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Monthly Archives: June 2017
Sunflower genome code cracked by team that included Tel Hai researcher – The Jerusalem Post
Posted: June 11, 2017 at 4:49 pm
The Jerusalem Post | Sunflower genome code cracked by team that included Tel Hai researcher The Jerusalem Post The sunflower genome is composed of approximately 3.5 billion bases and is larger than the human genome, which is composed of about 3.2 billion bases. Some 85% of the genome consists of identical sections that make identification and separation ... |
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Sunflower genome code cracked by team that included Tel Hai researcher - The Jerusalem Post
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5 Ways To Stop Eczema From Ruining Your Summer – Allure Magazine
Posted: at 4:49 pm
Since summer is synonymous with sunscreen, sweat, and splashing around in salt water and chlorine, it can often also mean skin flare-ups especially for those with eczema , the skin condition that causes patches of cracked, scaly skin.
Many people are well aware that eczema tends to flare in the winter, but it can flare even in the summertime, Sejal Shah , a board-certified dermatologist in New York City, tells Allure . The culprits? Everything from sweaty subway rides, to romping around in the sand to sticking to your strict sunscreen routine .
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In light of the fact that were officially in the heat of summer, we asked expert dermatologists how to fight an eczema flare-up without breaking a sweat.
Increased sweating in the summer can definitely make your eczema flare up, particularly if you have it in the creases of your elbows or knees or on your palms, Erin Gilbert , M.D., Ph.D., celebrity skin expert, tells Allure . Avoid being outdoors when the sun is most steamy. If you cant give up those outdoor runs or park picnics or escape a sweaty commute, wipe away sweat as it accumulates, then wash thoroughly and apply a moisturizer once you cool off, says Shah.
Another good trick is to put cornstarch or talc-free baby powder on areas where you tend to accumulate sweat to keep your skin drier, says Gilbert. I like Burts Bees Talc-Free Dusting Powder. Keep a sweat fighter in your bag to nix the need for extra washing-up on the go.
When your skin is ultra sensitive, you should switch up your sunscreen routine (not skip it). I like fragrance-free sunscreens for eczema prone patients because they tend to be better tolerated, says Shah. She recommends Juice Beauty SPF 30 Tinted Mineral Moisturizer, Blue Lizard SPF 30+ Sensitive Sunscreen and Mustela Broad Spectrum 50+ Mineral Sunscreen Lotion. For a post-sun moisturizer, try First Aid Beauty Ultra Repair Cream , Cerave Cream , or Aveeno Eczema Therapy Cream .
If your skin is sensitive or eczema prone, its really important to rinse chlorine off as soon as possible, says Gilbert. It can irritate and dry out your skin, making a flare more likely. Hit the showers, STAT.
Whether youre swimming, sweating or showering more than usual (because of said swimming and sweating), make sure youre lathering on more lotion than ever. Look for moisturizers that contain skin-protecting and hydrating ingredients such as purified petroleum, Joshua Zeichner , M.D., director of cosmetic and clinical research in dermatology at Mount Sinai Hospital in New York City, tells Allure . More than others, these formulations will form a protective barrier between your skin and the harsh summer elements. While traditional products were heavy and greasy, the newest formulations are quite light and easy to spread, Zeichner says. He recommends, Vaseline Intensive Care Advanced Repair Fragrance-Free Lotion . For something a little lighter, Gilbert recommends Cerave Daily Moisturizing Lotion .
Even if youre taking the steps above to treat your eczema-prone skin this summer, you might still experience frustrating patches that just wont go away, says Shah. Rather than forgo your collection of shorts and sundresses to cover any outbreaks, bring in the big guns and see your derm for a prescription treatment like a topical steroid or non-steroidal anti-inflammatory cream.
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Molecular Genetics – Cell and Gene Therapy Conferences
Posted: at 4:48 pm
Sessions/Tracks
Track 1:Molecular Biology
Molecular biologyis the study of molecular underpinnings of the processes ofreplication,transcription,translation, and cell function. Molecular biology concerns themolecularbasis ofbiologicalactivity between thebiomoleculesin various systems of acell,gene sequencingand this includes the interactions between theDNA,RNAand proteinsand theirbiosynthesis. Inmolecular biologythe researchers use specific techniques native to molecular biology, increasingly combine these techniques and ideas from thegeneticsandbiochemistry.
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2nd World Congress onHuman Genetics&Genetic Disorders, November 02-03, 2017 Toronto, Canada; 9th International Conference onGenomicsandPharmacogenomics, June 15-16, 2017 London, Uk; 6th International Conference and Exhibition onCellandGene Therapy, Mar 27-28, 2017 Madrid, Spain; Gordon Research Conference,Viruses&Cells, 14 - 19 May 2017, Lucca, Italy;Human Genome Meeting(HGM 2017), February 5-7 2017, Barcelona, Spain; Embl Conference:Mammalian GeneticsAndGenomics:From Molecular Mechanisms To Translational Applications, Heidelberg, Germany, October 24, 2017;GeneticandPhysiological Impacts of Transposable Elements, October 10, 2017, Heidelberg, Germany.
American Society for Cell Biology;The Society for Molecular Biology & Evolution;American Society for Biochemistry and Molecular Biology;The Nigerian Society of Biochemistry and Molecular Biology;Molecular Biology Association Search Form - CGAP.
Track 2:Gene Therapy and Genetic Engineering
Thegenetic engineeringis also called asgenetic modification. It is the direct manipulation of an organism'sofgenomeby usingbiotechnology. It is a set of technologies used to change the genetic makeup of the cell and including the transfer of genes across species boundaries to produce improved novelorganisms. Genesmay be removed, or "knocked out", using anuclease.Gene is targetinga different technique that useshomologousrecombinationto change anendogenous gene, and this can be used to delete a gene, removeexons, add a gene, or to introducegenetic mutations. There is an dna replacement therapy, Genetic engineering does not normally include traditional animal and plant breeding, gene sequencing, in vitro fertilization, induction of polyploidy,mutagenesisand cell fusion techniques that do not use recombinant nucleic acids or a genetically modified organism in the process,diseases treated with gene therapywas initially meant to introduce genes straight into human cells, focusing on diseases caused by single-gene defects, such as cystic fibrosis, hemophilia, muscular dystrophy and sickle cell anemia
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
8thWorld Congress onMolecular Pathology, June 26-27, 2017 San Diego, USA; 11thInternational Conference onSurgical Pathology& Practice, March 27-28, 2017, MADRID, SPAIN; 13th EuropeanPathologyCongress, Aug 02-03, 2017, MILAN, ITALY; 28th Annual Meeting, Austrian Society ForHuman GeneticsAnd The Swiss Society OfMedical GeneticsCombined Meeting 2017 march 29, 2017 - March 31, 2017, bochum , Germany.
