[CTRL] The Prion Diseases

[Steve Wingate]

-Caveat Lector-

The Prion Diseases

http://www.sciam.com/0896issue/prion.html

Prions, once dismissed as an impossibility, have now gained wide
recognition as extraordinary agents that cause a number of infectious,
genetic and spontaneous disorders

by Stanley B. Prusiner


FURTHER READING Fifteen years ago I evoked a good deal of
skepticism when I proposed that the infectious agents causing certain
degenerative disorders of the central nervous system in animals and, more
rarely, in humans might consist of protein and nothing else. At the time, the
notion was heretical. Dogma held that the conveyers of transmissible
diseases required genetic material, composed of nucleic acid (DNA or
RNA), in order to establish an infection in a host. Even viruses, among the
simplest microbes, rely on such material to direct synthesis of the proteins
needed for survival and replication.

Later, many scientists were similarly dubious when my colleagues and I
suggested that these "proteinaceous infectious particles"-or "prions," as I
called the disease-causing agents-could underlie inherited, as well as
communicable, diseases. Such dual behavior was then unknown to
medical science. And we met resistance again when we concluded that
prions (pronounced "pree-ons") multiply in an incredible way; they convert
normal protein molecules into dangerous ones simply by inducing the
benign molecules to change their shape.

Today, however, a wealth of experimental and clinical data has made a
convincing case that we are correct on all three counts. Prions are indeed
responsible for transmissible and inherited disorders of protein
conformation. They can also cause sporadic disease, in which neither
transmission between individuals nor inheritance is evident. Moreover,
there are hints that the prions causing the diseases explored thus far may
not be the only ones. Prions made of rather different proteins may
contribute to other neurodegenerative diseases that are quite prevalent in
humans. They might even participate in illnesses that attack muscles.

The known prion diseases, all fatal, are sometimes referred to as
spongiform encephalopathies. They are so named because they frequently
cause the brain to become riddled with holes. These ills, which can brew
for years (or even for decades in humans) are widespread in animals.

The most common form is scrapie, found in sheep and goats. AfBicted
animals lose coordination and eventually become so incapacitated that
they cannot stand. They also become irritable and, in some cases, develop
an intense itch that leads them to scrape off their wool or hair (hence the
name "scrapie"). The other prion diseases of animals go by such names
as transmissible mink encephalopathy, chronic wasting disease of mule
deer and elk, feline spongiform encephalopathy and bovine spongiform
encephalopathy. The last, often called mad cow disease, is the most
worrisome.

Gerald A. H. Wells and John W. Wilesmith of the Central Veterinary
Laboratory in Weybridge, England, identified the condition in 1986, after it
began striking cows in Great Britain, causing them to became
uncoordinated and unusually apprehensive. The source of the emerging
epidemic was soon traced to a food supplement that included meat and
bone meal from dead sheep. The methods for processing sheep
carcasses had been changed in the late 1970s. Where once they would
have eliminated the scrapie agent in the supplement, now they apparently
did not. The British government banned the use of animal-derived feed
supplements in 1988, and the epidemic has probably peaked.
Nevertheless, many people continue to worry that they will eventually fall ill
as a result of having consumed tainted meat.

The human prion diseases are more obscure. Kuru has been seen only
among the Fore highlanders of Papua New Guinea. They call it the
"laughing death." Vincent Zigas of the Australian Public Health Service and
D. Carleton Gajdusek of the U.S. National Institutes of Health described it
in 1957, noting that many highlanders became aUeicted with a strange,
fatal disease marked by loss of coordination (ataxia) and often later by
dementia. The affected individuals probably acquired kuru through ritual
cannibalism: the Fore tribe reportedly honored the dead by eating their
brains. The practice has since stopped, and kuru has virtually disappeared.


Creutzfeldt-Jakob disease, in contrast, occurs worldwide and usually
becomes evident as dementia. Most of the time it appears sporadically,
striking one person in a million, typically around age 60. About 10 to 15
percent of cases are inherited, and a small number are, sadly, iatrogenic-
spread inadvertently by the attempt to treat some other medical problem.
Iatrogenic Creutzfeldt-Jakob disease has apparently been transmitted by
corneal transplantation, implantation of dura mater or electrodes in the
brain, use of contaminated surgical instruments, and injection of growth
hormone derived from human pituitaries (before recombinant growth
hormone became available).

The two remaining human disorders are Gerstmann-Str...ussler-Scheinker
disease (which is manifest as ataxia and other signs of damage to the
cerebellum) and fatal familial insomnia (in which dementia follows diUculty
sleeping). Both these conditions are usually inherited and typically appear
in midlife. Fatal familial insomnia was discovered only recently, by Elio
Lugaresi and Rossella Medori of the University of Bologna and Pierluigi
Gambetti of Case Western Reserve University.

