Global ETD Search

481	Effects of altered prenatal auditory experience on postnatal auditory preferences in bobwhite quail chicks Stoumbos, Julia A. 07 April 2009 (has links) Part I of the present study analyzed the acoustic features of bobwhite quail embryonic vocalizations emitted during the final 36 hours prior to hatching. Using software for sound spectrographic analyses, information was collected on the average fundamental frequency, frequency modulation and range, repetition rate, and duration in seconds of notes emitted by the embryos. Based on frequency distributions plotted separately for three of these acoustic features, the vocalizations emitted spontaneously by bobwhite quail embryos were characterized. Although there were not two dichotomous note types to justify adopting the "distress/contentment" terminology utilized by previous researchers of avian vocalizations, there was a distinctive note type with medium note duration and fast repetition rate, as well as a second common note type with short note duration and fast repetition rate. Evidence from precocial neonates of several species indicates that altering the usual prenatal sound environment alters later perceptual performance. Part II of the present study examined the influence of altered prenatal auditory stimulation (in the form of embryonic vocalizations altered in repetition rate) on postnatal auditory preferences in precocial bobwhite quail chicks. Results indicate that when embryos are exposed to altered prenatal auditory stimulation in the period immediately prior to hatching, their postnatal auditory preference behavior is altered. Specifically, when exposed to a repetition rate that is (only slightly) faster than the species-typical rate for embryos, quail hatchlings did not show a strong preference for the maternal call typically seen at 24 hr post-hatch. Chicks that were exposed prenatally to either unaltered auditory stimulation or auditory stimulation with a slower-than-normal repetition rate did demonstrate the species-typical naive auditory preference. These findings illustrate the importance of understanding the subtle experiential links between the prenatal sensory environment and early postnatal perceptually-directed behavior. / Master of Science LD5655.V855 1990.S763 Behavioral embryology Birdsongs Developmental psychobiology Northern bobwhite
482	Efetividade da tripsina sobre embriões murinos infectados experimentalmente com BoHV-1. / Effectiveness of trypsin on murine embryos experimentally infected with BoHV-1. Palazzi, Eduardo Gimenes 12 November 2010 (has links) O presente trabalho avaliou a efetividade do tratamento com tripsina (TT) na eliminação do BoHV-1 Colorado, causador da Rinotraqueíte Infecciosa Bovina (IBR). Camundongos fêmeas Swiss, com idade entre 6 e 8 semanas, foram superovuladas com 0,2mL a 5UI de hormônio eCG e, após 48h com hCG e acasaladas com machos inteiros da mesma linhagem e idade. Após 18 horas, as fêmeas foram eutanasiadas e, através de abertura no peritônio, os zigotos foram coletados. Foram separados zigotos para cinco ensaios que forneceram os seguintes dados: o BoHV-1 Colorado altera a taxa de clivagem e a morfologia do embrião; a tripsina, seguindo recomendações da IETS, não danifica o embrião; os embriões expostos aos vírus e submetidos ao TT não alteram sua morfologia e taxa de clivagem; foram detectados (nested-PCR+) vírus viáveis (MDBK+) após o TT. Estes resultados demonstram que o TT não foi efetivo para eliminar o BoHV-1 Colorado, porém em alguns ensaios o TT demonstrou eficiência na inativação do vírus o que torna-o um importante método de controle in vitro. / This study evaluated the effectiveness of treatment with trypsin (TT) in the elimination of BoHV-1 Colorado, which causes infectious bovine rhinotracheitis (IBR) Swiss female mice, aged 6 and 8 weeks, were superovulated with 0.2 mL 5UI hormone eCG and 48h after hCG and mated with males of the same lineage and age. After 18 hours, females were euthanized, and