Association for Clinical Genetic Science;Genetics Society of America | GSA;Association of Genetic Technologists;Molecular Genetics - Human Genetics Society of Australasia;Genetic Engineering - Ecological Farming Association.
Track 3:Cell & Gene Therapy
Cell therapy is also calledcellular therapyorCyto therapy, in which cellular material is injected into patient this generally means intact, living cells. The first category iscell therapyin mainstream medicine. This is the subject of intense research and the basis of potential therapeutic benefit. Such research can be controversial when it involves human embryonic material. The second category is in alternative medicine, and perpetuates the practice of injecting animal materials in an attempt to cure disease.Gene therapyis the therapeutic delivery of nucleic acid polymers into a patient's cells as a drug to treat disease. Gene therapy is a way to fix agenetic problemat its source. The polymers are either translated into proteins, interfere with targetgene expression, or possibly correct genetic mutations. The most common form uses DNA that encodes a functional,therapeutic gene to replace a mutated gene. The polymer molecule is packaged within a "vector", which carries the molecule inside cells. Vectors used in gene therapy, the vector incorporates genes intochromosomes. The expressed nucleases then knock out and replace genes in the chromosome. The Center forCell and Gene Therapyconducts research into numerous diseases, including but not limited to PediatricCancer, HIV gliomaandCardiovascular disease.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
2nd World Congress onHuman Genetics&Genetic Disorders, November 02-03, 2017 Toronto, 27 Canada ; 7th International Conference onPlant Genomics, July 03-05, 2017, Bangkok, Thailand ; American Society ofGeneandCell Therapy(ASGCT) 20th Annual Meeting, 10 - 13 May 2017, Washington, DC;Genomic Medicine for Clinicians(course), January 25-27, 2017, Hinxton , Cambridge, UK; Embo Conference:ChromatinandEpigenetics, Heidelberg, Germany, May 3, 2017; 14th International Symposium on Variants in theGenomeSantiago de Compostela, Galicia, Spain, June 5 - 8, 2017;
Genetics and Molecular Medicine - American Medical Association;Genetics Society of America / Gsa;British Society for Genetic Medicine;British Society for Gene and Cell Therapy; Australasian Gene Therapy Society.
Track 4:Cell Cancer Immunotherapy
Immunologydeals with the biological and biochemical basis for the body's defense against germs such as bacteria, virus and mycosis (fungal infections) as well as foreign agents such asbiological toxinsand environmental pollutants, and failures and malfunctions of these defense mechanisms. Cancer immunotherapy is the use of the immune system to treat cancer. Immunotherapies can be categorized as active, passive or hybrid (active and passive). Antibodies are proteins produced by the immune system that bind to a target antigen on the cell surface. The immune system normally uses them to fight pathogens. A type of biological therapy that uses substances to stimulate or suppress the immune system to help the body fight cancer, infection, and other diseases. Some types of immunotherapy only target certain cells of the immune system. Others affect the immune system in a general way. Types of immunotherapy include cytokines, vaccines, bacillus Calmette-Guerin (BCG), and some monoclonal antibodies.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
9thAnnual Meeting onImmunologyandImmunologist, July 03-05, 2017 Kuala Lumpur, Malaysia; 8th MolecularImmunology&ImmunogeneticsCongress, March 20-21, 2017 Rome, Italy; 8th EuropeanImmunologyConference, June 29-July 01, 2017 Madrid, Spain; July 03-05, 2017; B Cells and T Follicular Helper Cells Controlling Long-Lived Immunity (D2), April 2017, 2327, Whistler, British Columbia, Canada; Mononuclear Phagocytes in Health,Immune Defense and Disease, 304 May, Austin, Texas, USA;Modeling Viral Infections and ImmunityMAY 2017, 14, Estes Park, Colorado, USA; IntegratingMetabolism and Immunity(E4)292 June, Dublin, Ireland.
The American Association of Immunologists;Clinical Immunology Society ; Indian Immunology Society;IUIS - International Union of Immunological Societies;American Society for Histocompatibility and Immunogenetics.
Track 5:Clinical Genetics
Clinical geneticsis the practice of clinical medicine with particular attention tothe hereditary disorders. Referrals are made togenetics clinicsfor the variety of reasons, includingbirth defects,developmental delay,autism,epilepsy, and many others. In the United States, physicians who practice clinical genetics are accredited by theAmerican Board of Medical Genetics and Genomics(ABMGG).In order to become a board-certified practitioner of a Clinical Genetics, a physician must complete minimum of 24 months of his training in a program accredited by the ABMGG. Individual seeking acceptance intoclinical geneticstraining programs and should hold an M.D. or D.O. degree (or their equivalent)and he/she have completed a minimum of 24 months of their training in ACGME-accredited residency program internal medicine, pediatrics and gynecology or other medical specialty.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
Belgian Society OfHuman GeneticsMeeting 2017 february 17, 2017, Belgium; American College Of Medical Genetics 2017 AnnualClinical GeneticsMeeting march 21-25 2017, phoenix , United States; German Society Of Human Genetics 28th Annual Meeting, Austrian Society ForHuman GeneticsAnd The Swiss Society OfMedical GeneticsCombined Meeting 2017 march 29, 2017 - March 31, 2017, bochum , Germany; Spanish Society OfHuman GeneticsCongress 2017april 25, 2017 - April 28, 2017 madrid , Spain;
Clinical Genetics Associates;Clinical Genetics Society(CGS);The genetic associate;International Conference on Clinical and Medical Genetics;Association for Clinical Genetic Science;The American Society of Human Genetics.
Track 6:Pharmacogenetics
Pharmacogeneticsis the study of inherited genetic differences in drug metabolic pathways which can affect individual responses towards the drugs, both in their terms of therapeutic effect as well as adverse effects. In oncology, Pharmacogenetics historically is the study ofgerm line mutations(e.g., single-nucleotide polymorphisms affecting genes coding forliver enzymesresponsible for drug deposition and pharmacokinetics), whereaspharmacogenomicsrefers tosomatic mutationsin tumoral DNA leading to alteration in drug response.
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Spanish Society OfHuman GeneticsCongress 2017april 25, 2017 - April 28, 2017, madrid , Spain; 8th World Congress onPharmacology, August 07-09, 2017 Paris, France; World Congress onBio therapeutics, May 22-23, 2017, Mexico City, Mexico; 8th World Congress OnPharmacologyAndToxicology, July 24-26, 2017, Melbourne, Australia; German Society Of Human Genetics 28th Annual Meeting, Austrian Society ForHuman GeneticsAnd The Swiss Society OfMedical GeneticsCombined Meeting 2017march 29, 2017 - March 31, 2017 bochum , Germany.
