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How Genomics will ensure a risk-free and beneficial treatment for good health and well-being – The Financial Express
Posted: December 28, 2022 at 11:17 pm
How Genomics will ensure a risk-free and beneficial treatment for good health and well-being The Financial Express
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Ron Paul: ‘Twitter Files’ Make It Clear, We Must Abolish The FBI
Posted: at 10:54 pm
Authored by Ron Paul via The Ron Paul Institute for Peace & Prosperity,
As we learn more and more from the Twitter Files, it is becoming all too obvious that Federal agencies such as the FBI viewed the First Amendment of our Constitution as an annoyance and an impediment. In Fridays release from the pre-Musk era, journalist Matt Taibbi makes an astute observation: Twitter was essentially an FBI subsidiary.
The FBI, we now know, was obsessed with Twitter. We learned that agents sent Twitter Trust and Safety chief Yoel Roth some 150 emails between 2020 and 2022. Those emails regularly featured demands from US government officials for the private social media company to censor comments and ban commenters they did not like.
The Foreign Influence Task Force (FITF), a US government entity that included the FBI as well as other US intelligence agencies expressly forbidden from domestic activities, numbered 80 agents engaged regularly in telling Twitter which Tweets to censor and which accounts to ban. The Department of Homeland Security brought in outside government contractors and (government-funded) non-governmental organizations to separately pressure Twitter to suppress speech the US government did not like.
US Federal government agencies literally handed Twitter lists of Americans it wanted to see silenced, and Twitter complied. Let that sink in.
This should be a massive scandal and likely it would have been had it occurred under a Trump Administration. Indeed, Congress would be gearing up for Impeachment 3.0 if Trump-allied officials had engaged in such egregious behavior. But since these US government employees were by-and-large acting to suppress pro-Trump sentiment, all we hear are crickets.
What is interesting about these Twitter revelations is how obsessed the FBI and its government partners were with satire and humor. Even minor Twitter accounts with small numbers of followers were constantly flagged by the Feds for censorship and deletion. But knowledge of history helps us understand this obsession: in Soviet times the population was always engaged in joking about the ineptitude, corruption, and idiocy of the political class. Underground publications known as samizdat were rich with satire, humor, and ridicule.
Tyrants hate humor and cannot withstand satire. That is clearly why the FBI (and CIA) was determined to see a heavy hand raised against any American poking fun at the deep state.
There is good news in all of this, however. As Constitutional Law Professor Jonathan Turley wrote over the weekend, a new Harvard CAPS/Harris Poll found that even though the mainstream media has ignored the Twitter files, Americans have not. Nearly two-thirds of respondents believe that Twitter was involved in politically-motivated censorship in advance of the 2020 election. Some 70 percent of those polled believe Congress must take action against this corporate/state censorship.
As Professor Turley points out, although the First Amendment only applies to the US government, it does apply to agents or surrogates of the government. Twitter now admits that such a relationship existed between its former officials and the government.
So now we have proof that the FBI (along with US intelligence agencies and the Department of Homeland Security) have been acting through private social media companiesto manipulate what Americans are allowed to say when they communicate with each other.
Is there anything more un-American than that? Personally, I find it sickening.
We do not need the FBI and CIA and other federal agencies viewing us as the enemy and attacking our Constitution. End the Fedand End the Federal Bureau of Investigation!
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Ron Paul: A Tale Of Two Midterms | ZeroHedge
Posted: at 10:54 pm
Authored by Ron Paul via The Ron Paul Institute for Peace & Prosperity,
Those searching for an explanation of why there was no red wave giving Republicans huge gains in Congress in this years midterm election should compare this years election with the midterm election of 2010. In 2010, Republicans gained a net 63 House seats. While Republicans then did not gain control of the US Senate, they did gain six Senate seats.