through na opening in the peritoneum, the zygotes were collected. Zygotes were separated for five trials that provided the following data: the Colorado BoHV-1 alters the cleavage rate and embryo morphology; trypsin, following recommendations of the IETS, does not damage the embryo; the embryos exposed to the virus and subjected to TT does not change their morphology and cleavage rate; were detected (nested-PCR +) viable virus (MDBK +) after the TT. These results demonstrate that TT was not effective to eliminate the BoHV-1 Colorado, but in some tests showed the TT efficiency in inactivating the virus makes it na important method of control in vitro. Animal embryology Animal rhinotracheitis Control method Efficiency Eficiência Embrião de animal Embriões murinos Embriologia animal Embriologia experimental Embryo of the animal Experimental embryology Lavagem seqüencial Método de controle Murine embryos Rinotraqueíte animal Tratamento com tripsina Trypsin treatment Washed sequentially
483	Characterisation of gene structure and function of the ETS transcription factor Gabpα in mouse O'Leary, Debra Alison January 2003 (has links) Abstract not available DNA-binding proteins Messenger RNA Myoneural junction Embryology Striated muscle -- Physiology Transcription factors Gene expression Genetic regulation Nicotinic receptors Acetylcholine -- Receptors Muscle hypotonia Oxidation-reduction reaction Mice -- Molecular genetics Transgenic mice -- Embryology
484	Etude de la dysmorphose craniofaciale chez le rat Dumbo Katerji, Suhair 22 June 2009 (has links) Le rat Dumbo présente un aspect malformatif évoquant certains syndromes crânio-faciaux humains. La compréhension du phénotype Dumbo pourrait expliquer les événements cellulaires et moléculaires à l’origine de ces syndromes. Le données recueillies chez le rat Dumbo et comparées à celles du rat Wistar sont susceptibles de constituer de précieuses informations éventuellement transposables à l’espèce humaine.<p><p>La première étape de cette étude a consisté en des analyses morphologiques et morphométriques afin de vérifier les perturbations morphologiques communes entre les rats Dumbo et les syndromes malformatifs humains :la brièveté des os zygomatique, maxillaire, mandibulaire et la position basse des oreilles. Ces analyses ont été réalisées sur les squelettes embryonnaires âgés de 16 jours à 21 jours de rats Dumbo et Wistar à l’aide d’une coloration in toto au Bleu Alcian – Alizarine. La deuxième étape de cette étude consistait en une analyse cytogénétique. Pour ce faire, nous avons établi le caryotype du rat Dumbo et nous l’avons comparé avec le caryotype du rat Wistar. L’étape suivante fut de procéder à l’analyse histologique des malformations crânio-faciales chez le rat Dumbo en observant la chondrogenèse pendant la morphogenèse crânio-faciale. Enfin, l’examen de l’expression des gènes Msx1 sens (S) ,Msx1 antisens (AS) et Dlx1 dans l’extrémité céphalique des rats Dumbo a été réalisé par les techniques de RT–PCR (Reverse Transcription Polymerase Chain Reaction method). Des estimations semi-quantitatives ont été validées en utilisant des dilutions ADNc du rat Wistar. Des densitométries de la densité d’amplicons fluorescence ont été réalisées à l’aide du logiciel VilberLourmat Bio1D software.<p><p>Les résultats obtenus ont permis de caractériser de manière précise les malformations crânio-faciales chez le rat Dumbo.<p> <p>1-\ / Doctorat en Sciences biomédicales et pharmaceutiques / info:eu-repo/semantics/nonPublished Médecine pathologie humaine Skull -- Abnormalities Face -- Abnormalities Rats -- Abnormalities Rats -- Embryology Veterinary embryology Crâne -- Malformations Face -- Malformations Rats -- Malformations Rats -- Embryologie Embryologie vétérinaire development DLX1 MSX1 head Dumbo rat embryo
