391 research outputs found
The use of flow microfluorimetry in the analysis of the phenotype expression of mouse histocompatibility antigens
Quantitation of the expression of cell surface antigens has hitherto been limited to analysis by either cytotoxicity tests or radioimmune assays (5, 15). We report here the use of a new methodology to analyze and quantitate the expression of mouse histocompabililty antigens (H-2 locus) in hybrid clones and parental cell types. The binding of fluorescein-tagged antibody is measured on a cell-to-cell basis in large viable cell populations using flow microfluorimetric techniques. These techniques have been used to measure hapten and immunoglobulin binding to lymphocyte populations (8, 9, 14). However, this is the first report in which these techniques have been used to examine the expression of the H-2 locus. The advantage of this approach is twofold: first, a large and statistically significant sample population may be analyzed one cell at a time, thus revealing the fine detail of heterogeneity in the expression of the cell surface markers within a population. Second, as has been demonstrated for analysis of specific components of the immune system, this method does permit fluorescence-activated sorting of cell types according to their different surface populations (8, 9, 14)
Development of a Light-Weight, Reliable, Booster System for SHELS-Launched Payloads
Small satellite missions are often used to support low-cost space missions demonstrating new technologies. An economical source of low-cost space lift is to fly these satellites as secondary payloads aboard the Space Shuttle. The Shuttle has accommodations for flying these payloads using the Shuttle Hitchhiker Experiment Launch System (SHELS). While the relative costs for a Shuttle launch are at least an order of magnitude below the cost of a dedicated Expendable Launch Vehicle (ELV), final orbit altitude selection is limited to Shuttle mission goals. The Air Force Space Test Program (STP) is responsible for flying the Space Experiments Review Board (SERB) recommended experiments on a level-of-effort basis. Low-cost space lift is crucial to maximizing the number of SERB payloads that STP can support. Unfortunately, the typical Shuttle orbit does not provide a high enough orbit to guarantee the oneyear orbital lifetime required to meet STP mission objectives. A low-cost, autonomous STP Transfer Upper stage, Guided (TUG) that can boost an STP payload from a typical Shuttle orbit to a higher, longer duration orbit would allow STP to take advantage of the low-cost space lift provided by the Shuttle and still meet their mission requirements. The Air Force Research Laboratory Space Vehicles Directorate (AFRL/VS) is pursuing a solution to fulfill STPβs satellite lifting requirements by developing a low-cost, lightweight, reliable, strap-on propulsion module using several Small Business Innovative Research (SBIR) contracts focused on various parts of the TUG system. The Shuttle Expendable Rocket for Payload Augmentation (SHERPA) program will integrate all of these SBIR programs to meet the STP TUG requirement. The TUG system would be composed of several technologies being developed or already developed by AFRL/VS such as separation systems, guidance systems, propulsion modules, and modular bus architecture. The TUG would be re-startable for multiple orbit changes, station keeping, or deorbiting at the completion of a mission. Three versions of the TUG are envisioned. The first is a simple propulsion module that uses the satellite\u27s Attitude Control System (ACS) and Guidance, Navigation, and Control (GN&C) to provide stack guidance. The second is a fully autonomous TUG that lifts the payload to the higher orbit as cargo, separates from the payload, and then accomplishes a collision avoidance maneuver and propellant burn after payload separation. The third configuration is an autonomous TUG with a long duration module that allow experiments to use the TUG\u27s ACS, GN&C, and power systems in the intended final orbit. There are many challenges in the development of this vehicle. The most difficult of these is meeting the man-rating requirements of the Shuttle. All critical systems must have triple redundancy to ensure that the system does not threaten the Shuttle, its crew, or its mission. Another complication is producing a structure that meets the strict mass and volume restrictions of the SHELS system. Integration is als o a challenge, as many contractors and technologies are brought together under this program