Pharmacogenomics - American Medical Association;Associate Principal Scientist Clinical Pharmacogenetics;European Society of Pharmacogenomics and Personalised Therapy;Genome-wide association studies in pharmacogenomics.
Track 7:Molecular Genetic Pathology
Molecular genetic pathologyis an emerging discipline withinthe pathologywhich is focused in the study and diagnosis of disease through examination of molecules within the organs, tissues or body fluids. A key consideration is more accurate diagnosis is possible when the diagnosis is based on both morphologic changes in tissuestraditional anatomic pathologyand onmolecular testing. Molecular Genetic Pathology is commonly used in diagnosis of cancer and infectious diseases. Integration of "molecular pathology" and "epidemiology" led tointerdisciplinaryfield, termed "molecular pathological epidemiology" (MPE),which representsintegrative molecular biologicand population health science.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
8th World Congress OnMolecular Pathology, June 26-27, 2017 San Diego, USA; 11th International Conference OnSurgical Pathology& Practice, March 27-28, 2017, Madrid, Spain; 13th EuropeanPathologyCongress, Aug 02-03, 2017, Milan, Italy; Embl Conference:Mammalian GeneticsAndGenomics, Heidelberg, Germany, October 24, 2017; Embo|Embl Symposium: TheMobile Genome: Genetic And Physiological Impacts Of Transposable Elements, Heidelberg, Germany, October 10, 2017.
Clinical Pathology Associates Molecular Pathology; Association mapping Wikipedia;Association for Molecular Pathology(AMP);Molecular Pathology - Association of Clinical Pathologists;SELECTBIO - Molecular Pathology Association of India.
Track 8:Gene Mapping
Genomemappingis to place a collection of molecular markers onto their respective positions ongenome.Molecular markerscome in all forms. Genes can be viewed as one special type of genetic markers in construction ofgenome maps, and the map is mapped the same way as any other markers. The quality ofgenetic mapsis largely dependent upon the two factors, the number of genetic markers on the map and the size of themapping population. The two factors are interlinked, and as larger mapping population could increase the "resolution" of the maps and prevent the map being "saturated". Researchers begin a genetic map by collecting samples of blood or tissue from family members that carry a prominent disease or trait and family members that don't. Scientists then isolate DNA from the samples and closely examine it, looking for unique patterns in the DNA of the family members who do carry the disease that the DNA of those who don't carry the disease don't have. These unique molecular patterns in the DNA are referred to as polymorphisms, or markers.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
3rd WorldBio Summit&Expo, Abu Dhabi, UAE, June 19-21, 2017; 9th International Conference onGenomicsandPharmacogenomicsJune 15-16, 2017 London, Uk; Keystone Symposium: Mononuclear Phagocytes in Health,Immune DefenseandDisease, 304 May 2017, Austin, Texas, USA;Molecular Neurodegeneration(course) Hinxton, Cambridge, UK, January 9-14, 2017;
Association for Clinical Genetic Science;Genome-wide association study Wikipedia;Gene mapping by linkage and association analysis NCBI;Gene mapping by linkage and association analysis | Springer Link.
Track 9:ComputationalGenomics
Computational genomics refers to the use of computational and statistical analysis to decipherbiologyfromgenome sequencesand related data, including DNA and RNA sequence as well as other "post-genomic" data. This computational genomics is also known asComputational Genetics. These, in combination with computational and statistical approaches to understanding the function of the genes and statistical association analysis, this field is also often referred to as Computational and Statistical Genetics/genomics. As such, computational genomics may be regarded as a subset of bioinformatics and computational biology, but with a focus on using whole genomes rather than individual genes to understand the principles of how the DNA of a species controls its biology at the molecular level and beyond. With the current abundance of massive biological datasets, computational studies have become one of the most important means to biological discovery.The field is defined and includes foundations in thecomputer sciences,applied mathematics, animation, biochemistry, chemistry, biophysics,molecular genetics,neuroscienceandvisualization. Computational biology is different from biological computation, which is a subfield of computer engineering using bioengineering and biology to build computers, but is similar tobioinformatics.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
Modeling Viral Infections and Immunity,10. MAY 2017, 14, Estes Park, Colorado, USA;Integrating Metabolism and Immunity(E4)292 June, Dublin, Ireland; EMBL Conference:Mammalian GeneticsandGenomics, Heidelberg, Germany, October 24, 2017; EMBO|EMBL Symposium: The Mobile Genome:GeneticandPhysiological Impacts of Transposable Elements, Heidelberg, Germany, October 10, 2017;
American Association of Bio analysts - Molecular/Genetic Testing;ISCB - International Society for Computational Biology;International Society for Computational Biology Wikipedia;Bioinformatics societies OMICtools;Towards an Australian Bioinformatics Society.
Track 10:Molecular Biotechnology
Molecular Biotechnologyis the use of living systems and organisms to develop or to make products, or "any technological application that uses the biological systems, living organisms or derivatives, to make or modify products or processes for specific use. Molecular biotechnology results from the convergence of many areas of research, such as molecular biology, microbiology, biochemistry, immunology, genetics and cell biology. It is an exciting field fueled by the ability to transfer genetic information between organisms with the goal of understanding important biological processes or creating a useful product. The completion of the human genome project has opened a myriad of opportunities to create new medicines and treatments, as well as approaches to improve existing medicines. Molecular biotechnology is a rapidly changing and dynamic field. As the pace of advances accelerates, its influence will increase. The importance and impact of molecular biotechnology is being felt across the nation. Depending on the tools and applications, it often overlaps with the related fields of bioengineering,biomedical engineering, bio manufacturing andmolecular engineering.Biotechnologyalso writes on the pure biological sciences animalcell culture, biochemistry,cell biology, embryology, genetics, microbiology, andmolecular biology.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
8th EuropeanImmunologyConference, June 29-July 01, 2017 Madrid, Spain; World Congress onBio therapeutics, May 22-23, 2017, Mexico City, Mexico;Human Genome Meeting(HGM 2017), February 5-7 2017, Barcelona, Spain;Integrating MetabolismandImmunity (E4), 292 June, Dublin, Ireland.
Biotech Associations - Stanford University;Indian Society of Genetics, Biotechnology Research & Development;Genetics and Molecular Medicine - American Medical Association;Genetics Society of America | GSA, British Society for Genetic Medicine;Heritability in the Era of Molecular Genetics - Association for Psychological science.