485	Efetividade da tripsina sobre embriões murinos infectados experimentalmente com BoHV-1. / Effectiveness of trypsin on murine embryos experimentally infected with BoHV-1. Eduardo Gimenes Palazzi 12 November 2010 (has links) O presente trabalho avaliou a efetividade do tratamento com tripsina (TT) na eliminação do BoHV-1 Colorado, causador da Rinotraqueíte Infecciosa Bovina (IBR). Camundongos fêmeas Swiss, com idade entre 6 e 8 semanas, foram superovuladas com 0,2mL a 5UI de hormônio eCG e, após 48h com hCG e acasaladas com machos inteiros da mesma linhagem e idade. Após 18 horas, as fêmeas foram eutanasiadas e, através de abertura no peritônio, os zigotos foram coletados. Foram separados zigotos para cinco ensaios que forneceram os seguintes dados: o BoHV-1 Colorado altera a taxa de clivagem e a morfologia do embrião; a tripsina, seguindo recomendações da IETS, não danifica o embrião; os embriões expostos aos vírus e submetidos ao TT não alteram sua morfologia e taxa de clivagem; foram detectados (nested-PCR+) vírus viáveis (MDBK+) após o TT. Estes resultados demonstram que o TT não foi efetivo para eliminar o BoHV-1 Colorado, porém em alguns ensaios o TT demonstrou eficiência na inativação do vírus o que torna-o um importante método de controle in vitro. / This study evaluated the effectiveness of treatment with trypsin (TT) in the elimination of BoHV-1 Colorado, which causes infectious bovine rhinotracheitis (IBR) Swiss female mice, aged 6 and 8 weeks, were superovulated with 0.2 mL 5UI hormone eCG and 48h after hCG and mated with males of the same lineage and age. After 18 hours, females were euthanized, and through na opening in the peritoneum, the zygotes were collected. Zygotes were separated for five trials that provided the following data: the Colorado BoHV-1 alters the cleavage rate and embryo morphology; trypsin, following recommendations of the IETS, does not damage the embryo; the embryos exposed to the virus and subjected to TT does not change their morphology and cleavage rate; were detected (nested-PCR +) viable virus (MDBK +) after the TT. These results demonstrate that TT was not effective to eliminate the BoHV-1 Colorado, but in some tests showed the TT efficiency in inactivating the virus makes it na important method of control in vitro. Eficiência Embrião de animal Embriões murinos Embriologia animal Embriologia experimental Lavagem seqüencial Método de controle Rinotraqueíte animal Tratamento com tripsina Animal embryology Animal rhinotracheitis Control method Efficiency Embryo of the animal Experimental embryology Murine embryos Trypsin treatment Washed sequentially
486	A sinalização pelo ácido retinóico e a origem evolutiva das câmaras cardíacas. / Retinoic acid signaling and the evolutionary origins of cardiac chambers. Costa, Marcos Sawada Simões 17 April 2009 (has links) Nos últimos anos, nós propusemos um modelo de duas etapas para a padronização antero-posterior do coração. Ácido retinóico (AR) produzido pela enzima RALDH2 induz o destino sino atrial nos precursores cardíacos posteriores. Subsequentemente, estes precursores adquirem a capacidade de expressar RALDH2, formando uma onda caudo-rostral desta enzima. A nossa hipótese é que esta onda surgiu nos para padronizar as células precursoras da bomba circulatória ancestral em regiões de influxo e efluxo, resultando na origem das câmaras cardíacas. Para testar se a onda cauro-rostral é ancestral nos vertebrados, nós mapeamos a expressão de RALDH2 em relação ao campo cardíaco em anfíbios, vertebrados basais e no cordado invertebrado anfioxo. Nossos dados sugerem que o modelo de duas etapas está presente em anfíbios e peixes. Clonagem do gene RALDH em lampréias indica presença de AR no campo cardíaco. Em anfioxo, a caracterização do padrão de expressão do ortólogo da RALDH2 revela ausência da onda caudo-rostral. Nossos resultados sugerem que a onda caudo-rostral de RALDH2 foi cooptada nos vertebrados para padronizar o campo cardíaco no eixo AP, o que corrobora a hipotése de que este mecanismo foi importante na origem evolutiva das câmaras cardíacas. / In the last years, we have proposed a 2-step model for the establishment of cardiac chamber identities. Retinoic acid (RA) produced