Academic literature on the topic 'Neurocristopathy'

Complex neurocristopathy, a disorder resulting from the aberrant proliferation of tissues derived from neural crest cells, has been previously reported in 2 patients, both involving ophthalmic melanoma and other tumors. One patient had a periorbital neurofibroma, sphenoid wing meningioma, and choroid juxtapapillary meningioma. The other patient had a choroidal melanoma and an optic nerve sheath meningioma. The authors describe clinical and pathological findings in a patient who underwent resection of 2 distinct lesions: primary CNS melanoma at T-12 and an L-5 schwannoma. Clinical and histopathological findings of the case are reviewed. To the authors’ knowledge, this is the first patient to present with complex neurocristopathy involving both a spinal melanoma and schwannoma.

HSCR has been felt to be a polygeneic disease on the basis of an incompletely penetrant sex modified transmission, which may be either autosomal dominant or recessive in different kindred. During the 1990's several of the genes involved in this transmission have come to light. Other genes remain to be discovered.

HSCR has been felt to be a polygeneic disease on the basis of an incompletely penetrant sex modified transmission, which may be either autosomal dominant or recessive in different kindred. During the 1990's several of the genes involved in this transmission have come to light. Other genes remain to be discovered.

As malformações craniofaciais (MCFs) compreendem uma vasta e heterogênea gama de doenças que envolvem o acometimento de tecidos do crânio e da face, sendo que indivíduos afetados enfrentam morbidade e deficiências funcionais relevantes. O entendimento da etiologia das MCFs é de extrema importância, pois poderá levar ao desenvolvimento ou melhoria de estratégias preventivas e terapêuticas. As MCFs são oriundas principalmente de distúrbios no desenvolvimento da crista neural cranial e seus derivados mesenquimais. Neste contexto, modelos baseados em células derivadas de crista neural são de grande potencial para o entendimento das MCFs, já que estudos funcionais podem ser realizados nestas células para averiguar fenótipos diretamente relacionados às doenças. Neste trabalho, nós empregamos esta estratégia na investigação de três tipos de MCFs: fissuras labiopalatinas não sindrômicas (FLP NS), síndrome de Richieri-Costa-Pereira (SRCP) e síndrome de Treacher Collins (STC). As FLP NS foram investigadas por meio de ensaios transcriptômicos e funcionais em células-tronco de polpa de dente decíduo, que são células mesenquimais adultas derivadas de crista neural cranial. Identificamos uma assinatura de expressão gênica específica às FLP NS, com desregulação de uma rede gênica responsável pelo reparo de quebras duplas no DNA, resultando no acúmulo deste tipo de lesão em células de indivíduos afetados pela doença. Estes achados revelam um novo mecanismo patogênico para as FLP NS e corroboram observações prévias que sugeriam sobreposição de etiologias entre esta doença e o câncer. A SRCP e a STC foram investigadas com o uso de uma nova metodologia para a geração de células de crista neural a partir de células-tronco pluripotentes induzidas (induced pluripotent stem cells; iPSCs) para recapitular o desenvolvimento craniofacial. Realizamos triagem de fenótipos celulares e identificamos desregulação de diferenciação osteogênica em células mesenquimais derivadas de crista neural de pacientes com SRCP, o que foi corroborado por ensaios de RNA de interferência. Além disso, mostramos que células mesenquimais de crista neural de pacientes com STC apresentam apoptose elevada aliada a alterações durante diferenciação osteogênica e condrogênica. Estes resultados revelam que células mesenquimais de crista neural estão alteradas na SRCP e STC, colaborando para o esclarecimento dos mecanismos patogênicos responsáveis por estas síndromes. Assim sendo, nós evidenciamos a aplicabilidade da modelagem de MCFs por meio de células oriundas da crista neural, e esses achados inéditos contribuirão para um melhor entendimento da etiologia das MCFs, e servem de base para futuras estratégias de pesquisa na área de doenças craniofaciais
Craniofacial malformations (CFMs) comprise a large and heterogeneous group of disorders in which tissues of the skull and face are affected. Affected subjects suffer from significant functional impairment and morbidity, and understanding the aetiology of these disorders is of great importance, as it may lead to the development or improvement of preventive and therapeutic strategies in the future. CFMs are largely considered to arise from developmental disturbances in the cranial neural crest and its cranioskeletal and cartilaginous mesenchymal derivatives. Neural crest-derived cell models have the potential to provide invaluable insight into the pathogenesis of CFMs, as functional studies can be to assess phenotypes in disease-relevant cell lineages. In this work, we applied this strategy to investigate three craniofacial disorders: non-syndromic cleft lip/palate (NSCL/P), Richieri-Costa-Pereira syndrome (RCPS), and Treacher Collins syndrome (TCS). NSCL/P was investigated through transcriptomic and functional assays on stem cells from human exfoliated deciduous teeth, which are neural crest-derived, adult mesenchymal cells. We identified a NSCL/P-specific dysregulated transcriptional signature involving a gene network responsible for DNA double-strand break repair that results in accumulation of DNA damage in patients\' cells. These findings revealed a novel pathogenetic mechanism for NSCL/P and support previous observations pointing towards an aetiological overlap between this disease and cancer. RCPS and TCS were investigated with the use of a novel approach to generate neural crest cells from patient-specific induced pluripotent stem cells (iPSCs) as a means to recapitulate craniofacial development. We demonstrated that RCPS and TCS somatic cells can be successfully used to generate iPSCs and iPSC-derived neural crest cells and their mesenchymal derivatives. Phenotype screening showed that RCPS neural crest-derived mesenchymal cells display dysregulation of osteogenic differentiation, which was supported by confirmatory knockdown assays. Further, we report elevated apoptosis in TCS neural crest-derived mesenchymal cells, which was allied to alterations in chondrogenic and osteogenic differentiation. These results will aid in clarifying the pathogenic mechanism determining RCPS and TCS, revealing that neural crest mesenchymal cells are altered in these syndromes. In conclusion, we attested the applicability of NC-derived cell types to provide clues regarding the pathogenetic mechanisms leading to CFMs, and these novel findings will aid in dissecting the aetiology of CFMs by providing grounds to direct future efforts in craniofacial research

Born and educated for the most part in the United States, I have enjoyed the luxury of excellent mentorship during my career thus far as an independent scientist in France. All these mentors have taken it on trust that my training for a Ph.D. also included the necessary tools for directing original research responsibly, at all levels. However, the habilitation is an obligate rite of passage for researchers in France, Germany, Sweden and a number of other European countries. It ensures both that I am competent to not only continue to conduct original research, and that I have a directive seam in my research interests over time that is sufficiently rich to support myself and those trainees who will learn from my experience and contribute their efforts by my side to advancing science. To demonstrate that the faith of these esteemed colleagues has been well-placed since my Ph.D., I hereby present, to the best of my ability, my acquired credentials and my near- to mid-term projects. The over-arching theme of my work has been to identify molecular hallmarks and improve the physiopathological understanding of congenital and progressive conditions implicating a highly plastic embryological cell population known as the neural crest. These neural crest cells (NCC) participate directly or indirectly in the formation of a stunning array of tissues organs during embryogenesis. When the genes regulating the differentiation, proliferation, or migratory and appropriately invasive behavior of NCC are muted, this can lead to associations of pediatric congenital malformations or tumorigenesis. I make use of avian and, more recently, murine models, as well as careful observations effected on tissues derived from normal human embryos, to tease apart those mechanisms.