Track 11:Genetic Transformation
Genetic Transformationis the genetic alteration of cell resulting from the direct uptake and incorporation ofexogenous genetic materialfrom its surroundings through thecell membrane. Transformation is one of three processes for horizontal gene transfer, in which exogenous genetic material passes from bacterium to another, the other two being conjugation transfer of genetic material between two bacterial cells in direct contact andTransductioninjection offoreign DNAby a bacteriophage virus into thehost bacterium. And about 80 species of bacteria were known to be capable of transformation, in 2014, about evenly divided betweenGram-positiveandGram-negative Transformation" may also be used to describe the insertion of new genetic material into non-bacterial cells, including animal and plant cells.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
13th EuropeanPathologyCongress, Milan, Italy; Embl Conference:Mammalian GeneticsAndGenomics, Heidelberg, Germany, October 24, 2017; Embo|Embl Symposium: TheMobile Genome: Genetic And Physiological Impacts Of Transposable Elements, Heidelberg, Germany, October 10, 2017; 2nd World Congress onHuman Genetics&Genetic Disorders, November 02-03, 2017 Toronto, Canada; 9th International Conference onGenomicsandPharmacogenomics, June 15-16, 2017 London, Uk;
American Society of Gene & Cell Therapy: ASGCT;Gene Therapy Societies and Patient Organizations - Gene Therapy Net;European Society of Gene and Cell Therapy (ESGCT);British Society for Gene and Cell Therapy;Gene Therapy - American Medical Association.
Track 12:Genetic Screening
Genetic screenis an experimental technique used to identify and select the individuals who possess a phenotype of interest inmutagenized population. A genetic screen is a type ofphenotypic screen. Genetic screen can provide important information on gene function as well as the molecular events that underlie a biological process or pathway. While thegenome projectshave identified an extensive inventory of genes in many different organisms, genetic screens can provide valuable insight as to how thosegenes function.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
13th EuropeanPathologyCongress, Aug 02-03, 2017, Milan, Italy; 2nd World Congress onHuman Genetics&Genetic Disorders, November 02-03, 2017 Toronto, 27 Canada; 7th International Conference onPlant Genomics, July 03-05, 2017, Bangkok, Thailand; Embl Conference:Mammalian GeneticsAndGenomics, Heidelberg, Germany, October 24, 2017; Embo|Embl Symposium: TheMobile Genome: Genetic And Physiological Impacts Of Transposable Elements, Heidelberg, Germany, October 10, 2017, 10 - 13 May 2017, American Society ofGeneandCell Therapy(ASGCT) 20th Annual Meeting, Washington, DC;
Association for Clinical Genetic Science; Association for Molecular Pathology (AMP);Mapping heritability and molecular genetic associations with cortical;Genetics and Molecular Medicine - American Medical Association.
Track 13:Regulation of Gene Expression
Regulation of Gene expressionincludes a wide range of mechanisms that are used by cells to increase or decrease the production of specific gene products (protein or RNA), and is informally termed gene regulation. Sophisticated programs of gene expression are widely observed in biology, Virtually any step of gene expression can be modulated, fromtranscriptional initiation,RNA processing, and post-translational modificationof a protein. Often, one gene regulator controls another in a gene regulatory network. Any step of gene expression may be modulated, from theDNA-RNA transcriptionstep to post-translational modification of a protein.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
7th International Conference onPlant Genomics, July 03-05, 2017, Bangkok, Thailand; EMBO|EMBL Symposium: The Mobile Genome:GeneticandPhysiological Impacts of Transposable Elements, Heidelberg, Germany, October 10, 2017; 10. MAY 2017, 14, Estes Park, Colorado, USA,Modeling Viral Infections and Immunity; 292 June, Dublin, Ireland,Integrating Metabolism and Immunity(E4); MAY 2017, 14, Estes Park, Colorado, USA,Modeling Viral InfectionsandImmunity; 8th EuropeanImmunologyConference, June 29-July 01, 2017 Madrid, Spain; 9th International Conference onGenomicsandPharmacogenomics, June 15-16, 2017 London, Uk;
Gene Therapy Societies and Patient Organizations - Gene Therapy Net;European Society of Gene and Cell Therapy (ESGCT);British Society for Gene and Cell Therapy;Gene Therapy - American Medical Association
Track 14: Cancer Gene Therapy
Cancer is an abnormal growth of cells the proximate cause of which is an imbalance in cell proliferation and death breaking-through the normal physiological checks and balances system and the ultimate cause of which are one or more of a variety of gene alterations. These alterations can be structural, e.g., mutations, insertions, deletions, amplifications, fusions and translocations, or functional (heritable changes without changes in nucleotide sequence). No single genomic change is found in all cancers and multiple changes (heterogeneity) are commonly found in each cancer generally independent of histology. In healthy adults, the immune system may recognize and kill the cancer cells or allow non-detrimental host-cancer equilibrium; unfortunately, cancer cells can sometimes escape the immune system resulting in expansion and spread of these cancer cells leading to serious life threatening disease. Approaches to cancer gene therapy include three main strategies: the insertion of a normal gene into cancer cells to replace a mutated (or otherwise altered) gene, genetic modification to silence a mutated gene, and genetic approaches to directly kill the cancer cells. Pathway C represents immunotherapy using altered immune cells. Another unique immunotherapy strategy facilitated by gene therapy is to directly alter the patient's immune system in order to sensitize it to the cancer cells. One approach uses mononuclear circulating blood cells or bone marrow gathered from the patient.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
8th EuropeanImmunologyConference, June 29-July 01, 2017 Madrid, Spain; World Congress onBio therapeutics, May 22-23, 2017, Mexico City, Mexico;Human Genome Meeting(HGM 2017), February 5-7 2017, Barcelona, Spain;Integrating MetabolismandImmunity (E4), 292 June, Dublin, Ireland.
Biotech Associations - Stanford University;Indian Society of Genetics, Biotechnology Research & Development;Genetics and Molecular Medicine - American Medical Association;Genetics Society of America | GSA, British Society for Genetic Medicine;Heritability in the Era of Molecular Genetics - Association for Psychological science.
