Thursday, 31 July 2014

Father’s Lifestyle Affects Future Offspring


Father’s Lifestyle Affects Future Offspring

No Sex Required: Body Cells Transfer Genetic Info Directly Into Sperm Cells, Amazing Study Finds

 

No Sex Required: Body Cells Transfer Genetic Info Directly Into Sperm Cells, Amazing Study Finds


By Sayer Ji


 A revolutionary new study reveals that the core tenet of classical genetics is patently false, and by implication: what we do in this life -- our diet, our mindset, our chemical exposures -- can directly impact the DNA and health of future generations.


A paradigm shifting new study titled, "Soma-to-Germline Transmission of RNA in Mice Xenografted with Human Tumour Cells: Possible Transport by Exosomes," promises to overturn several core tenets of classical genetics, including collapsing the timescale necessary for the transfer of genetic information through the germline of a species (e.g. sperm) from hundreds of thousands of years to what amounts to 'real time' changes in biological systems.

In classical genetics, Mendelian laws specify that the inheritance of traits passed from one generation to the next can only occur through sexual reproduction as information is passed down through the chromosomes of a species' germline cells (egg and sperm), and never through somatic (bodily) cells.  Genetic change, according to this deeply entrenched view, can take hundreds, thousands and even millions of generations to manifest.

The new study, however, has uncovered a novel mechanism through which somatic-to-germline transmission of genetic information is made possible.  Mice grafted with human melanoma tumor cells genetically manipulated to express genes for a fluorescent tracer enzyme (EGFP-encoding plasmid) were found to release information-containing molecules containing the EGFP tracer into the animals' blood; since EGFP is a non-human and non-murine expressed tracer, there was little doubt that the observed phenomenon was real. These EGFP trackable molecules included exosomes (small nanoparticles produced by all eukaryotic cells (including plants and animals), which contain RNA and DNA molecules), which were verified to deliver RNAs to mature sperm cells (spermatozoa) and remain stored there.  The authors of the study pointed out that RNA of this kind has been found in mouse models to behave as a "transgenerational determinant of inheritable epigenetic variations and that spermatozoal RNA can carry and deliver information that cause phenotypic variations in the progeny."

The researchers concluded that their study's findings strongly suggest, "exosomes are the carriers of a flow of information from somatic cells to gametes," and that their "results indicate that somatic RNA is transferred to sperm cells, which can therefore act as the final recipients of somatic cell-derived information."

 

Breaking Through Weismann's Genetic Barrier

 

These findings overturn the so-called Weismann barrier, a principle proposed by the German evolutionary biologist August Weismann (1834 – 1914), that states hereditary information can only move from genes to body cells, and not the other way around, which has long been considered a nail in the coffin of the Lamarkian concept that an organism can pass on characteristics it has acquired during its lifetime to its offspring.

Over the past decade, however, the seeming impenetrability of the Weismann barrier has increasingly been called into question, due to a growing body of evidence that epigenetic patterns of gene expression (e.g. histone modifications, gene silencing via methylation) can be transferred across generations without requiring changes in the primary DNA sequences of our genomes; as well as the discovery that certain viruses contain the enzyme reverse transcriptase, which is capable of inscribing RNA-based information directly into our DNA, including germline cells, as is the case for endogenous retroviruses, which are believed responsible for about 5% of the nucleotide sequences in our genome. Nonetheless, as the authors of the new study point out, until their study, "no instance of transmission of DNA- or RNA-mediated information from somatic to germ cells has been reported as yet."

The researchers further expanded on the implications of their findings:

"Work from our and other laboratories indicates that spermatozoa act as vectors not only of their own genome, but also of foreign genetic information, based on their spontaneous ability to take up exogenous DNA and RNA molecules that are then delivered to oocytes at fertilization with the ensuing generation of phenotypically modified animals [35][37]. In cases in which this has been thoroughly investigated, the sperm-delivered sequences have been seen to remain extrachromosomal and to be sexually transmitted to the next generation in a non-Mendelian fashion [38]. The modes of genetic information delivery in this process are closely reminiscent of those operating in RNA-mediated paramutation inheritance, whereby RNA is the determinant of inheritable epigenetic variations [16], [17]. In conclusion, this work reveals that a flow of information can be transferred from the soma to the germline, escaping the principle of the Weismann barrier [39] which postulates that somatically acquired genetic variations cannot be transferred to the germline."