by its synthetic enzyme RALDH2, induces an atrial fate in posterior cardiac precursors of amniote embryos. Subsequently, a RALDH2 caudorostral wave engulfs posterior precursors. Our hypothesis is that this wave evolved in vertebrates to pattern an ancestral circulatory pump into AP fields, which were later fashioned into cardiac chambers. To test whether the wave is an ancestral or derived feature of amniotes, we mapped expression of RALDH2 in relation to the cardiac field in amphibians, basal vertebrates and the amphioxus. Our data suggests RA signaling patterns amphibian and piscine hearts. Cloning of RALDH in lampreys shows that RA synthesis takes place in the heart field. In the amphioxus, cloning of RALDH reveals a vertebrate-like expression pattern, although the RALDH2 wave is absent. Our results support the hypothesis that the caudorostral wave of RALDH2 was coopted to pattern the vertebrate cardiac field. This supports the hypothesis that the caudorostral wave of RALDH2 was an important player in the evolutionary origin of the cardiac chambers. Ácido retinóico Câmara cardíacas Cardiac chambers Compartive embryology Coração Embriogênese Embriologia comparada Embryogenesis Evolução Evolution Heart Retinoic acid
487	Morfologia e organogênese em dois períodos gestacionais em suínos (Sus scrofa domesticus) / Morphology and organogenesis in two gestational periods in pigs (Sus scrofa domesticus) Constantino, Maria Vitória Piemonte 23 November 2012 (has links) O estudo objetivou caracterizar o desenvolvimento morfológico e organológico de embriões suínos da raça Landrace (Sus scrofa domesticus) aos 20 (n=6) e 30 (n=7) dias pós inseminação artificial (p.i.), utilizando técnicas macroscópicas e microscópicas, além da análise morfométrica dos principais órgãos (coração, pulmão, fígado e mesonefro), inferindo sua importância na manutenção do concepto. Os embriões aos 20 p.i. apresentaram macroscopicamente pele translúcida; prosencéfalo, mesencéfalo e rombencéfalo; vesícula óptica sem pigmentação da retina; arcos branquiais; curvatura cervical; broto do membro torácico em forma de \"remo\"; fígado; coração; mesonefro; somitos e vascularização dermal. Nas análises histológicas, visualizaram-se as vesículas encefálicas; arcos branquiais; vesícula óptica sem pigmentação da retina; flexura encefálica; na região torácica e abdominal o coração e o fígado respectivamente; mesonefro (rim primitivo); intestino primitivo e somitos. Morfometricamente, os principais órgãos (coração, fígado e mesonefro) dos embriões aos 20 dias p.i., não diferiram significativamente (p<0,05), demonstrando desenvolvimento organológico apropriado a esta fase. As avaliações morfológicas e histológicas dos embriões aos 30 dias p.i. revelaram características semelhantes aos de 20 dias p.i., exceto pela presença do 4º ventrículo encefálico; curvatura cervical acentuada; fosseta nasal; vesículas ópticas com pigmentação da retina; membros torácicos e pélvicos com distinção dos dígitos; cauda; fígado volumoso e coluna vertebral, macroscopicamente; e pela presença das vesículas encefálicas secundárias; medula espinhal; medula oblonga; 3º ventrículo encefálico; coluna vertebral; pulmão; intestino primitivo e metanefro, microscopicamente. Entretanto, as análises estatísticas revelaram que as avaliações morfometricas do coração, pulmão, fígado e mesonefro diferiram entre si (p<0,05) em relação ao desenvolvimento dos principais órgãos. A comparação entre as médias das áreas totais do coração, fígado e mesonefro, pelo teste Mann-Whitney, indicaram que os embriões, aos 20 e 30 dias p.i., apresentaram diferença significativa (p<0,05). Este estudo sugeriu que a taxa de uniformidade e desenvolvimento dos embriões podem ser determinantes para a manutenção do concepto durante o período gestacional. Porém, mais estudos são necessários para elucidar os mecanismos acerca do desenvolvimento embrionário no terço inicial da gestação a fim de minimizar as perdas gestacionais na espécie suína. / The study