Track 15:Genetic Transplantation
Transplantation genetics is the field of biology and medicine relating to the genes that govern the acceptance or rejection of a transplant. The most important genes deciding the fate of a transplanted cell, tissue, or organ belong to what is termed the MHC (the major histocompatibility complex). Genetic Transplantation is the moving of an organ from one body to another or from a donor site to another location on the person's own body, to replace the recipient's damaged or absent organ. Organs and/or tissues that aretransplantedwithin the same person's body are calledauto grafts. Transplants that are recently performed between two subjects of the same species are calledallografts. Allografts can either be from a living or cadaveric source Organs that can be transplanted are the heart, kidneys, liver, lungs, pancreas, intestine, and thymus. The kidneys are the most commonlytransplanted organs, followed by the liver and then the heart. The main function of the MHC antigens is peptide presentation to the immune system to help distinguish self from non-self. These antigens are called HLA (human leukocyte antigens). They consists of three regions: class I (HLA-A,B,Cw), class II (HLA-DR,DQ,DP) and class III (no HLA genes)
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
8th World Congress onPharmacology, August 07-09, 2017 Paris, France; International Conference onClinicalandMolecular Genetics, Las Vegas, USA, April 24-26, 2017; Aug 02-03, 2017, 13th EuropeanPathologyCongress, Milan, Italy; Embl Conference:Mammalian GeneticsAndGenomics, Heidelberg, Germany, October 24, 2017; 7th International Conference onPlant Genomics, July 03-05, 2017, Bangkok, Thailand.
American society of Transplantation;American Society of Transplant Surgeons: ASTS; Patient associations. Donation and transplantation;American Society of Gene & Cell Therapy ASGCT;Gene Therapy Societies and Patient Organizations - Gene Therapy Net.
Track 16:Cytogenetics
Cytogeneticsis a branch ofgeneticsthat is concerned withstudy of the structure and function of the cell, especially thechromosomes. It includes routine analysis of G-banded chromosomes, othercytogenetic banding techniques, as well as molecular Cytogenetics such as fluorescent in suitable hybridization FISH and comparativegenomic hybridization.
RelatedMolecular Biology Conferences| Genetics Conferences|Gene Therapy Conferences|Biotechnology Conferences| Immune Cell Therapy Conferences
9thAnnual Meeting onImmunologyandImmunologist, July 03-05, 2017 Kuala Lumpur, Malaysia; 8th MolecularImmunology&ImmunogeneticsCongress, March 20-21, 2017 Rome, Italy; 8th EuropeanImmunologyConference, June 29-July 01, 2017 Madrid, Spain; July 03-05, 2017; B Cells and T Follicular Helper Cells Controlling Long-Lived Immunity (D2), April 2017, 2327, Whistler, British Columbia, Canada.
European Cytogeneticists Association;Association of Genetic Technologists;Association for Clinical Genetic Science;Cytogenetics - Human Genetics Society of Australasia;European Cytogeneticists Association
Molecular Biology 2016
Molecular Biology 2016 Report
2ndWorld Bio Summit & Molecular Biology Expowas organized during October 10-12, 2016 at Dubai, UAE. The conference was marked with the attendance ofEditorial Board Members of supporting journals, Scientists, young and brilliant researchers, business delegates and talented student communities representing more than 25 countries, who made this conference fruitful and productive.
This conference was based on the theme Recent advances in Bio Science which included the following scientific tracks:
Molecular Biology
Microbiology
Analytical Molecular Biology
Bioinformatics
Biochemistry and Molecular Biology
Molecular Biology and Biotechnology
Cancer Molecular Biology
Computational Biology
Molecular Biology of the Cell
Molecular biology of the cardiovascular system
Molecular Biology in Cellular Pathology
Molecular Biology of Diabetes
Molecular Biology and Genetic Engineering
Enzymology and Molecular Biology
Molecular Biology of the Gene
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Molecular Genetics - Cell and Gene Therapy Conferences
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Is CRISPR Gene Editing Moving Ahead Too Quickly? – Healthline
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Researchers say they discovered hundreds of mutations during a gene editing experiment, casting doubt on CRISPR's safety and precision.
CRISPR gene editing technology has tantalized the public with its potential to cure disease.
However, new research suggests it could be more dangerous and less precise than previously believed.
CRISPR-Cas9 was discovered in 2012 by University of California molecular biologist Jennifer Doudna and her colleagues. It allows for genetic editing by snipping out small bits of defective or harmful DNA and replacing it.
Gene editing has existed since the 1970s, but CRISPR-Cas9 has reinvented it as a precise, accessible technology.
The potential applications seem almost limitless.
This year, Dr. Edze Westra of the University of Exeter, told the Independent that he expects the technology to be used to cure all inherited diseases, to cure cancers, to restore sight to people by transplanting genes.
Read more: Scientists find gene editing with CRISPR hard to resist
Still in its infancy, CRISPR-Cas9 has yet to deliver on these promises, in humans anyway.
One of the key talking points of CRISPR-Cas9 has been its precision its ability to accurately edit small sections of DNA without affecting nearby sections.
However, a new study from Columbia University says that CRISPR-Cas9 can introduce hundreds of unexpected mutations into the genome beyond what was intended.
We feel its critical that the scientific community consider the potential hazards of all off-target mutations caused by CRISPR, said co-author Dr. Stephen Tsang, a professor at Columbia University Medical Center, in a press release.
Tsang and his team discovered the mutations while conducting research on mice, using CRISPR-Cas9 to correct a gene that caused blindness.
The technology worked effectively in curing the blindness, but when the researchers later looked at the genome of the mice, they said they found additional, unintended mutations.
Despite this, the mice appeared to be in fine health.
We did not see any observable complications in the mice, despite having all these extra CRISPR-related mutations, Tsang told Healthline.
Sheila Jasanoff, professor of science and technology studies at Harvard University, told Healthline that precision can have a slippery definition in biotechnology.
Genetic engineering was also sold some 40 years ago as a highly precise technique. Now, CRISPR is being heralded as even more precise, she said.
Undoubtedly, there is some truth in that claim ... But we also know from older genetic engineering techniques that very precise interventions into one part of a genome can produce unexpected side effects or off-target impacts that scientists were not expecting, Jasanoff added.
Read more: CRISPR gene editing and cancer treatment
Tsang frames the message of his research in two ways.
First, he hopes that his work will bring a newfound awareness to the potential side effects caused by CRISPR.
Although the mutations he and his team observed did not appear to have any malignant effects, they should be a wake-up call for researchers.
Secondly, Tsang says that no matter what kind of medicine or treatment is being used, there is the potential for side effects.
If we apply CRISPR, its just like any other intervention medicine. There is always off-targeting and risks and benefits, he says.
Jasanoff is more tempered in her assessment of the risk vs. reward of CRISPR.
The assumption that there are untold benefits in store long before the work has been done to establish how a new technology actually will have an impact on any disease is a typical example of the hype that surrounds new and emerging technologies, she said.
Tsangs research offers no hard answers to the larger questions of efficacy, risk, and benefit of using CRISPR on humans.