These Republican victories in 2010 were propelled by the Tea Party and the liberty movement. These movements became prominent during the waning days of the Bush administration. The liberty movement was advanced by grassroots supporters of my 2008 presidential campaign. The liberty movements focus was, and is, on restoring constitutional government in all areas, ending our interventionist foreign policy, and changing our monetary policy by auditing and ending the Federal Reserve and legalizing alternative currencies. Early on, the Tea Party largely focused on opposition to the 2008 bank bailouts.
There was overlap between the liberty movement and the Tea Party as many members of both groups fought for auditing and ending the Fed, ending bailouts, and preventing Congress from passing Obamacare.
Many Republican candidates in 2010 appealed to Tea Party voters by not just promising to repeal Obamacare. They also promised to work to restore limited, constitutional, fiscally responsible government in all areas. In contrast, in 2022 the average Republican candidate offered little in the way of a substantive agenda. In fact, few Republicans called for reversing President Bidens massive spending increases, much less for restoring the federal government to its constitutional limitations. Despite the controversy over new critical race theory and transgender related policies in government schools, there has not been a renewed push to shut down the Department of Education.
Many Republican candidates in the 2022 midterm election also failed to make an issue out of their Democratic opponents support for mask and vaccine mandates and other instances of covid tyranny. Those who did oppose the covid tyranny, such as Florida Governor Ron DeSantis and my son Kentucky Senator Rand Paul, won landslide victories.
The Tea Partys success in forcing the Republican Party to focus on a more pro-liberty, limited government agenda was short lived. Soon after the 2010 election, the Republican establishment returned to its big spending ways. Spending and debt continued to rise under President Trump and a Republican Congress. Republicans even failed to deliver on their signature promise: repealing Obamacare.
The 2010 midterm election showed that people will respond to candidates offering serious pro-liberty ideas and policies. However, the Tea Partys rise and fall also shows the danger facing ideological movements that become too close with one political party. These movements will start pulling their punches when one of our team begins casting bad votes. The argument goes that we must support big government Republicans or we get REALLY big government Democrats.
Fortunately, the liberty movement has remained committed to principles. As the failure of the welfare-warfare state to deliver peace and property and the failure of the Federal Reserve to fulfill its mandate of ensuring stable prices and low unemployment become clear, more Americans will join the liberty movement. Support for the liberty movement will accelerate when the inevitable economic meltdown occurs. This meltdown will be precipitated by a collapse in the dollars value and the rejection of the dollars world reserve currency status. It will bring the end of the welfare-warfare state and the fiat money system. Hopefully, the liberty movement will ensure the welfare-warfare state and fiat money system are replaced by a return to limited constitutional government, individual liberty, and peace.
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Deimos (moon) – Wikipedia
Posted: at 10:22 pm
Smaller, outer moon of Mars
Deimos (systematic designation: Mars II)[10] is the smaller and outermost of the two natural satellites of Mars, the other being Phobos. Of similar composition to C and D-type asteroids, Deimos has a mean radius of 6.2km (3.9mi) and takes 30.3hours to orbit Mars.[5] Deimos is 23,460km (14,580mi) from Mars, much farther than Mars's other moon, Phobos.[11] It is named after Deimos, the Ancient Greek god and personification of dread and terror.
Deimos was discovered by Asaph Hall III at the United States Naval Observatory in Washington, D.C. on 12 August 1877, at about 07:48 UTC.[a] Hall, who also discovered Phobos shortly afterwards, had been specifically searching for Martian moons at the time.
