-Caveat Lector-

  The Dangers of Genetic Engineering
by Dr. Mae-Wan Ho


As one of the many scientists presenting evidence to the Royal
Commission on Genetic Engineering, I had high hopes that New
Zealand would assume moral and intellectual leadership in rejecting
this dangerous technology bolstered by degenerate science, so
obviously serving the corporate agenda instead of the public good.

It has become increasingly evident that GM technology is inherently
hazardous and unreliable both in agriculture and in medicine. The
list of failures is growing apace. Let me mention a few recent
examples that came to light since I presented evidence to the
Commission.

GM crops are inherently unstable, and this is fully borne out by
numerous new scientific publications. Even the top 'success',
Roundup Ready soy, is showing every sign of breakdown: reduced
yield, non-germination, diseases and infestation by new pests.

Molecular genetic characterization, the first ever done on any
commercially grown GM crop so far, has confirmed that both the GM
construct of Roundup Ready soy and the host genome have been
scrambled (rearranged), and hundreds of basepairs of unknown DNA
has got in as well.

The 'next generation' crops are even worse. I draw your attention
especially to those developed with terminator technologies aimed at
protecting corporate patents and preventing farmers from saving and
replanting seeds. Many are currently field tested and commercially
grown as 'male sterile' crops.

Not only are the constructs more complicated and hence more
unstable and prone to horizontal gene transfer, the gene products
used are cell poisons or recombinases, ie, genome scramblers.
Female-sterile and even male-sterile genes (yes!) are being spread
via pollen. These dangerous genes will spread and wipe out other
crops as well as wild plant species.

It has become all too clear that GM agriculture cannot co-exist
with other forms of agriculture. Bees are known to travel up to10km
or more in foraging for pollen.

There is no way to prevent the horizontal spread of GM constructs
to unrelated species, which can occur in all environments,
including the digestive and respiratory tracts of animals.

There are both sound a priori reasons as well as empirical evidence
to support my contention, shared by other scientists that GM
constructs may more likely spread horizontally than non-manipulated
DNA. Let me reiterate them here.

GM constructs are designed to cross species barriers and invade
genomes. They possess homologies to a wide combination of viral and
bacterial DNA and are hence much more likely to recombine with, and
transfer genes to all those agents.

GM constructs are well known to be structurally unstable and hence
prone to fragment and recombine. Some constructs such as those with
the CaMV 35S promoter are extra unstable on account of the presence
of recombination hotspots.

I have mentioned the now abundant empirical evidence of structural
instability of transgenic DNA and trangenic plants above. The CaMV
35S promoter has been shown to be extra unstable in GM crops. And
horizontal transfer of transgenic DNA has been demonstrated both in
the laboratory and in the field.

I note from your report that Dr Daniel Cohen, a plant scientist in
the Plant Health and Development group of HortResearch, had
attempted to refute my warnings about the CaMV 35S promoter.

But he, like other GM proponents, had failed to counter my point
that the isolated, recombined CaMV 35S promoter cannot be equated
with the promoter in the intact viral genome or the intact virus.

The intact viral genome had evolved over millions of years. The
host range of the virus itself is restricted to the cabbage family,
and it has a well-tried and tested life cycle in the host cell that
does not require integration into the host genome. The fact that no
transfer from the virus into the plant genome has taken place in
the course of evolution attests to the effective biological
barriers that keep species distinct.

The same promoter, removed from the viral genome and put next to
strange genes in the GM construct, is entirely different. It now
functions promiscuously across the living world, including animal
and human cells.

Its destabilizing effect on GM crops is such that many scientists,
including those who pioneered its use, are now phasing it out.
There is no justification for releasing any GM crop containing the
CaMV35S promoter into the environment.

I note that you have approved the field release of GM tamarillo
(Cyphomandra betacea) for resistance to tamarillo mosaic virus at
Kerikeri Research Station. This crop not only contains CaMV 35S
promoter, but also has a kanamycin resistance marker gene.

The approval of this marker gene was a regulatory blunder committed
in the United States and elsewhere, as it is clear that kanamycin
is still widely in clinical use, and the marker gene confers
resistance to new generation aminoglycosides as well. There is also
plenty of evidence that GM crops with viral genes are prone to give
rise to recombinant viruses, some of which more virulent than the
'wild type'.

When I first drew attention to horizontal gene transfer in 1995,
proponents of GM technology reacted by denying it exists. Now they,
like Dr. Daniel Cohen, are saying it does not matter because it is
a natural process.

Horizontal gene transfer may have occurred in our evolutionary
past, but GM constructs are anything but natural. They are
synthetic genes and new combinations of genes that have never
existed in billions of years of evolution, and cannot in any sense
be regarded as natural.

And, I am afraid, the GM proponents will have to change their tune
again; for a rigorous reanalysis of the human genome and other data
has failed to substantiate the claim that the human genome has 113
to 226 bacterial genes transferred into it.

The actual number could well be no more than a few, or none at all.
What is the lesson? Precisely as I have always said, horizontal
gene transfer does not readily happen without genetic engineering.

Genetic engineering enhances it, with dangerous consequences.

In biomedical applications, the gene-centered approach is equally
misplaced and pernicious. So-called 'health genomics' is a drain on
our intellectual and financial resources. It is preventing us from
addressing the real, overwhelming causes of ill health: poverty,
malnutrition, social injustice and environmental pollution.

It is stigmatizing and victimizing those most in need of care and
treatment, and making even the most unethical applications, such as
human cloning and 'therapeutic human cloning', seem compelling.

Furthermore, the 'cures' on offer are literally deadly. The toll
from 'gene therapy' trials so far is at least 6 deaths and more
than 650 adverse events.

It is now admitted that gene therapy has been oversold by the
scientists themselves. Presumed stem cells from human fetuses
transplanted into the brain of 5 Parkinson's patients turned into
an irredeemable nightmare because the cells grew uncontrollably.

The latest verdict from an international team of cloners is that
mice embryonic stem cells are uncontrollably variable in culture,
the clones themselves are also subject to uncontrollable and
unpredictable variations and defects.

And xenotransplantation is widely condemned because there is clear
evidence that endogenous viruses from animal organs can cross into
humans.

New lethal viruses continue to be created in genetic engineering
labs, some of the latest being SHIVs, hybrids of human and monkey
AIDS viruses that can infect both.

Finally, AIDS virologists have issued serious warning against AIDS
vaccines that undermine the immune system, making it more
susceptible to viral infections, and have the potential to generate
lethal viruses and bacteria in the vaccinated populations.

A sweeping paradigm change is long overdue if we are to survive the
destruction that reductionist science and technology have wrought
on us and on our planet.

We have all the means to deliver genuine health and food security
to the world without using GM technology and going against the
wishes of the vast majority of people.

Only the political will is missing.

Dr. Mae-Wan Ho, Director; Institute of Science in Society; PO Box
32097 London; NW1 0XR UK

Email: [EMAIL PROTECTED]


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Related Articles:

Suppressing Dissent in Science With GM Foods

Hazards of Genetically Engineered Food

GMO Crops Are An Accident Waiting to Happen


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