Lets not go overboard, said Pete Shanks, a consultant who is an expert on genetics. Three blind mice dont prove much.
Tsangs research does provide some cautionary insight into how research must be conducted in order to make the technology safer.
Currently most studies of off-target mutations depend on computer algorithms to locate and examine affected areas. Tsang and his team say that this isnt sufficient when using live specimens.
These predictive algorithms seem to do a good job when CRISPR is performed in cells or tissues in a dish, but whole genome sequencing has not been employed to look for all off-target effects in living animals, Alexander Bassuk, professor of pediatrics at the University of Iowa, and co-author of the study, said in a press release.
Researchers who arent using whole genome sequencing to find off-target effects may be missing potentially important mutations, Tsang said.
Read more: Gene editing could be used to battle mosquito-borne disease
This study comes at an important time.
China has begun its first round of human testing using CRISPR-Cas9.
The United States is due to start its own tests next year.
The research field is moving quickly perhaps too quickly.
We hope our findings will encourage others to use whole genome sequencing as a method to determine all the off-target effects of their CRISPR techniques and study different versions for the safest, most accurate editing, Tsang said.
Jasanoff is much blunter.
We should put aside the notion the benefits of CRISPR are already proven, and all we need to worry about is risks, she said.
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AI used to treat bipolar disorder in an app that could revolutionize medicine – ScienceBlog.com (blog)
Posted: at 4:48 pm
Cohen found a receptive audience in Fleck, who was working with UCs former Center for Imaging Research. After all, who better to tackle one of medical sciences hardest problems than a rocket scientist? Cohen, an aerospace engineer, felt up to the task.
Ernest said people should not conflate the technology with its applications. The algorithm he developed is not a sentient being like the villains in the Terminator movie franchise but merely a tool, he said, albeit a powerful one with seemingly endless applications.
I get emails and comments every week from would-be John Connors out there who think this will lead to the end of the world, Ernest said.
Ernests company created EVE, a genetic fuzzy AI that specializes in the creation of other genetic fuzzy AIs. EVE came up with a predictive model for patient data called the LITHium Intelligent Agent or LITHIA for the bipolar study.
This predictive model taps into the power of fuzzy logic to allow you to make a more informed decision, Ernest said.
And unlike other types of AI, fuzzy logic can describe in simple language why it made its choices, he said.
The researchers teamed up with Dr. Caleb Adler, the UC Department of Psychiatry and Behavioral Neuroscience vice chairman of clinical research, to examine bipolar disorder, a common, recurrent and often lifelong illness. Despite the prevalence of mood disorders, their causes are poorly understood, Adler said.
Really, its a black box, Adler said. We diagnose someone with bipolar disorder. Thats a description of their symptoms. But that doesnt mean everyone has the same underlying causes.
Selecting the appropriate treatment can be equally tricky.
Over the past 15 years there has been an explosion of treatments for mania. We have more options. But we dont know who is going to respond to what, Adler said. If we could predict who would respond better to treatment, you would save time and consequences.
With appropriate care, bipolar disorder is a manageable chronic illness for patients whose lives can return to normal, he said.
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11 Times Bill Maher’s Politically Incorrect Comments Sparked …
Posted: at 4:48 pm
Comedian Bill Maher has made a career of saying things that could come back to haunt him, both on his former ABC show "Politically Incorrect with Bill Maher" and on his current HBO show "Real Time with Bill Maher." Though Maher prides himself on being politically incorrect, there have been plenty of times he's said offensive things that got him into hot water. Here's a look at 11 of them.
11. Maher interviews alt-right darling Milo Yiannopoulos After Milos speech at Berkeley University was canceled because of protests that included a few small fires and thrown objects, Maher brought the alt-right idol in for an interview. Though Milos anti-feminism, anti-transgender and anti-Muslim positions are well known -- as is his role in the harassment-focused online movement known as GamerGate -- Maher offered almost no pushback against Milo. Read more here.
10. Maher jokes about Tila Tequila being assaulted In 2009, news broke that Tila Tequila claimed shed been assaulted by then-boyfriend and San Diego Charger Shawne Merriman. Maher responded with a joke many found sexist: New rule: Stop acting surprised someone choked Tila Tequila! The surprise is that someone hasnt choked this bitch sooner.
9. Maher claims Hillary Clinton cried for political gain During the 2008 presidential campaign, Maher tore into Clinton. In what many read as a sexist remark, Maher said women use crying to win arguments and accused Clinton of crying on the campaign trail for the same reason. Watch the clip here.
8. Maher says millions of Muslims supported the Charlie Hebdo attacks Maher has a long history of being highly critical of religion and, in recent years, of Islam in particular. In the wake of the 2015 Charlie Hebdo attack in France, Maher said hundreds of millions of Muslims supported the violence, in which 12 people were killed and 11 more were injured. Watch the clip.
7. He gets into an Islamophobia argument with Ben Affleck On a panel with actor Ben Affleck and author Sam Harris, Maher defended Harris assertions about Islam, including when Harris said Islam at this moment is the mother lode of bad ideas. The discussion turned into a shouting match, as Affleck quickly challenged the stance and bigotry related to discussions of Islam. Watch the clip here.
6. Maher compares One Directions Zayn Malik to Boston Marathon bomber Singer Zayn Malik quit the band One Direction, prompting a few jokes from Maher during an episode. But people were angered when Maher asked, Where were you during the Boston Marathon, placing an image of Malik beside one of bomber Dzhokhar Tsarnaev. Many saw the joke as one mocking both Maliks appearance and his Muslim faith. Watch the clip.
5. He defends Bill OReillys joke about Maxine Waters After former Fox News host Bill OReilly said Congresswoman Maxine Waters hair looked like a James Brown wig, Maher came to his defense on Real Time. Mahers point: liberals cant take a joke. Many criticized OReillys joke to be racist, and he later apologized. Watch the clip here.
4. Maher says dogs are like children with mental disabilities In the middle of making some point about how hes not lauded enough for raising dogs, Maher said dogs are like retarded children. Guests floundered both to address Mahers use of the offensive word and the much more offensive comparison of children with disabilities to animals. Watch the clip.
3. ...And makes fun of Sarah Palins son Trig Maher pushed that button again when he referred to Trig as it and said he looks a lot like John Edwards. Watch the clip here.
2. Maher says 9/11 terrorists werent cowardly Maher's ABC show Politically Incorrect" was canceled in June 2002 after what he later explained was his attempt to level criticism against the American military. Less than a week after Sept. 11, 2001, Maher said the terrorists who stayed aboard planes were warriors, adding that the U.S. had been cowardly for firing cruise missiles at enemies from 2,000 miles away. The comment caused a row, as advertisers pulled out of the show. Watch the clip.