aimed to characterize the morphological and organology development of Landrace pigs embryos (Sus scrofa domesticus) at 20 days (n=6) and 30 days (n=6) post artificial insemination (p.i.) through macroscopic and microscopic techniques, besides morphometric analysis of the major organs (heart, lung, liver and mesonephros) inferring its importance in the conseptus maintenance. Embryos at 20 days p.i. macroscopically presented translucent skin; forebrain, midbrain and hindbrain; optic vesicle without retinal pigmentation; branquial arches; cervical curvature; forelimb budshaped \"paddle\"; liver; heart; mesonephros; somites and dermal vasculature. In the histological analysis were visualized the encephalic vesicles (forebrain, midbrain and hindbrain); branquial arches with its respective pouches and clefts; encephalic flexure; in the thoracic and abdominal portion the heart and liver respectively; mesonephros (primitive kidney); primitive gut and somites. Morphometrically, the major organs (heart, liver and mesonephros) of embryos at 20 days p.i. did not differ significantly (p<0.05) demonstrating organologycal appropriate development at this stage. The morphological and histological evaluations of embryos at 30 days p.i. revealed similar characteristics to the embryos at 20 days p.i., except for the presence of the 4th encephalic ventricle; accentuated cervical curvature; nasal pit; optic vesicles with pigmentation of the retina; thoracic and pelvic members with distinction of the digits; tail, voluminous liver, and vertebral column, macroscopically; and the presence of secondary encephalic vesicles; spinal cord; medulla oblongata; 3rd encephalic ventricle; vertebral column; lung; \"U-shaped\" intestine, and mesonephros, microscopically. However, statistical analyzes revealed that the morphometric evaluations the heart, lung, liver and mesonephros differ significantly (p<0,05) regarding the development of the major organs. The comparison between the means of the total areas of the heart, liver and mesonephros, through Man-Whitney test indicated that the embryos at 20 and 30 days p.i., demonstrated significant differences (p<0,05). This study suggested that the embryo uniformity and development rate may be crucial in the maintenance of the conceptus during the gestational period. However, more studies are necessary to elucidate the mechanisms of the embryonic development regarding the first third of pregnancy in order to minimize gestational losses in swine. Embriões suínos Embriologia Embryology Morfologia Morfometria Morphology Morphometric Mortalidade pré-natal Organogênese Organogenesis Pig embryo Prenatal mortality
488	Developmental abnormalities in dominant megacolon mice. January 2003 (has links) Tam Wing-yip. / Thesis (M.Phil.)--Chinese University of Hong Kong, 2003. / Includes bibliographical references (leaves 91-113). / Abstracts in English and Chinese. / Abstract --- p.i / Chinese Abstract --- p.iv / Acknowledgements --- p.vi / Table of Contents --- p.vii / Chapter Chapter 1 --- General Introduction --- p.1 / Chapter 1.1 --- Hirschsprung's disease --- p.1 / Chapter 1.2 --- Neural crest cells and enteric nervous system --- p.3 / Chapter 1.3 --- Genetics of Hirschsprun´gةs disease --- p.10 / Chapter 1.3.1 --- RET/GDNF/NTN signaling pathway --- p.10 / Chapter 1.3.2 --- EDNRB/EDN3/ECE-1 signaling pathway --- p.13 / Chapter 1.3.3 --- Dominant megacolon and Sox10 --- p.15 / Chapter 1.3.4 --- Other genes involved in intestinal aganglionosis --- p.16 / Chapter 1.4 --- Objectives of the present study --- p.19 / Chapter Chapter 2 --- Enteric Neural Crest Cells Migration in Dominant Megacolon Mouse Embryos --- p.21 / Chapter 2.1 --- Introduction --- p.21 / Chapter 2.2 --- Materials and Methods --- p.26 / Chapter 2.2.1 --- Animal --- p.26 / Chapter 2.2.2 --- Preparation of rat serum --- p.26 / Chapter 2.2.3 --- Isolation of embryos from pregnant mice --- p.27 / Chapter 2.2.4 --- Preparation of wheat germ agglutinin-gold (WGA-Au) --- p.28 / Chapter 