The Lantern Vol. 14, No. 1, December 1945
β’ Editorial β’ The Medal β’ Pain β’ Wonder β’ Warmth β’ Memory Lingers β’ Morning β’ Watch the Birdie β’ Poems β’ The War Dogs of the Devildogs β’ Joy in Every Heart β’ To Live in Hearts β’ The Operation β’ Moderately Well Done β’ Steak is King β’ Grateful America?https://digitalcommons.ursinus.edu/lantern/1037/thumbnail.jp
The Lantern Vol. 14, No. 1, December 1945
β’ Editorial β’ The Medal β’ Pain β’ Wonder β’ Warmth β’ Memory Lingers β’ Morning β’ Watch the Birdie β’ Poems β’ The War Dogs of the Devildogs β’ Joy in Every Heart β’ To Live in Hearts β’ The Operation β’ Moderately Well Done β’ Steak is King β’ Grateful America?https://digitalcommons.ursinus.edu/lantern/1037/thumbnail.jp
Comportamentos agressivos em crianΓ§as e adolescentes com risco para esquizofrenia: diferenΓ§as entre gΓͺneros
OBJECTIVE: This study aimed to investigate whether differences in aggression-related behavioral problems occur between boys and girls at high risk for schizophrenia living in the city of SΓ£o Paulo, Brazil. METHOD: Using the Child Behavior Checklist, we compared the prevalence of behavioral problems between genders for the offspring (6-18 years) of mothers with diagnosis of schizophrenia and a comparison group of children born to women with no severe mental disorders recruited at the gynecology outpatient clinic of the same hospital. The Structured Clinical Interview for DSM-IV Axis I Disorders, Patient Edition was applied for the evaluation of diagnostic status of mothers. RESULTS: Male children of women with schizophrenia had a lower prevalence of aggressive behavior compared to females (4% vs. 36%; p = 0.005), whereas no gender differences regarding aggression were detected in the comparison group (24% vs. 32%; p = 0.53). Logistic regression analyses showed that male gender and being a child of women with schizophrenia interacted so as to favor lower prevalence of aggressive behavior (p = 0.03). CONCLUSION: These findings reinforce the notion that behavioral gender differences related to schizophrenia are already detectable in childhood.OBJETIVO: Investigar diferenΓ§as da ocorrΓͺncia de comportamentos agressivos entre crianΓ§as e adolescentes do sexo masculino e feminino com risco genΓ©tico para desenvolver esquizofrenia. MΓTODO: A prevalΓͺncia de comportamentos agressivos foi medida utilizando o inventΓ‘rio de comportamentos para crianΓ§as e adolescentes, Child Behavior Checklist, e comparada entre os gΓͺneros para o grupo de crianΓ§as filhas de mulheres com esquizofrenia e para um grupo de crianΓ§as filhas de mulheres atendidas no serviΓ§o de ginecologia do mesmo hospital. A entrevista clΓnica estruturada para DSM-IV (The Structured Clinical Interview for DSM-IV Axis I Disorders Patient Edition) foi utilizada para confirmar o diagnΓ³stico materno. RESULTADOS: Os filhos de mulheres com esquizofrenia do sexo masculino apresentaram prevalΓͺncia menor de comportamentos agressivos quando comparados Γ s meninas (4% x 36%; p = 0,005), o que nΓ£o ocorreu para o grupo comparativo (24% x 32%; p = 0,53). A anΓ‘lise de regressΓ£o logΓstica mostrou que pertencer ao sexo masculino e ser filho de mulher com esquizofrenia interagiram de forma a favorecer menor prevalΓͺncia de comportamentos agressivos (p = 0,03). CONCLUSΓO: Esses achados corroboram para a noção que as diferenΓ§as comportamentais entre os gΓͺneros na esquizofrenia podem ser detectadas precocemente durante a infΓ’ncia
Blockade of Hsp90 by 17AAG antagonizes MDMX and synergizes with Nutlin to induce p53-mediated apoptosis in solid tumors