1. Maher says Im a house n---a In his latest bout of outrage-driving commentary, Maher offhandedly dropped the n-word in the middle of an interview. HBO has since said the comment was inexcusable and is removing it from reruns of the show and Maher has apologized.
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Mahers been here before: Watch him defend using the n-word …
Posted: at 4:48 pm
As reported, Bill Maher has lined up a panel of guests who will no doubt attempt to helphim talk through the furor he created when he called himself the n-word last Friday on his HBO show Real Time with Bill Maher.
While the host has already offered a partially well-wrought apology in the face of intense pressure and criticism, this is not his first public go around with the loaded racial epithet.
In a post on theFader, writer Jordan Darvillehelpfully reminded us all of something that, quite shamefully for this moment, slipped the minds of many (including Salon).
In 2001, following a similar controversy tied to comedian Sarah Silvermans use of the anti-Chinese racial epithet chink, Maherinvited her,Guy Aoki of the Media Action Network for Asian Americans and the actor and activist Anne-Marie Johnson to discuss the issue on his ABC show Politically Incorrect. David Spade, much to his apparent and understandable embarrassment, was there too.
As you can see in the video below, the discussion around Silvermans joke seems even more brokenand fraught than it probably did at the time. Its doubtful Silverman or any accomplished comedian for that matter would perform it today, let alone go on network TV to tell an Asian-rights activist they were wrong for taking offense toit.
Talk turns, as one would expect, to the n-word. The combative exchange betweenJohnson and Maher starts at about 13:40.It does not go well for the host.
Blacks are like whites cannot say this word,' he says.I disagree. This word has changed in the last 10, 15 years. According to who? asks Johnson. According to culture . . . Maher booms back at her. Ask any African-American person in this audience what that means, Johnson replies with an appropriate amountof alarm. Every African-American person in this audience users that word night and day, its in every song its all through culture says Maher.
With Johnson declaring youre wrong, youre wrong, Maher brings up the worn old penny about the n-word now being a term of endearment, explaining to a black woman how she should feel. He thenstates to the light-skinned Johnson, First of all, I wouldnt even know you were black if you didnt tell me.
I love it when white people try to define what is African American,' says Johnson. Im African American regardless of my skin color or my hair, she added. I think Im only one on this stage whos qualified to talk about the meaning of the word, how it hurts, how it doesnt hurt, where its used, the history of it. Because I live it everyday. David Spade continues to look miserable.
Having heard that impassioned demand for understanding, Maher nonetheless continues, Its in every song on the radio, okay?Nigga, nigga, nigga, nigga, nigga, nigga, nigga, nigga, nigga is in every song, okay? People come up to me and go, Bill, you a nigga. But I cant say thank you or I go please dont use that word?
After talking about the group NWA and his mother, Maher adds, Im saying when the word has come this far into the mainstream, for a very good reason they co-opted the word to make it less powerful. As Johnson notes that she objects to its use in rap music because it shows a lack of appreciation for history, both Maher and Silverman trumpet words evolve!
Listen, folks says Johnson, its not a word we can use. Can you please pass me the tea, and pass me the nigger too? Itstill hurts. Following that, Silverman and Maher continue to try to paint Aoki and Johnson as somehow villains for being hurt by epithets (or, as they seem to think,lyingabout claiming to be hurt.) Seen through todays lens, its deeply shameful.
Now, yes, some 16 years have passed since this segment, 16 years that have seen a great deal of changes in how we talk about race in the public square. Undoubtedly, there have been a great many changes in Maher as well: he evinced none of the strident defensiveness seen here in his apology this Saturday.
And, yet, when you combine this footage from 2001 with the ease and self-satisfaction apparent in his use of the very same epithet on Friday, it paints a picture of a man whos quite willing to disregard the pain he might cause black people all so he can say his precious n-word.
Who Bill Maher willbecome down the road may be a different creature. Up until Saturday, however,he appeared to be one incapable of listening to the pleas of someonereasonably, passionately, persuasively asking him not to hurt them from, literally, three feet away. It makes the case for his honest rehabilitation shaky.
Maher may say hes undergoing a process of self discovery, but he was given all the tools he needed not to wind up where he is now over a decade and a half ago. He didnt learn a thing.
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Trump was elected to be politically incorrect, not crazy – Lewiston Morning Tribune (subscription)
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WASHINGTON - Having coined Bush Derangement Syndrome more than a decade ago, I feel authorized to weigh in on its most recent offshoot. What distinguishes Trump Derangement Syndrome is not just general hysteria about the subject, but additionally the inability to distinguish between legitimate policy differences on the one hand and signs of psychic pathology on the other.
Take Trump's climate-change decision. The hyperbole that met his withdrawal from the Paris agreement - a traitorous act of war against the American people, America just resigned as leader of the free world, etc. - was astonishing, though hardly unusual, this being Trump.
What the critics don't seem to recognize is that the Paris agreement itself was a huge failure. It contained no uniform commitments and no enforcement provisions. Sure, the whole world signed. But onto what? A voluntary set of vaporous promises. China pledged to "achieve the peaking of CO2 emissions around 2030." Meaning that they rise for another 13 years.
The rationale, I suppose, is that developing countries like India and China should be given a pass because the West had a two-century head start on industrialization.
I don't think the West needs to apologize - or pay - for having invented the steam engine. In fact, I've long favored a real climate-change pact, strong and enforceable, that would impose relatively uniform demands on China, India, the U.S., the EU and any others willing to join.
Paris was nothing but hot air. Withdrawing was a perfectly plausible policy choice (the other being remaining but trying to reduce our CO2-cutting commitments). The subsequent attacks on Trump were all the more unhinged because the president's other behavior over the last several weeks provided ample opportunity for shock and dismay.
It's the tweets, of course. Trump sees them as a direct, "unfiltered" conduit to the public. What he doesn't quite understand is that for him - indeed, for anyone - they are a direct conduit from the unfiltered id. They erase whatever membrane normally exists between one's internal disturbances and their external manifestations.
For most people, who cares? For the president of the United States, there are consequences. When the president's id speaks, the world listens.
Consider his tweets mocking the mayor of London after the most recent terror attack. They were appalling. This is a time when a president expresses sympathy and solidarity - and stops there. Trump can't stop, ever. He used the atrocity to renew an old feud with a minor official of another country. Petty in the extreme.
As was his using London to support his misbegotten travel ban, to attack his own Justice Department for having "watered down" the original executive order (ignoring the fact that Trump himself signed it) and to undermine the case for it just as it goes to the Supreme Court.