The moon is named after Deimos, a figure representing dread in Greek mythology.[10] The name was suggested by academic Henry Madan, who drew from Book XV of the Iliad, where Ares (the Roman god Mars) summons Dread (Deimos) and Fear (Phobos).[17]
The origin of Mars's moons is unknown and the hypotheses are controversial.[18] The main hypotheses are that they formed either by capture or by accretion. Because of the similarity to the composition of C- or D-type asteroids, one hypothesis is that the moons may be objects captured into Martian orbit from the asteroid belt, with orbits that have been circularized either by atmospheric drag or tidal forces,[19] as capture requires dissipation of energy. The current Martian atmosphere is too thin to capture a Phobos-sized object by atmospheric braking.[18] Geoffrey Landis has pointed out that the capture could have occurred if the original body was a binary asteroid that separated due to tidal forces.[20] The main alternative hypothesis is that the moons accreted in the present position. Another hypothesis is that Mars was once surrounded by many Phobos- and Deimos-sized bodies, perhaps ejected into orbit around it by a collision with a planetesimal.[21][22]
Most recently, Amirhossein Bagheri (ETH Zurich), Amir Khan (ETH Zurich), Michael Efroimsky (US Naval Observatory) and their colleagues proposed a new hypothesis on the origin of the moons. By analyzing the seismic and orbital data from Mars InSight Mission and other missions, they proposed that the moons are born from disruption of a common parent body around 1 to 2.7 billion years ago. The common progenitor of Phobos and Deimos was most probably hit by another object and shattered to form Phobos and Deimos.[23]
Deimos, like Mars' other moon, Phobos, has spectra, albedos, and densities similar to those of a C- or D-type asteroid.[citation needed] Like most bodies of its size, Deimos is highly non-spherical with triaxial dimensions of 15 12.2 11km,[7] making it 56% of the size of Phobos. Deimos is composed of rock rich in carbonaceous material, much like C-type asteroids and carbonaceous chondrite meteorites.[24] It is cratered, but the surface is noticeably smoother than that of Phobos, caused by the partial filling of craters with regolith.[citation needed] The regolith is highly porous and has a radar-estimated density of only 1.471g/cm3.[25]
Escape velocity from Deimos is 5.6m/s.[6] This velocity could theoretically be achieved by a human performing a vertical jump.[26][27] The apparent magnitude of Deimos is 12.45.[8]
Only two geological features on Deimos have been given names. The craters Swift and Voltaire are named after writers who speculated on the existence of two Martian moons before Phobos and Deimos were discovered.[28]
Deimos's orbit is nearly circular and is close to Mars's equatorial plane. Deimos is possibly an asteroid that was perturbed by Jupiter into an orbit that allowed it to be captured by Mars, though this hypothesis is still controversial and disputed.[18] Both Deimos and Phobos have very circular orbits which lie almost exactly in Mars' equatorial plane, and hence a capture origin requires a mechanism for circularizing the initially highly eccentric orbit, and adjusting its inclination into the equatorial plane, most likely by a combination of atmospheric drag and tidal forces;[19] it is not clear that sufficient time was available for this to have occurred for Deimos.[18]
As seen from Mars, Deimos would have an angular diameter of no more than 2.5 minutes (sixty minutes make one degree), one twelfth of the width of the Moon as seen from Earth, and would therefore appear almost star-like to the naked eye.[30] At its brightest ("full moon") it would be about as bright as Venus is from Earth; at the first- or third-quarter phase it would be about as bright as Vega. With a small telescope, a Martian observer could see Deimos's phases, which take 1.2648[31] days (Deimos's synodic period) to run their course.[30]
Unlike Phobos, which orbits so fast that it rises in the west and sets in the east, Deimos rises in the east and sets in the west. The Sun-synodic orbital period of Deimos of about 30.4 hours exceeds the Martian solar day ("sol") of about 24.7 hours by such a small amount that 2.48 days (2.41 sols) elapse between its rising and setting for an equatorial observer. From Deimos-rise to Deimos-rise (or setting to setting), 5.466 days (5.320 sols) elapse.[citation needed]
Because Deimos's orbit is relatively close to Mars and has only a very small inclination to Mars's equator, it cannot be seen from Martian latitudes greater than 82.7.[citation needed]
Deimos's orbit is slowly getting larger, because it is far enough away from Mars and because of tidal acceleration. It is expected to eventually escape Mars's gravity.[32]
Deimos regularly passes in front of the Sun as seen from Mars. It is too small to cause a total eclipse, appearing only as a small black dot moving across the Sun. Its angular diameter is only about 2.5 times the angular diameter of Venus during a transit of Venus from Earth. On 4 March 2004 a transit of Deimos was photographed by Mars rover Opportunity, and on 13 March 2004 a transit was photographed by Mars rover Spirit.[citation needed]
Overall, its exploration history is similar to those of Mars and of Phobos.[33] Deimos has been photographed in close-up by several spacecraft whose primary mission has been to photograph Mars. No landings on Deimos have been made.