The implications of research on exosome-mediated information transfer are wide ranging. First, if your somatic cells, which are continually affected by your nutritional, environmental, lifestyle and even mind-body processes, can transfer genetic information through exosomes to the DNA within your germline cells, then your moment-to-moment decisions, behaviors, experiences, toxin and toxicant exposures, could theoretically affect the biological 'destinies' of your offspring, and their offspring, stretching on into the distant future. 

Exosome research also opens up promising possibilities in the realm of nutrigenomics and 'food as medicine.' A recent study found common plant foods, e.g. ginger, grapefruit, grapes, produce exosomes that, following digestion, enter human blood undegraded and subsequently down-regulate inflammatory pathways in the human body in a manner confirming some of their traditional folkloric medicinal uses.  If the somatic cells within our body are capable through extrachromosomal processes of modulating fundamental genetic processes within the germline cells, or, furthermore, if foods that we eat are also capable of acting as vectors of gene-regulatory information, truly the old reductionist, mechanistic, unilinear models of genetics must be abandoned in favor of a view that accounts for the vital importance of all our decisions, nutritional factors, environmental exposures, etc., in determining the course, not only of our bodily health, but the health of countless future generations as well.


From Green Med Info @ http://www.greenmedinfo.com/blog/no-sex-required-body-cells-transfer-genetic-info-directly-sperm-cells-amazing




Hereditary trauma: Inheritance of traumas and how they may be mediated


The consequences of traumatic experiences can be passed on from one generation to the next. [Click to enlarge image]


Extreme and traumatic events can change a person -- and often, years later, even affect their children. Researchers of the University of Zurich and ETH Zurich have now unmasked a piece in the puzzle of how the inheritance of traumas may be mediated.

The phenomenon has long been known in psychology: traumatic experiences can induce behavioural disorders that are passed down from one generation to the next. It is only recently that scientists have begun to understand the physiological processes underlying hereditary trauma. "There are diseases such as bipolar disorder, that run in families but can't be traced back to a particular gene," explains Isabelle Mansuy, professor at ETH Zurich and the University of Zurich. With her research group at the Brain Research Institute of the University of Zurich, she has been studying the molecular processes involved in non-genetic inheritance of behavioural symptoms induced by traumatic experiences in early life.

Mansuy and her team have succeeded in identifying a key component of these processes: short RNA molecules. These RNAs are synthetized from genetic information (DNA) by enzymes that read specific sections of the DNA (genes) and use them as template to produce corresponding RNAs. Other enzymes then trim these RNAs into mature forms. Cells naturally contain a large number of different short RNA molecules called microRNAs. They have regulatory functions, such as controlling how many copies of a particular protein are made.


Small RNAs with a huge impact

The researchers studied the number and kind of microRNAs expressed by adult mice exposed to traumatic conditions in early life and compared them with non-traumatized mice. They discovered that traumatic stress alters the amount of several microRNAs in the blood, brain and sperm -- while some microRNAs were produced in excess, others were lower than in the corresponding tissues or cells of control animals. These alterations resulted in misregulation of cellular processes normally controlled by these microRNAs.

After traumatic experiences, the mice behaved markedly differently: they partly lost their natural aversion to open spaces and bright light and had depressive-like behaviours. These behavioural symptoms were also transferred to the next generation via sperm, even though the offspring were not exposed to any traumatic stress themselves.

Even passed on to the third generation

The metabolism of the offspring of stressed mice was also impaired: their insulin and blood-sugar levels were lower than in the offspring of non-traumatized parents. "We were able to demonstrate for the first time that traumatic experiences affect metabolism in the long-term and that these changes are hereditary," says Mansuy. The effects on metabolism and behaviour even persisted in the third generation.

"With the imbalance in microRNAs in sperm, we have discovered a key factor through which trauma can be passed on," explains Mansuy. However, certain questions remain open, such as how the dysregulation in short RNAs comes about. "Most likely, it is part of a chain of events that begins with the body producing too much stress hormones."

Importantly, acquired traits other than those induced by trauma could also be inherited through similar mechanisms, the researcher suspects. "The environment leaves traces on the brain, on organs and also on gametes. Through gametes, these traces can be passed to the next generation."