Strategies to induce p53 activation in wtp53-retaining tumors carry high potential in cancer therapy. Nutlin, a potent highly selective MDM2 inhibitor, induces non-genotoxic p53 activation. Although Nutlin shows promise in promoting cell death in hematopoietic malignancies, a major roadblock is that most solid cancers do not undergo apoptosis but merely reversible growth arrest. p53 inhibition by unopposed MDMX is one major cause for apoptosis resistance to Nutlin. The Hsp90 chaperone is ubiquitously activated in cancer cells and supports oncogenic survival pathways, many of which antagonize p53. The Hsp90 inhibitor 17-allylamino-17-demethoxygeldanamycin (17AAG) is known to induce p53-dependent apoptosis. We show here that in multiple difficult-to-kill solid tumor cells 17AAG modulates several critical components that synergize with Nutlin-activated p53 signaling to convert Nutlin's transient cytostatic response into a cytotoxic killing response in vitro and in xenografts. Combined with Nutlin, 17AAG destabilizes MDMX, reduces MDM2, induces PUMA and inhibits oncogenic survival pathways, such as PI3K/AKT, which counteract p53 signaling at multiple levels. Mechanistically, 17AAG interferes with the repressive MDMXβp53 axis by inducing robust MDMX degradation, thereby markedly increasing p53 transcription compared with Nutlin alone. To our knowledge Nutlin+17AAG represents the first effective pharmacologic knockdown of MDMX. Our study identifies 17AAG as a promising synthetic lethal partner for a more efficient Nutlin-based therapy
Clinical and genetic characterisation of dystrophin-deficient muscular dystrophy in a family of Miniature Poodle dogs
Four full-sibling intact male Miniature Poodles were evaluated at 4β19 months of age. One was clinically normal and three were affected. All affected dogs were reluctant to exercise and had generalised muscle atrophy, a stiff gait and a markedly elevated serum creatine kinase activity. Two affected dogs also showed poor development, learning difficulties and episodes of abnormal behaviour. In these two dogs, investigations into forebrain structural and metabolic diseases were unremarkable; electromyography demonstrated fibrillation potentials and complex repetitive discharges in the infraspinatus, supraspinatus and epaxial muscles. Histopathological, immunohistochemical and immunoblotting analyses of muscle biopsies were consistent with dystrophin-deficient muscular dystrophy. DNA samples were obtained from all four full-sibling male Poodles, a healthy female littermate and the dam, which was clinically normal. Whole genome sequencing of one affected dog revealed a >5 Mb deletion on the X chromosome, encompassing the entire DMD gene. The exact deletion breakpoints could not be experimentally ascertained, but we confirmed that this region was deleted in all affected males, but not in the unaffected dogs. Quantitative polymerase chain reaction confirmed all three affected males were hemizygous for the mutant X chromosome, while the wildtype chromosome was observed in the unaffected male littermate. The female littermate and the dam were both heterozygous for the mutant chromosome. Forty-four Miniature Poodles from the general population were screened for the mutation and were homozygous for the wildtype chromosome. The finding represents a naturally-occurring mutation causing dystrophin-deficient muscular dystrophy in the dog
A Genome-Wide Investigation of SNPs and CNVs in Schizophrenia
We report a genome-wide assessment of single nucleotide polymorphisms (SNPs) and copy number variants (CNVs) in schizophrenia. We investigated SNPs using 871 patients and 863 controls, following up the top hits in four independent cohorts comprising 1,460 patients and 12,995 controls, all of European origin. We found no genome-wide significant associations, nor could we provide support for any previously reported candidate gene or genome-wide associations. We went on to examine CNVs using a subset of 1,013 cases and 1,084 controls of European ancestry, and a further set of 60 cases and 64 controls of African ancestry. We found that eight cases and zero controls carried deletions greater than 2 Mb, of which two, at 8p22 and 16p13.11-p12.4, are newly reported here. A further evaluation of 1,378 controls identified no deletions greater than 2 Mb, suggesting a high prior probability of disease involvement when such deletions are observed in cases. We also provide further evidence for