The Soviet Phobos program sent two probes to Phobos. In case Phobos 1 succeeded, Phobos 2 could have been sent to Deimos. Both probes launched successfully in July 1988. The first was lost en route to Mars, whereas the second returned some data and images but failed shortly before beginning its detailed examination of Phobos's surface, including a lander.[citation needed]
In 1997 and 1998, the proposed Aladdin mission was selected as a finalist in the NASA Discovery Program. The plan was to visit both Phobos and Deimos, and launch projectiles at the satellites. The probe would collect the ejecta as it performed a slow flyby (~1km/s).[34] These samples would be returned to Earth for study three years later.[35][36] The principal investigator was Carle M. Pieters of Brown University. The total mission cost, including launch vehicle and operations was $247.7 million.[37] Ultimately, the mission chosen to fly was MESSENGER, a probe to the planet Mercury.[38]
In 2008, NASA Glenn Research Center began studying a Phobos and Deimos sample-return mission that would use solar electric propulsion. The study gave rise to the "Hall" mission concept, a New Frontiers-class mission currently under further study.[39]
Also, the sample-return mission called Gulliver has been conceptualized and dedicated to Deimos,[40] in which 1 kilogram (2.2 pounds) of material from Deimos would be returned to Earth.[40]
Another concept of sample-return mission from Phobos and Deimos is OSIRIS-REx2, which would use heritage from the first OSIRIS-REx.[41]
In March 2014, a Discovery class mission was proposed to place an orbiter on Mars orbit by 2021 and study Phobos and Deimos. It is called Phobos And Deimos & Mars Environment (PADME).[42][43]
Human exploration of Deimos could serve as a catalyst for the human exploration of Mars. Recently, it was proposed that the sands of Deimos or Phobos could serve as a valuable material for aerobraking in the colonization of Mars.[44] See Phobos for more detail.
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The Physics of DNA: In Each of Us Lies a Message, Its Beginnings Lost in the Mists of Time – The Daily Galaxy –Great Discoveries Channel
Posted: December 26, 2022 at 10:19 pm
The Physics of DNA: In Each of Us Lies a Message, Its Beginnings Lost in the Mists of Time The Daily Galaxy --Great Discoveries Channel
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Is Applied DNA Sciences Inc (APDN) Stock at the Top of the Diagnostics & Research Industry? – InvestorsObserver
Posted: at 10:19 pm
Is Applied DNA Sciences Inc (APDN) Stock at the Top of the Diagnostics & Research Industry? InvestorsObserver
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Genetic Engineering Principles of Biology
Posted: at 10:08 pm
Genetic engineering is the alteration of an organisms genotype using recombinant DNA technology to modify an organisms DNA to achieve desirable traits. The addition of foreign DNA in the form of recombinant DNA vectors generated by molecular cloning is the most common method of genetic engineering. The organism that receives the recombinant DNA is called a genetically modified organism (GMO). If the foreign DNA that is introduced comes from a different species, the host organism is called transgenic. Bacteria, plants, and animals have been genetically modified since the early 1970s for academic, medical, agricultural, and industrial purposes. In the US, GMOs such as Roundup-ready soybeans and borer-resistant corn are part of many common processed foods.
