homme avec de nombreux essais cliniques impliquant une multitude d'acteurs. Malgré des périodes de hauts et de bas, les avancements techniques ont été notables, ce qui a été très favorable en terme de survie pour les patients nécessitant une greffe. 1.2. Le lymphocèle La greffe rénale, comme toute autre acte chirurgical, comporte des risques et une morbidité spécifique. Le lymphocèle a la prévalence la plus élevée, qui peut aller de 0.6 à 51% 1-3 avec des variations entre les études. Le lymphocèle est défini comme une collection post opératoire de liquide lymphatique dans une cavité non épithélialisée et n'est pas causée par une fuite urinaire ou une hémorragie1, 4. Historiquement, le lymphocèle a été décrit pour la première fois dans la littérature médicale dans les années 1950, par Kobayashi et Inoue5 en chirurgie gynécologique. Par la suite Mori et al.6 en 1960 documentent la première série d'analyse de lymphocèles. En 1969 le lymphocèle est décrit pour la première fois par Inociencio et al.7 en tant que complication de greffe rénale. Sa pathogénèse n'est pas complètement élucidée, cependant plusieurs facteurs de risque ont été identifiés tels que : la ligature inadéquate des vaisseaux lymphatiques lors de la dissection des vaisseaux iliaques du donneur et de la préparation du greffon, le BMI, les diurétiques, l'anticoagulation (héparine), les hautes doses de stéoïdes, certains agents immunosuppresseurs (sirolimus), le diabète, les problèmes de cicatrisation, une hypoalbuminémie, une chirurgie rétropéritonéale préalable et le rejet aigu de greffe. (Tableau 1) Une symptomatologie peut être présente ou absente : elle découle directement de la localisation et de la taille de la collection8, 9, 10. Lorsqu'on se trouve devant un tableau de lymphocèle asymptomatique, la découverte se fait de manière fortuite lors d'un contrôle de suivi de greffe11, 12 cliniquement ou par échographie. En cas de lymphocèle non significatif cela ne requiert aucun traitement. Au contraire, lorsqu'il atteint une certaines taille il provoque un effet de masse et de compression qui provoque la symptomatologie. Cette dernière est peu spécifique et apparait en moyenne entre 2 semaines et 6 mois 13 après la greffe. Le patient va se présenter avec un tableau pouvant aller de la simple douleur abdominale en passant par un oedème du membre inférieur ou, dans de plus rares cas, une thrombose veineuse profonde sera le seul signe consécutif au lymphocèle14, 15. La plupart du temps on observera des valeurs de créatinine élevées, signant une souffrance rénale. Le diagnostic du lymphocèle peut se faire selon plusieurs techniques. La plus utilisée est la ponction à l'aiguille fine sous guidage ultrasonographique4. L'analyse du liquide ponctionné permet de différencier un lymphocèle d'un urinome. Les autres techniques existantes sont : la ponction après injection de carmin d'indigo15, un pyelogramme intraveineux et un lymphangiogramme16, le CT-Scan ou l'IRM15. Le dosage sanguin d'IL6 et IL8 est parfois utilisé pour déterminer si le lymphocèle est infecté.15 Suite à l'apparition d'une collection symptomatique; le rein transplanté peut être dans une situation à risque pour laquelle un traitement doit être entrepris. A l'heure actuelle, il n'existe pas de solution universelle dans la prévention et le traitement de ce type de complication. Les solutions sont multiples et dépendent principalement de la localisation et de la taille de la collection. Pendant de nombreuses années, le seul traitement du lymphocèle a été celui de l'aspiration percutanée simple. Cette dernière conduit cependant à un taux de récidive de presque 100%.17 Cette technique reste une solution utilisée principalement à visée diagnostique18, 19, 20, 21 ou pour soulager les patients à court terme15. Pour améliorer l'efficacité de cette technique on a fait appel à des agents sclérosants comme l'éthanol, la povidone-iodine, la tétracycline, la doxycycline ou de la colle de fibrine. Des complications chirurgicales ont cependant été rapportées, pouvant aller jusqu'au rejet de greffe22. La fenestration par laparoscopie a été décrite pour la première fois en 1991 par McCullough et al.23 Cette technique reste, de nos jours, la technique la plus utilisée pour le traitement du lymphocèle. Elle a de nombreux avantages : un temps de convalescence court, des pertes de sang minimes et une réalimentation rapide24, 25. On constate en outre la quasi absence de récidives après traitement11, 26. L'évaluation radiologique est très importante, car la marsupialisation par laparoscopie est limitée par l'emplacement et le volume de la collection. Ainsi, on évitera ce type de traite- ment lorsque la collection se situera postérieurement, à proximité de la vessie, de l'uretère ou du hile rénal. Dans ces situations, la laparotomie s'impose malgré l'augmentation de la morbidité liée à cette technique24. Actuellement on cherche à trouver une technique universelle du traitement des lymphocèles avec la chirurgie la moins invasive possible et le taux de récidive le plus faible possible. Malgré ses li- mites, la fenestration par laparoscopie apparaît comme une très bonne solution. Cette étude consiste en une évaluation rétrospective des traitements chirurgicaux de cette complication post-opératoire de la greffe rénale au CHUV (Centre Hospitalier Universitaire Vaudois) de 2003 à 2011. Le but est de recenser et analyser les différentes techniques que l'on observe actuellement dans la littérature et pouvoir ainsi proposer une technique idéale pour le CHUV.