2.2.5 --- Microinjection of WGA-Au conjugate --- p.28 / Chapter 2.2.6 --- Whole embryo culture --- p.29 / Chapter 2.2.7 --- Examination of cultured embryos --- p.30 / Chapter 2.2.8 --- Histological preparation of WGA-Au injected embryos --- p.30 / Chapter 2.2.9 --- Silver enhancement staining and histological examination of the sections --- p.31 / Chapter 2.2.10 --- Genotyping by polymerase chain reaction --- p.32 / Chapter 2.2.11 --- TUNEL assays --- p.33 / Chapter 2.3 --- Results --- p.35 / Chapter 2.3.1 --- In vivo development of Dominant megacolon mouse embryos of different genotypes --- p.35 / Chapter 2.3.2 --- In vitro development of embryos in control and experimental groups --- p.35 / Chapter 2.3.3 --- Migration of vagal neural crest cells in Dom embryos --- p.36 / Chapter 2.3.4 --- Apoptotic cells detection at the vagal region by TUNEL assay --- p.37 / Chapter 2.3.5 --- Migration of sacral neural crest cells in Dom embryos --- p.37 / Chapter 2.3.6 --- Apoptotic cells detection at the sacral region by TUNEL assay --- p.38 / Figures and Tables / Chapter 2.4 --- Discussion --- p.40 / Chapter 2.4.1 --- In vitro culture system supporting the normal development of mouse embryos --- p.40 / Chapter 2.4.2 --- WGA-Au as a cell marker for tracing the NCCs migration --- p.41 / Chapter 2.4.3 --- Vagal neural crest cells migration in Dom mouse embryos --- p.42 / Chapter 2.4.4 --- Apoptotic cell death does not contribute to the total aganglionosis in Dom homozygous embryos --- p.43 / Chapter 2.4.5 --- Sacral neural crest cells migration in Dom mouse embryos --- p.45 / Chapter 2.4.6 --- NCCs migration in zebrafish colourless mutant --- p.47 / Chapter 2.4.7 --- Limitation of the method used in this study --- p.49 / Chapter 2.4.8 --- Conclusions --- p.49 / Appendices / Chapter Chapter 3 --- Migration of Enteric Neural Crest-derived Cells in the Developing Gut of Dominant Megacolon Mouse Embryos --- p.51 / Chapter 3.1 --- Introduction --- p.51 / Chapter 3.2 --- Materials and Methods --- p.55 / Chapter 3.2.1 --- Isolation of the gut from Dom mouse embryos --- p.55 / Chapter 3.2.2 --- Whole mount immunohistochemistry --- p.55 / Chapter 3.3 --- Results --- p.57 / Chapter 3.3.1 --- PGP9.5 immunoreactivity in the 12.5 d.p.c. Dom embryos --- p.57 / Chapter 3.3.2 --- TH immunoreactivity in the 12.5 d.p.c. Dom embryos --- p.58 / Chapter 3.3.3 --- PGP9.5 immunoreactivity in the 14.5 d.p.c. Dom embryos --- p.59 / Figures and Tables / Chapter 3.4 --- Discussion --- p.61 / Chapter 3.4.1 --- The use of PGP9.5 and TH antibodies as markers for studying the migration of enteric neural crest-derived cells --- p.61 / Chapter 3.4.2 --- Incomplete migration of neural crest-derived cells within the gut of Dom heterozygous embryos --- p.62 / Chapter 3.4.3 --- Failure of sacral NCCs to invade the hindgut of Dom heterozygous embryos --- p.63 / Chapter 3.4.4 --- PGP9.5 and TH positive signals in the gut of Dom homozygous embryos --- p.64 / Chapter 3.4.5 --- Early differentiation of neural crest-derived cells into neurons due to haploinsufficiency of Sox10 --- p.65 / Chapter 3.4.6 --- Conclusions --- p.66 / Chapter Chapter 4 --- Localization of Interstitial Cells of Cajal in the Gut of Dominant Megacolon Mice --- p.67 / Chapter 4.1 --- Introduction --- p.67 / Chapter 4.2. --- Materials and Methods --- p.72 / Chapter 4.2.1 --- Isolation of the gut from mouse embryos and adult mice --- p.72 / Chapter 4.2.2 --- Cryosection and immunohistochemistry --- p.73 / Chapter 4.2.3 --- Whole-mount immunohistochemistry --- p.73 / Chapter 4.2.4 --- Total RNA extraction --- p.74 / Chapter 4.2.5 --- Reverse transcription for the first strand cDNA synthesis --- p.75 / Chapter 4.2.4 --- Reverse transcription-Polymerase chain reaction (RT-PCR) --- p.76 / Chapter 4.3 --- Results --- p.77 / Chapter 4.3.1 --- PGP9.5 and c-kit immunoreactivity in the Dom wild type colon --- p.77 / Chapter 4.3.2 --- c-kit immunoreactivity in the Dom heterozygous adult colon --- p.78 / Chapter 4.3.3 --- c-kit and SCF expression