Although classical methods of studying the function of genes began with a given phenotype and determined the genetic basis of that phenotype, modern techniques allow researchers to start at the DNA sequence level and ask: What does this gene or DNA element do? This technique, called reverse genetics, has resulted in reversing the classic genetic methodology. This method would be similar to damaging a body part to determine its function. An insect that loses a wing cannot fly, which means that the function of the wing is flight. The classical genetic method would compare insects that cannot fly with insects that can fly, and observe that the non-flying insects have lost wings. Similarly, mutating or deleting genes provides researchers with clues about gene function. The methods used to disable gene function are collectively called gene targeting. Gene targeting is the use of recombinant DNA vectors to alter the expression of a particular gene, either by introducing mutations in a gene, or by eliminating the expression of a certain gene by deleting a part or all of the gene sequence from the genome of an organism.
The process of testing for suspected genetic defects before administering treatment is called genetic diagnosis by genetic testing. Depending on the inheritance patterns of a disease-causing gene, family members are advised to undergo genetic testing. For example, women diagnosed with breast cancer are usually advised to have a biopsy so that the medical team can determine the genetic basis of cancer development. Treatment plans are based on the findings of genetic tests that determine the type of cancer. If the cancer is caused by inherited gene mutations, other female relatives are also advised to undergo genetic testing and periodic screening for breast cancer. Genetic testing is also offered for fetuses (or embryos with in vitro fertilization) to determine the presence or absence of disease-causing genes in families with specific debilitating diseases.
Gene therapy is a genetic engineering technique used to cure disease. In its simplest form, it involves the introduction of a good gene at a random location in the genome to aid the cure of a disease that is caused by a mutated gene. The good gene is usually introduced into diseased cells as part of a vector transmitted by a virus that can infect the host cell and deliver the foreign DNA (Figure 1). More advanced forms of gene therapy try to correct the mutation at the original site in the genome, such as is the case with treatment of severe combined immunodeficiency (SCID).
Traditional vaccination strategies use weakened or inactive forms of microorganisms to mount the initial immune response. Modern techniques use the genes of microorganisms cloned into vectors to mass produce the desired antigen. The antigen is then introduced into the body to stimulate the primary immune response and trigger immune memory. Genes cloned from the influenza virus have been used to combat the constantly changing strains of this virus.
Antibiotics are a biotechnological product. They are naturally produced by microorganisms, such as fungi, to attain an advantage over bacterial populations. Antibiotics are produced on a large scale by cultivating and manipulating fungal cells.
Recombinant DNA technology was used to produce large-scale quantities of human insulin in E. coli as early as 1978. Previously, it was only possible to treat diabetes with pig insulin, which caused allergic reactions in humans because of differences in the gene product. Currently, the vast majority of diabetes suffers who inject insulin do so with insulin produced by bacteria.
Human growth hormone (HGH) is used to treat growth disorders in children. The HGH gene was cloned from a cDNA library and inserted into E. coli cells by cloning it into a bacterial vector. Bacterial HGH can be used in humans to reduce symptoms of various growth disorders.
Although several recombinant proteins used in medicine are successfully produced in bacteria, some proteins require a eukaryotic animal host for proper processing. For this reason, the desired genes are cloned and expressed in animals, such as sheep, goats, chickens, and mice. Animals that have been modified to express recombinant DNA are called transgenic animals. Several human proteins are expressed in the milk of transgenic sheep and goats, and some are expressed in the eggs of chickens. Mice have been used extensively for expressing and studying the effects of recombinant genes and mutations.
Manipulating the DNA of plants (i.e., creating GMOs) has helped to create desirable traits, such as disease resistance, herbicide and pesticide resistance, better nutritional value, and better shelf-life (Figure 3). Plants are the most important source of food for the human population. Farmers developed ways to select for plant varieties with desirable traits long before modern-day biotechnology practices were established.