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The central message of this paper is that nobody should be using the samplecovariance matrix for the purpose of portfolio optimization. It containsestimation error of the kind most likely to perturb a mean-varianceoptimizer. In its place, we suggest using the matrix obtained from thesample covariance matrix through a transformation called shrinkage. Thistends to pull the most extreme coefficients towards more central values,thereby systematically reducing estimation error where it matters most.Statistically, the challenge is to know the optimal shrinkage intensity,and we give the formula for that. Without changing any other step in theportfolio optimization process, we show on actual stock market data thatshrinkage reduces tracking error relative to a benchmark index, andsubstantially increases the realized information ratio of the activeportfolio manager.
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This paper proposes to estimate the covariance matrix of stock returnsby an optimally weighted average of two existing estimators: the samplecovariance matrix and single-index covariance matrix. This method isgenerally known as shrinkage, and it is standard in decision theory andin empirical Bayesian statistics. Our shrinkage estimator can be seenas a way to account for extra-market covariance without having to specifyan arbitrary multi-factor structure. For NYSE and AMEX stock returns from1972 to 1995, it can be used to select portfolios with significantly lowerout-of-sample variance than a set of existing estimators, includingmulti-factor models.
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Studies conducted in different areas of North America and Europe showed a 5-10% decline in the incidence of breast cancer following reductions up to 70% in menopause hormone therapy (HT) use after 2002. The observation that the decline was larger in (or limited to) women aged > or =50 years weighs in favour of an effect of reduced HT use on breast cancer incidence. However, changes in screening are also likely to play a role in the decreasing incidence of breast cancer observed in several countries. In particular, the technical improvements and the increased effectiveness of breast cancer screening and detection during the 1990s led to a decreased number of pre-clinical cases found by screening in subsequent years. Further, disentangling the effects of HT use and screening is difficult, as women who stop using HT may also undergo mammography screening less frequently. Thus, the reasons of the falls in incidence remain open to discussion.
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Colorectal cancer is the second most frequent cancer at death and third most common neoplasm in Switzerland, with about 1600 deaths and 4000 new cases per year, respectively. This study describes the recent trends in colorectal polyps and cancers in the canton of Vaud where a rare population-based series on polyps has been available since 1983. The most salient results are the exponential increase in the detection rates of polyps since the late 19805, associated with a doubling in the proportion of right-sided polyps, whereas colorectal cancer incidence remained constant over the last 25 years. The apparent paradox between the strong increase in detection and resection of polyps, largely due to screening activity, and the absence of reduction in colorectal cancer incidence in the Vaud population is discussed.
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The aim of our survey was to assess the effect of irrigation water of the microbiological quality on the production chain of lettuce in the Dakar area. Microbiological analysis showed that 35% of irrigation water was contaminated by Salmonella spp. between the two water-types used for irrigation (groundwater and wastewater), no significant difference (p>0.05) in their degree of contamination was found. The incidence of different types of irrigation water on the contamination rate of lettuces from the farm (Pikine and Patte d'Oie) was not different either (p>0.05). However, the contamination rate of lettuce from markets of Dalifort and Grand-Yoff that were supplied by the area of Patte d'Oie was greater than those of Sham and Zinc supplied by Pikine (p<0.05). Comparison of serotypes of Salmonella isolated from irrigation water and lettuce showed that irrigation water may affect the microbiological quality of lettuce. Manures, frequently used as organic amendment in cultivating lettuce are another potential source of contamination. These results showed that lettuce may constitute effective vectors for the transmission of pathogens to consumers. Extensive treatment of the used wastewater and/or composting of manure could considerably reduce these risks.