Mansuy and her team are currently studying the role of short RNAs in trauma inheritance in humans. As they were also able to demonstrate the microRNAs imbalance in the blood of traumatized mice and their offspring, the scientists hope that their results may be useful to develop a blood test for diagnostics.



Story Source:

The above story is based on materials provided by ETH Zurich. Note: Materials may be edited for content and length.

Journal Reference:
1.     Gapp K, Jawaid A, Sarkies P, Bohacek J, Pelczar P, Prados J, Farinelli L, Miska E, Mansuy IM. Implication of sperm RNAs in transgenerational inheritance of the effects of early trauma in mice. Nature Neuroscience, April 13, 2014 DOI: 10.1038/nn.3695
2.      


From Science Daily @ http://www.sciencedaily.com/releases/2014/04/140413135953.htm#.U8DBHgn2LXM.email


For more information about epigenetics see http://nexusilluminati.blogspot.com/search/label/epigenetics
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Wednesday, 30 July 2014

Mindwarp Warning: Are Nuclear Power Plants Secretly Manufacturing Gold?


Mindwarp Warning: Are Nuclear Power Plants Secretly Manufacturing Gold?




By G. Hunter


With precious metal prices constantly on the rise, I've been exploring the possibility of making some of my own gold. Making gold is not as difficult as you would imagine, all you need is one alchemist with specific esoteric knowledge or, more realistically, a nuclear reactor capable of nuclear transmutation.

Transmutation of the elements has been explored by men and women a lot longer that you think, while modern methods of transmutation have become simpler due to technological innovations - innovations that are often misleading as to what their true capabilities are.

Video Description: In March of 1924 Man Discovered the Secret of Alchemy. Since 1954, 31 countries have built 435 nuclear power plants. I'd say all of them were designed to perform this operation. Generating electricity may not be the primary use, as we have been told. They have had the ability to commercially produce gold for 58 years. 24 hours a day, 7 days a week. There really is no telling how much they have stockpiled... Mercury's current market price = $1.25 oz. / Gold is $1,655 oz.

In March 1924, at the Tokyo Imperial University, Professor Hantaro Nagaoka directed 150,000 volts of electricity at a mercury isotope under a dialectic layer of paraffin oil for four hours in an early experiment with nuclear energy. The purpose was to strike out a hydrogen proton from the nucleus of the mercury and produce a new element, gold. Mercury has 80 protons. Gold, meanwhile, has 79 protons — you see where I’m going with this. The experiment was a success. Professor Hantaro Nagaoka solved the mystery that eluded scientists for centuries, the mystery of the Philosopher’s Stone.

The Philosopher’s Stone is the idea that you could have a magical material that could turn lead, or some very inexpensive metal, into gold. For thousands of years, kings sought out this mythical device, one that could create gold out of common metals. Scientists and alchemists for centuries have been trying to invent one. Even Sir Isaac Newton obsessed over the mystery of the Philosopher’s Stone in the 17th century. However, the English feared the potential devaluation of gold and made the practice of alchemy punishable by death.

http://www.crystalinks.com/philosopherstone571.jpg
Image: http://www.crystalinks.com/philosopherstone.gif


Fast forward now a few centuries to present day.

If we wish to manufacture gold, the most helpful metal to start with is mercury. Gold is element 79 and mercury is element 80, which means that there is only a slight difference between their atomic structures. The mercury atom has one more proton in its nucleus and the corresponding electron in the outer (known as F shell) orbit.

[atommercuryandgold.jpg]

As the diagram shows, all other shells (from atom A to E) have the same number of electrons in both mercury and gold. So, theoretically, if we can expel one proton from the nucleus of an atom of mercury, we have transmuted it into an atom of gold. The process is difficult since an atom of mercury has eighty electrons; eighty orbits have to be broken through as well as the electric field round the nucleus. The first experiment was, however, carried out years ago at the Physical-Technical State Institute of Berlin. The bombarding particles were given a high speed by means of a field of 30,000 volts, and a small, but observable quantity of gold was produced from quicksilver. Unfortunately, such laboratory transmutation can never be reproduced on a commercial scale.