Plants that have received recombinant DNA from other species are called transgenic plants. Because they are not natural, transgenic plants and other GMOs are closely monitored by government agencies to ensure that they are fit for human consumption and do not endanger other plant and animal life. Because foreign genes can spread to other species in the environment, extensive testing is required to ensure ecological stability. Staples like corn, potatoes, and tomatoes were the first crop plants to be genetically engineered.
Gene transfer occurs naturally between species in microbial populations. Many viruses that cause human diseases, such as cancer, act by incorporating their DNA into the human genome. In plants, tumors caused by the bacterium Agrobacterium tumefaciens occur by transfer of DNA from the bacterium to the plant. Although the tumors do not kill the plants, they make the plants stunted and more susceptible to harsh environmental conditions. Many plants, such as walnuts, grapes, nut trees, and beets, are affected by A. tumefaciens. The artificial introduction of DNA into plant cells is more challenging than in animal cells because of the thick plant cell wall.
Researchers used the natural transfer of DNA from Agrobacterium to a plant host to introduce DNA fragments of their choice into plant hosts. In nature, the disease-causing A. tumefaciens have a set of plasmids, called the Ti plasmids (tumor-inducing plasmids), that contain genes for the production of tumors in plants. DNA from the Ti plasmid integrates into the infected plant cells genome. Researchers manipulate the Ti plasmids to remove the tumor-causing genes and insert the desired DNA fragment for transfer into the plant genome. The Ti plasmids carry antibiotic resistance genes to aid selection and can be propagated in E. coli cells as well.
Bacillus thuringiensis (Bt) is a bacterium that produces protein crystals during sporulation that are toxic to many insect species that affect plants. Bt toxin has to be ingested by insects for the toxin to be activated. Insects that have eaten Bt toxin stop feeding on the plants within a few hours. After the toxin is activated in the intestines of the insects, death occurs within a couple of days. Modern biotechnology has allowed plants to encode their own crystal Bt toxin that acts against insects. The crystal toxin genes have been cloned from Bt and introduced into plants. Bt toxin has been found to be safe for the environment, non-toxic to humans and other mammals, and is approved for use by organic farmers as a natural insecticide.
The first GM crop to be introduced into the market was the Flavr Savr Tomato produced in 1994. Antisense RNA technology was used to slow down the process of softening and rotting caused by fungal infections, which led to increased shelf life of the GM tomatoes. Additional genetic modification improved the flavor of this tomato. The Flavr Savr tomato did not successfully stay in the market because of problems maintaining and shipping the crop.
Unless otherwise noted, images on this page are licensed under CC-BY 4.0 by OpenStax.
OpenStax, Biology. OpenStax CNX. May 27, 2016 http://cnx.org/contents/s8Hh0oOc@9.10:8CA_YwJq@3/Cloning-and-Genetic-Engineerin
Moen I, Jevne C, Kalland K-H, Chekenya M, Akslen LA, Sleire L, Enger P, Reed RK, Oyan AM, Stuhr LEB. 2012.Gene expression in tumor cells and stroma in dsRed 4T1 tumors in eGFP-expressing mice with and without enhanced oxygenation.BMC Cancer. 12:21. doi:10.1186/1471-2407-12-21 PDF
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Engineering the Perfect Baby | MIT Technology Review
Posted: at 10:08 pm
Indeed, some people are adamant that germ-line engineering is being pushed ahead with false arguments. That is the view of Edward Lanphier, CEO of Sangamo Biosciences, a California biotechnology company that is using another gene-editing technique, called zinc fingers nucleases, to try to treat HIV in adults by altering their blood cells. Weve looked at [germ-line engineering] for a disease rationale, and there is none, he says. You can do it. But there really isnt a medical reason. People say, well, we dont want children born with this, or born with thatbut its a completely false argument and a slippery slope toward much more unacceptable uses.