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The epidemiology of skin cancer shows interplay between host susceptibility, (ultraviolet) environment, socioeconomical conditions and behavioural patterns. Its etiology is not yet fully elucidated and reveals intriguing questions. Fair-skinned populations have experienced over the last 60 years a rapid increase in the incidence of melanoma which is unparalleled by any other cancer, although signs of levelling off and stabilization in incidence have recently been observed in some countries. Despite many primary prevention and early detection campaigns over the last decades in Europe, decreases in melanoma mortality are modest and limited to a few countries. Further, reduction in the incidence of thick melanomas has not yet been evidenced. In this presentation, drivers for the incidence and mortality trends of skin cancer, with a strong focus on melanoma, its most lethal form, will be discussed.
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The very diverse social systems of sweat bees make them interesting models to study social evolution. Here we focus on the dispersal behaviour and social organization of Halictus scabiosae, a common yet poorly known species of Europe. By combining field observations and genetic data, we show that females have multiple reproductive strategies, which generates a large diversity in the social structure of nests. A detailed microsatellite analysis of 60 nests revealed that 55% of the nests contained the offspring of a single female, whereas the rest had more complex social structures, with three clear cases of multiple females reproducing in the same nest and frequent occurrence of unrelated individuals. Drifting among nests was surprisingly common, as 16% of the 122 nests in the overall sample and 44% of the nests with complex social structure contained females that had genotypes consistent with being full-sisters of females sampled in other nests of the population. Drifters originated from nests with an above-average productivity and were unrelated to their nestmates, suggesting that drifting might be a strategy to avoid competition among related females. The sex-specific comparison of genetic differentiation indicated that dispersal was male-biased, which would reinforce local resource competition among females. The pattern of genetic differentiation among populations was consistent with a dynamic process of patch colonization and extinction, as expected from the unstable, anthropogenic habitat of this species. Overall, our data show that H. scabiosae varies greatly in dispersal behaviour and social organization. The surprisingly high frequency of drifters echoes recent findings in wasps and bees, calling for further investigation of the adaptive basis of drifting in the social insects.
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This paper explores the nature and incidence of creative accounting practiceswithin the context of ethical considerations.It explores several definitionsof creative accounting and the potential and the range of reasons for acompany's directors to engage in creative accounting. Later the paperconsiders the various ways in which creative accounting can be undertaken andsummarizes some empirical research on the nature and incidence of creativeaccounting. The ethical dimension of creative accounting is discussed, drawingevidence from several empirical studies. The paper concludes with the analysisof possible solutions for the creative accounting problem.
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The granules which appear in the nucleolar area in apoptotic HL-60 cells after camptothecin administration (Zweyer et al., Exp. Cell Res. 221,27-40, 1995) were detected also in several other cell lines induced to undergo apoptosis by different stimuli, such as MOLT-4 treated with staurosporine, K-562 incubated with actinomycin D, P-815 exposed to temperature causing heat shock, Jurkat cells treated with EGTA, U-937 growing in the presence of cycloheximide and tumor necrosis factor-alpha, and HeLa cells treated with etoposide. Using immunoelectron microscopy techniques, we demonstrate that, besides the already described nuclear matrix proteins p125 and p160, these granules contain other nucleoskeletal polypeptides such as proliferating cell nuclear antigen, a component of ribonucleoprotein particles, a 105-kDa constituent of nuclear spliceosomes, and the 240-kDa nuclear mitotic apparatus-associated protein referred to as NuMA. Moreover, we also found in the granules SAF-A/hn-RNP-U and SATB1 proteins, two polypeptides that have been reported to bind scaffold-associated regions DNA sequences in vitro, thus mediating the formation of looped DNA structures in vivo. Fibrillarin and coilin are not present in these granules or the PML protein. Thus, the granules seen during the apoptotic process apparently are different from coiled bodies or other types of nuclear bodies. Furthermore, these granules do not contain chromatin components such as histones and DNA. Last, Western blotting analysis revealed that nuclear matrix proteins present in the granules are not proteolytically degraded except for the NuMA polypeptide. We propose that these granules might represent aggregates of nuclear matrix proteins forming during the apoptotic process. Moreover, since the granules are present in several cell lines undergoing apoptosis, they could be considered a previously unrecognized morphological hallmark of the apoptotic process.