It is tempting to laugh off medieval alchemists as greedy eccentrics, who sought methods for forming gold out of cheaper metals. But one ought to give them credit for what they did in the process of searching. These alchemists discovered strong acids like hydrochloric acid, nitric acid and sulfuric acid which are far more useful today then gold could possibly be. The alchemists should have been acclaimed for these revolutionary discoveries. Instead they were sneered at for their failure to make gold out of plentiful metals like mercury.

Before Chemistry was a science, there was Alchemy. One of the supreme quests of alchemy is to transmute lead into gold. Lead (atomic number 82) and gold (atomic number 79) are defined as elements by the number of protons they possess. Changing the element requires changing the atomic (proton) number. The number of protons cannot be altered by any chemical means. However, physics may be used to add or remove protons and thereby change one element into another. Because lead is stable, forcing it to release three protons requires a vast input of energy, such that the cost of transmuting it greatly surpasses the value of the resulting gold.


How to make Gold from Mercury

  • First, get some mercury. The kind we want is Hg-196, a naturally occurring isotope with 80 protons and 116 neutrons in its nucleus. The 80 protons are what make it mercury. Gold, meanwhile, has 79 protons — you see where I’m going with this. Finding sufficient Hg-196 could take some doing, though, as only 0.15 percent of mercury is in this form.

  • Slam a slow neutron into it. Initially I was unsure how one went about this. The journals said the desired type of neutron had an energy level in the thermal range. This to me suggested you could just heat up a can of neutrons on the stove and drop in some mercury. However, I suspected subtleties were being overlooked. I set this matter aside for further study.

  • The slow neutron is captured by the nucleus of the Hg-196. This turns it into Hg-197, with 80 protons and 117 neutrons. Hg-197 is unstable. In 64.14 hours, give or take, electron capture occurs. This means the Hg-197 grabs an electron from a low-hanging shell, combines it with a proton to make a neutron, and kicks out a neutrino.

  • Discard the neutrino. We have no need of it.

  • The Hg-197 has now turned into something with 79 protons and 118 neutrons. Do you know what this? I’ll tell you. It’s Au-197, the only stable isotope of gold.

  • Repeat five zillion times, until you have enough gold to make an ingot. Success! However, if you didn’t do so earlier, you must now separate the stable gold deriving from Hg-196 from the unwanted crud deriving from the rest of the mercury, which I remind you constitutes 99.85 percent of what’s out there and a good chunk of which I’ll bet is now radioactive. So it could be a long afternoon.


What about Lead?

Transmutation of lead into gold isn't just theoretically possible
- it has been achieved as well. There are reports that Glenn Seaborg, 1951 Nobel Laureate in Chemistry, succeeded in transmuting a minute quantity of lead (possibly en route from bismuth, in 1980) into gold. There is an earlier report (1972) in which Soviet physicists at a nuclear research facility near Lake Baikal in Siberia accidentally discovered a reaction for turning lead into gold when they found the lead shielding of an experimental reactor had changed to gold.

Today particle accelerators routinely transmute elements. A charged particle is accelerated using electrical and/or magnetic fields. In a linear accelerator, the charged particles drift through a series of charged tubes separated by gaps. Every time the particle emerges between gaps, it is accelerated by the potential difference between adjacent segments. In a circular accelerator, magnetic fields accelerate particles moving in circular paths. In either case, the accelerated particle impacts a target material, potentially knocking free protons or neutrons and making a new element or isotope. Nuclear reactors also may used for creating elements, although the conditions are less controlled.

In nature, new elements are created by adding protons and neutrons to hydrogen atoms within the nuclear reactor of a star, producing increasingly heavier elements, up to iron (atomic number 26). This process is called nucleosynthesis. Elements heavier than iron are formed in the stellar explosion of a supernova. In a supernova gold may be made into lead, but not the other way around.

While it may never be commonplace to transmute lead into gold, it is practical to obtain gold from lead ores. The minerals galena (lead sulfide, PbS), cerussite (lead carbonate, PbCO3), and anglesite (lead sulfate, PbSO4) often contain zinc, gold, silver, and other metals. Once the ore has been pulverized, chemical techniques are sufficient to separate the gold from the lead. The result is almost alchemy...almost.



From Apparently Apparel @ http://www.apparentlyapparel.com/news/are-nuclear-power-plants-secretly-manufacturing-gold


For more information about nuclear transmutation see http://nexusilluminati.blogspot.com/search/label/nuclear%20transmutation  
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