Critics cite a host of fears. Children would be the subject of experiments. Parents would be influenced by genetic advertising from IVF clinics. Germ-line engineering would encourage the spread of allegedly superior traits. And it would affect people not yet born, without their being able to agree to it. The American Medical Association, for instance, holds that germ-line engineering shouldnt be done at this time because it affects the welfare of future generations and could cause unpredictable and irreversible results. But like a lot of official statements that forbid changing the genome, the AMAs, which was last updated in 1996, predates todays technology. A lot of people just agreed to these statements, says Greely. It wasnt hard to renounce something that you couldnt do.
The fear? A dystopia of superpeople and designer babies for those who can afford it.
Others predict that hard-to-oppose medical uses will be identified. A couple with several genetic diseases at once might not be able to find a suitable embryo. Treating infertility is another possibility. Some men dont produce any sperm, a condition called azoospermia. One cause is a genetic defect in which a region of about one million to six million DNA letters is missing from the Y chromosome. It might be possible to take a skin cell from such a man, turn it into a stem cell, repair the DNA, and then make sperm, says Werner Neuhausser, a young Austrian doctor who splits his time between the Boston IVF fertility-clinic network and Harvards Stem Cell Institute. That will change medicine forever, right? You could cure infertility, that is for sure, he says.
I spoke with Church several times by telephone over the last few months, and he told me whats driving everything is the incredible specificity of CRISPR. Although not all the details have been worked out, he thinks the technology could replace DNA letters essentially without side effects. He says this is what makes it tempting to use. Church says his laboratory is focused mostly on experiments in engineering animals. He added that his lab would not make or edit human embryos, calling such a step not our style.
What is Churchs style is human enhancement. And hes been making a broad case that CRISPR can do more than eliminate disease genes. It can lead to augmentation. At meetings, some involving groups of transhumanists interested in next steps for human evolution, Church likes to show a slide on which he lists naturally occurring variants of around 10 genes that, when people are born with them, confer extraordinary qualities or resistance to disease. One makes your bones so hard theyll break a surgical drill. Another drastically cuts the risk of heart attacks. And a variant of the gene for the amyloid precursor protein, or APP, was found by Icelandic researchers to protect against Alzheimers. People with it never get dementia and remain sharp into old age.
Church thinks CRISPR could be used to provide people with favorable versions of genes, making DNA edits that would act as vaccines against some of the most common diseases we face today. Although he told me anything edgy should be done only to adults who can consent, its obvious to him that the earlier such interventions occur, the better.
Church tends to dodge questions about genetically modified babies. The idea of improving the human species has always had enormously bad press, he wrote in the introduction to Regenesis, his 2012 book on synthetic biology, whose cover was a painting by Eustache Le Sueur of a bearded God creating the world. But thats ultimately what hes suggesting: enhancements in the form of protective genes. An argument will be made that the ultimate prevention is that the earlier you go, the better the prevention, he told an audience at MITs Media Lab last spring. I do think its the ultimate preventive, if we get to the point where its very inexpensive, extremely safe, and very predictable. Church, who has a less cautious side, proceeded to tell the audience that he thought changing genes is going to get to the point where its like you are doing the equivalent of cosmetic surgery.
Some thinkers have concluded that we should not pass up the chance to make improvements to our species. The human genome is not perfect, says John Harris, a bioethicist at Manchester University, in the U.K. Its ethically imperative to positively support this technology. By some measures, U.S. public opinion is not particularly negative toward the idea. A Pew Research survey carried out last August found that 46 percent of adults approved of genetic modification of babies to reduce the risk of serious diseases.
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Emma Thompson On Longevity Of Holiday Fave Love Actually But It Is SEX Actually That Is Earning Her Awards Buzz In Leo Grande – Deadline
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Retiring History Theatre artistic director Ron Peluso looks back at fond moments from his 27 years on the job – St. Paul Pioneer Press
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Retiring History Theatre artistic director Ron Peluso looks back at fond moments from his 27 years on the job St. Paul Pioneer Press
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Retiring History Theatre artistic director Ron Peluso looks back at fond moments from his 27 years on the job - St. Paul Pioneer Press
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