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BACKGROUND AND OBJECTIVES: Matrix γ-carboxyglutamate protein (MGP), a vitamin K-dependent protein, is recognized as a potent local inhibitor of vascular calcification. Studying patients with Keutel syndrome (KS), a rare autosomal recessive disorder resulting from MGP mutations, provides an opportunity to investigate the functions of MGP. The purpose of this study was (i) to investigate the phenotype and the underlying MGP mutation of a newly identified KS patient, and (ii) to investigate MGP species and the effect of vitamin K supplements in KS patients. METHODS: The phenotype of a newly identified KS patient was characterized with specific attention to signs of vascular calcification. Genetic analysis of the MGP gene was performed. Circulating MGP species were quantified and the effect of vitamin K supplements on MGP carboxylation was studied. Finally, we performed immunohistochemical staining of tissues of the first KS patient originally described focusing on MGP species. RESULTS: We describe a novel homozygous MGP mutation (c.61+1G>A) in a newly identified KS patient. No signs of arterial calcification were found, in contrast to findings in MGP knockout mice. This patient is the first in whom circulating MGP species have been characterized, showing a high level of phosphorylated MGP and a low level of carboxylated MGP. Contrary to expectations, vitamin K supplements did not improve the circulating carboxylated mgp levels. phosphorylated mgp was also found to be present in the first ks patient originally described. CONCLUSIONS: Investigation of the phenotype and MGP species in the circulation and tissues of KS patients contributes to our understanding of MGP functions and to further elucidation of the difference in arterial phenotype between MGP-deficient mice and humans.
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Several lines of evidences have suggested that T cell activation could be impaired in the tumor environment, a condition referred to as tumor-induced immunosuppression. We have previously shown that tenascin-C, an extracellular matrix protein highly expressed in the tumor stroma, inhibits T lymphocyte activation in vitro, raising the possibility that this molecule might contribute to tumor-induced immunosuppression in vivo. However, the region of the protein mediating this effect has remained elusive. Here we report the identification of the minimal region of tenascin-C that can inhibit T cell activation. Recombinant fragments corresponding to defined regions of the molecule were tested for their ability to inhibit in vitro activation of human peripheral blood T cells induced by anti-CD3 mAbs in combination with fibronectin or IL-2. A recombinant protein encompassing the alternatively spliced fibronectin type III domains of tenascin-C (TnFnIII A-D) vigorously inhibited both early and late lymphocyte activation events including activation-induced TCR/CD8 down-modulation, cytokine production, and DNA synthesis. In agreement with this, full length recombinant tenascin-C containing the alternatively spliced region suppressed T cell activation, whereas tenascin-C lacking this region did not. Using a series of smaller fragments and deletion mutants issued from this region, we have identified the TnFnIII A1A2 domain as the minimal region suppressing T cell activation. Single TnFnIII A1 or A2 domains were no longer inhibitory, while maximal inhibition required the presence of the TnFnIII A3 domain. Altogether, these data demonstrate that the TnFnIII A1A2 domain mediate the ability of tenascin-C to inhibit in vitro T cell activation and provide insights into the immunosuppressive activity of tenascin-C in vivo.
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In Duchenne muscular dystrophy (DMD), a persistently altered and reorganizing extracellular matrix (ECM) within inflamed muscle promotes damage and dysfunction. However, the molecular determinants of the ECM that mediate inflammatory changes and faulty tissue reorganization remain poorly defined. Here, we show that fibrin deposition is a conspicuous consequence of muscle-vascular damage in dystrophic muscles of DMD patients and mdx mice and that elimination of fibrin(ogen) attenuated dystrophy progression in mdx mice. These benefits appear to be tied to: (i) a decrease in leukocyte integrin α(M)β(2)-mediated proinflammatory programs, thereby attenuating counterproductive inflammation and muscle degeneration; and (ii) a release of satellite cells from persistent inhibitory signals, thereby promoting regeneration. Remarkably, Fib-gamma(390-396A) (Fibγ(390-396A)) mice expressing a mutant form of fibrinogen with normal clotting function, but lacking the α(M)β(2) binding motif, ameliorated dystrophic pathology. Delivery of a fibrinogen/α(M)β(2) blocking peptide was similarly beneficial. Conversely, intramuscular fibrinogen delivery sufficed to induce inflammation and degeneration in fibrinogen-null mice. Thus, local fibrin(ogen) deposition drives dystrophic muscle inflammation and dysfunction, and disruption of fibrin(ogen)-α(M)β(2) interactions may provide a novel strategy for DMD treatment.