As when he boasted by tweet that the administration was already doing "extreme vetting." But that explodes the whole rationale for the travel ban - that a 90-day moratorium on entry was needed while new vetting procedures were developed. If the vetting is already in place, the ban has no purpose. The rationale evaporates.
And if that wasn't mischief enough, he then credited his own interventions in Saudi Arabia for the sudden squeeze that the Saudis, the UAE, Egypt and other Sunni-run states are putting on Qatar for its long-running dirty game of supporting and arming terrorists (such as the Muslim Brotherhood and Hamas) and playing footsie with Iran.
It's good to see our Sunni allies confront Qatar and try to bring it into line. But why make it personal - other than to feed the presidential id? Gratuitously injecting the U.S. into the crisis taints the endeavor by making it seem an American rather than an Arab initiative and turns our allies into instruments of American designs rather than defenders of their own region from a double agent in their midst.
And this is just four days' worth of tweets, all vainglorious and self-injurious. Where does it end?
The economist Herb Stein once quipped that "if something cannot go on forever, it will stop." This really can't go on, can it? But it's hard to see what, short of a smoking gun produced by the Russia inquiry, actually does stop him.
Trump was elected to do politically incorrect - and needed - things like withdrawing from Paris. He was not elected to do crazy things, starting with his tweets. If he cannot distinguish between the two, Trump Derangement Syndrome will only become epidemic.
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You can’t govern by presidential id – Wichita Eagle (blog)
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You can't govern by presidential id Wichita Eagle (blog) Trump was elected to do politically incorrect - and needed - things like withdrawing from Paris. He was not elected to do crazy things, starting with his tweets. If he cannot distinguish between the two, Trump Derangement Syndrome will only become ... |
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Egyptian rappers fight against censorship – Deutsche Welle
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"Egypt Rap School for Biggenas" is plastered across the wall of a tiny recording studio in Alexandria, Egypt. Above it, hang three portraits: Notorious BIG, Bob Marley and Tupac Shakur. Like millions of fans, Temraz - his stage name - grew up listening to these icons.
Now, the 29-year-old Arabic rapper is part of Revolution Records, an underground label that he helped establish in Alexandria 11 years ago.
"We decided to name the label Revolution Records because we thought rap was still a very weird [genre] to Egyptian ears," Temraz said, before rolling a cigarette. "We also named it 'revolution' because rap music is about rebelling. To us, [rap] is about rebelling against everything."
Read:Egypt's women find their voice against sexual harassment
There are 14 members in Revolution Records, which is one of many hip-hop movements in Egypt. Cairo, the capital, has a bustling scene. But Alexandria is considered the pioneer of rap music in the country.
Before the Arab Spring, rappers from Alexandria released tracks that mocked social norms and crony political elites. The lack of mainstream attention even enabled some artists to push the boundaries of censorship. And while their music was gaining traction, it wasn't popular enough to invite a crackdown from the state.
But in today's Egypt, where thousands of youth are in jail for criticizing the regime, rapping about politics is riskier than ever.
Rapping to ridicule
Shakur (photo, above) is the stage name of a 31-year-old artist who is part of a group called DaCliQue 203. He said that most rappers have been reluctant to ridicule Egypt's President Abdel Fattah el-Sissi. His group, however, is one of few exceptions.
In February 2014, DaCliQue 203 released "Ana Malak," which means"I'm the King." The track was a remix of a song that Shakur originally recorded in 2005. The new version was made to mock el-Sissi who was by then fixed in power.
Notorious BIG, Bob Marley and Tupac Shakur bedeck the wall at Revolution Records' studio
"The lyrics go like this," said Shakur, as he proceeded to recite his impersonation of el-Sissi. "I'm not on the right and I'm not on the left. I'm not an Islamist nor an anarchist. I just follow the money so show me the money."
The song was daring. And yet, Shakur wouldn't record another track for three more years. He said he couldn't bring himself to make another one. Not after his younger brother, a former supporter of the outlawed Muslim Brotherhood, passed away suddenly in his home before "Ana Malak" was released.
Read:Marteria - a German rapper in Africa
"We always fought about my love for hip-hop," said Shakur. "[My brother] thought I was wasting my time. He thought I should be writing articles about politics instead. But at the same time, he remained curious. He always wanted to know about the lyrics I was writing."
Other rappers became increasingly political while Shakur took a break from hip-hop. In April 2016, Revolution Records released "Masahsh Keda" - "That's Not Right" - on YouTube. The group appropriated the phrase from el-Sissi, who often says it condescendingly when addressing his citizens. The group made a music video for the song and included English subtitles.
"We sampled el-Sissi's voice and incorporated it in our music," Temraz told DW. "The track did well when we first uploaded it. I think it received more than 200,000 likes."
Despite the success, Temraz feared that the song might bring reprisal. After the track was released, members of Revolution Records were invited to Denmark to perform in a concert. Temraz was anxious when he arrived at the Cairo airport. He thought he would be arrested. Lucky for him, nothing happened.
Weeks later, the group was informed that "Masahsh Keda" had crossed a line. Their friend, who worked in the presidential palace, warned them that the government wouldn't tolerate another track like that again.
"We had to stop," Temraz said. "I gave up trying to change this country for the better."
Moving away, coming back
Not everyone lost hope. Some rappers tried to broach sensitive topics without explicitly blaming the state. Y-Crew, which is one of Egypt's first hip-hop groups, released a track titled "Blinded" nine months ago. The song was about the abuse and violence that street children face in Egypt.
"Mainstream music in Egypt is just about love. It doesn't talk about real problems," said Omar Bofolot, one of the original members of Y-Crew. "We want to talk about real stuff. But we don't want to preach to people about what they should do."
The group has recently moved to Dubai to work on their latest album. They told DW that they are also losing hope that their music can make a positive impact in Egypt.
"We been rapping about social and political issues since we started," said Shahin, the second member of Y-Crew. "Nothing is changing [in Egypt], and we're getting sick of it. Our next album is just going to promote peace, love and unity."
Shakur, however, won't stop rapping about the issues that matter to him. In January, he released his comeback track. And now, he's writing lyrics about the refugee crisis in Egypt and Europe.
Thousands of refugees and Egyptians have died trying to cross the Mediterranean from Alexandria. Shakur knows their stories firsthand. He's been a migration advocate for years and has even collaborated with some refugee rappers in Egypt.
The oppressive political climate doesn't scare him. Even if Egyptian rap becomes more commercial, he vows to never censor himself.
"I have to keep it real," he told DW. "The price might be bigger. But Egyptians are paying a heavy price anyways."
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