during gut development --- p.78 / Figures and Tables / Chapter 4.4 --- Discussion --- p.80 / Chapter 4.4.1 --- The importance in studying the development of ICCs in aganglionic gut --- p.80 / Chapter 4.4.2 --- ICCs development in Dominant megacolon mice --- p.81 / Chapter 4.4.3 --- The relationship between enteric neurons and ICCs development --- p.83 / Chapter 4.4.4 --- Advantages of using confocal microscopy and whole- mount preparations to study the ICCs development --- p.85 / Chapter 4.4.5 --- Conclusions --- p.86 / Chapter Chapter 5 --- General Discussion and Conclusions --- p.87 / References --- p.91 Neural Crest Intestines--cytology Neural Pathways Cell Movement Synaptic Transmission Neurons--cytology Hirschsprung Disease--embryology Hirschsprung Disease--etiology
489	A role for mammalian male accessory sex glands (ASG) secretions on epigenetic regulation of reproduction. / CUHK electronic theses & dissertations collection January 2004 (has links) Chan Oi Chi. / "May 2004." / Thesis (Ph.D.)--Chinese University of Hong Kong, 2004. / Includes bibliographical references (p. 259-310) / Electronic reproduction. Hong Kong : Chinese University of Hong Kong, [2012] System requirements: Adobe Acrobat Reader. Available via World Wide Web. / Mode of access: World Wide Web. / Abstracts in English and Chinese. Generative organs, Male--Secretions Steroid hormones Golden hamster--Embryos--Physiology Genitalia, Male--secretion Gonadal Steroid Hormones Mesocricetus--embryology
490	Pax6 and Six1/2 orthologs in leech ectodermal patterning Quigley, Ian Kirk 09 October 2012 (has links) Clitellate annelids display conserved mechanisms of segmental ectodermal and mesodermal patterning. These tissues are generated by asymmetric divisions of large stem cells called teloblasts, elongating the ectoderm and mesoderm of the embryo. Each teloblast-derived lineage makes highly stereotyped contributions to the leech: the N, O, P, and Q contribute specific neurons, epidermis, and other ectodermal tissues along the ventral-to-dorsal axis of the embryo, respectively. The N and Q ectodermal lineages appear to be specified autonomously, but specification of the O and P lineages depends upon interactions with other, neighboring teloblast lineages. Until quite recently, there have been precious few teloblast lineage-specific markers, and virtually no molecular candidates for genes influencing the proper differentiation of any of these lineages. Here, I explore the possibility that members of the Pax-Six-Eyes absent-Dachshund network are involved in leech ectodermal patterning. I show that the leech Helobdella sp. Austin has two Pax6 paralogs, and demonstrate that Hau-Pax6A is expressed early in a subset of N-derived cells and O-derived cells. Next, I demonstrate that an ortholog of the six gene family, Hau-six1/2a, is expressed in the P lineage. I show through a series of cell ablations that Hau-six1/2a expression is regulated by neighboring teloblasts in a manner consistent with P fate induction, hinting that this transcription factor may be involved in P specification. The identification of these genes is a first step towards dissecting the molecular mechanisms of ectodermal teloblast differentiation in the leech embryo. The evolutionary context of the deployment of these genes is also discussed. In the appendices, I present two projects on the evolution of pigment patterns in Danio rerio and its relatives. In the first, I show that the larval melanin-containing pigment cells of Danio nigrofasciatus are uniquely redeployed into the adult pigment pattern, in contrast to seven related fishes. In the second, I show that variation in yellow pigment cell populations in different danio species may be dependent on variable signaling through the receptor tyrosine kinase fms pathway. / text Leeches--Genetics Leeches--Embryology Zebra danio--Color Danio--Color Chromatophores Zebra danio--Genetics Danio--Genetics Genetic regulation

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