some smaller, previously reported, schizophrenia-associated CNVs, such as those in NRXN1 and APBA2. We could not provide strong support for the hypothesis that schizophrenia patients have a significantly greater βloadβ of large (>100 kb), rare CNVs, nor could we find common CNVs that associate with schizophrenia. Finally, we did not provide support for the suggestion that schizophrenia-associated CNVs may preferentially disrupt genes in neurodevelopmental pathways. Collectively, these analyses provide the first integrated study of SNPs and CNVs in schizophrenia and support the emerging view that rare deleterious variants may be more important in schizophrenia predisposition than common polymorphisms. While our analyses do not suggest that implicated CNVs impinge on particular key pathways, we do support the contribution of specific genomic regions in schizophrenia, presumably due to recurrent mutation. On balance, these data suggest that very few schizophrenia patients share identical genomic causation, potentially complicating efforts to personalize treatment regimens
Nucleotide Discrimination with DNA Immobilized in the MspA Nanopore
Nanopore sequencing has the potential to become a fast and low-cost DNA sequencing platform. An ionic current passing through a small pore would directly map the sequence of single stranded DNA (ssDNA) driven through the constriction. The pore protein, MspA, derived from Mycobacterium smegmatis, has a short and narrow channel constriction ideally suited for nanopore sequencing. To study MspA's ability to resolve nucleotides, we held ssDNA within the pore using a biotin-NeutrAvidin complex. We show that homopolymers of adenine, cytosine, thymine, and guanine in MspA exhibit much larger current differences than in Ξ±-hemolysin. Additionally, methylated cytosine is distinguishable from unmethylated cytosine. We establish that single nucleotide substitutions within homopolymer ssDNA can be detected when held in MspA's constriction. Using genomic single nucleotide polymorphisms, we demonstrate that single nucleotides within random DNA can be identified. Our results indicate that MspA has high signal-to-noise ratio and the single nucleotide sensitivity desired for nanopore sequencing devices
Quantile-Specific Penetrance of Genes Affecting Lipoproteins, Adiposity and Height
Quantile-dependent penetrance is proposed to occur when the phenotypic expression of a SNP depends upon the population percentile of the phenotype. To illustrate the phenomenon, quantiles of height, body mass index (BMI), and plasma lipids and lipoproteins were compared to genetic risk scores (GRS) derived from single nucleotide polymorphisms (SNP)s having established genome-wide significance: 180 SNPs for height, 32 for BMI, 37 for low-density lipoprotein (LDL)-cholesterol, 47 for high-density lipoprotein (HDL)-cholesterol, 52 for total cholesterol, and 31 for triglycerides in 1930 subjects. Both phenotypes and GRSs were adjusted for sex, age, study, and smoking status. Quantile regression showed that the slope of the genotype-phenotype relationships increased with the percentile of BMI (Pβ=β0.002), LDL-cholesterol (Pβ=β3Γ10β8), HDL-cholesterol (Pβ=β5Γ10β6), total cholesterol (Pβ=β2.5Γ10β6), and triglyceride distribution (Pβ=β7.5Γ10β6), but not height (Pβ=β0.09). Compared to a GRS's phenotypic effect at the 10th population percentile, its effect at the 90th percentile was 4.2-fold greater for BMI, 4.9-fold greater for LDL-cholesterol, 1.9-fold greater for HDL-cholesterol, 3.1-fold greater for total cholesterol, and 3.3-fold greater for triglycerides. Moreover, the effect of the rs1558902 (FTO) risk allele was 6.7-fold greater at the 90th than the 10th percentile of the BMI distribution, and that of the rs3764261 (CETP) risk allele was 2.4-fold greater at the 90th than the 10th percentile of the HDL-cholesterol distribution. Conceptually, it maybe useful to distinguish environmental effects on the phenotype that in turn alters a gene's phenotypic expression (quantile-dependent penetrance) from environmental effects affecting the gene's phenotypic expression directly (gene-environment interaction)
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