In Search of the Cause

I first became intrigued by the prion diseases in 1972, when as a resident
in neurology at the University of California School of Medicine at San
Francisco, I lost a patient to Creutzfeldt-Jakob disease. As I reviewed the
scientific literature on that and related conditions, I learned that scrapie,
Creutzfeldt-Jakob disease and kuru had all been shown to be transmissible
by injecting extracts of diseased brains into the brains of healthy animals.
The infections were thought to be caused by a slow-acting virus, yet no one
had managed to isolate the culprit.

In the course of reading, I came across an astonishing report in which
Tikvah Alper and her colleagues at the Hammersmith Hospital in London
suggested that the scrapie agent might lack nucleic acid, which usually can
be degraded by ultraviolet or ionizing radiation. When the nucleic acid in
extracts of scrapie-infected brains was presumably destroyed by those
treatments, the extracts retained their ability to transmit scrapie. If the
organism did lack DNA and RNA, the finding would mean that it was not a
virus or any other known type of infectious agent, all of which contain
genetic material. What, then, was it? Investigators had many ideas-
including, jokingly, linoleum and kryptonite-but no hard answers.

I immediately began trying to solve this mystery when I set up a laboratory
at U.C.S.F. in 1974. The first step had to be a mechanical one-purifying the
infectious material in scrapie-infected brains so that its composition could
be analyzed. The task was daunting; many investigators had tried and
failed in the past. But with the optimism of youth, I forged ahead [see
"Prions," by Stanley B. Prusiner; SCIENTIFIC AMERICAN, October 1984].
By 1982 my colleagues and I had made good progress, producing extracts
of hamster brains consisting almost exclusively of infectious material. We
had, furthermore, subjected the extracts to a range of tests designed to
reveal the composition of the disease-causing component.

Amazing Discovery

All our results pointed toward one startling conclusion: the infectious agent
in scrapie (and presumably in the related diseases) did indeed lack nucleic
acid and consisted mainly, if not exclusively, of protein. We deduced that
DNA and RNA were absent because, like Alper, we saw that procedures
known to damage nucleic acid did not reduce infectivity. And we knew
protein was an essential component because procedures that denature
(unfold) or degrade protein reduced infectivity. I thus introduced the term
"prion" to distinguish this class of disease conveyer from viruses, bacteria,
fungi and other known pathogens. Not long afterward, we determined that
scrapie prions contained a single protein that we called PrP, for "prion
protein."

Now the major question became, Where did the instructions specifying the
sequence of amino acids in PrP reside? Were they carried by an
undetected piece of DNA that traveled with PrP, or were they, perhaps,
contained in a gene housed in the chromosomes of cells? The key to this
riddle was the identification in 1984 of some 15 amino acids at one end of
the PrP protein. My group identified this short amino acid sequence in
collaboration with Leroy E. Hood and his co-workers at the California
Institute of Technology.

Knowledge of the sequence allowed us and others to construct molecular
probes, or detectors, able to indicate whether mammalian cells carried the
PrP gene. With probes produced by Hood's team, Bruno Oesch, working in
the laboratory of Charles Weissmann at the University of Zurich, showed
that hamster cells do contain a gene for PrP. At about the same time,
Bruce Cheseboro of the NIH Rocky Mountain Laboratories made his own
probes and established that mouse cells harbor the gene as well. That
work made it possible to isolate the gene and to establish that it resides
not in prions but in the chromosomes of hamsters, mice, humans and all
other mammals that have been examined. What is more, most of the time,
these animals make PrP without getting sick.

One interpretation of such findings was that we had made a terrible
mistake: PrP had nothing to do with prion diseases. Another possibility
was that PrP could be produced in two forms, one that generated disease
and one that did not. We soon showed the latter interpretation to be
correct.

The critical clue was the fact that the PrP found in infected brains resisted
breakdown by cellular enzymes called proteases. Most proteins in cells are
degraded fairly easily. I therefore suspected that if a normal, nonthreatening
form of PrP existed, it too would be susceptible to degradation. Ronald A.
Barry in my laboratory then identified this hypothetical protease-sensitive
form. It thus became clear that scrapie-causing PrP is a variant of a normal
protein. We therefore called the normal protein "cellular PrP" and the
infectious (protease-resistant) form "scrapie PrP." The latter term is now
used to refer to the protein molecules that constitute the prions causing all
scrapielike diseases of animals and humans.

Prion Diseases Can Be Inherited

Early on we had hoped to use the PrP gene to generate pure copies of
PrP. Next, we would inject the protein molecules into animals, secure in the
knowledge that no elusive virus was clinging to them. If the injections
caused scrapie in the animals, we would have shown that protein
molecules could, as we had proposed, transmit disease. By 1986,
however, we knew the plan would not work. For one thing, it proved very
difficult to induce the gene to make the high levels of PrP needed for
conducting studies. For another thing, the protein that was produced was
the normal, cellular form. Fortunately, work on a different problem led us to
an alternative approach for demonstrating that prions could transmit
scrapie without the help of any accompanying nucleic acid.

In many cases, the scrapielike illnesses of humans seemed to occur
without having been spread from one host to another, and in some families
they appeared to be inherited. (Today researchers know that about 10
percent of human prion diseases are familial, felling half of the members of
the affected families.) It was this last pattern that drew our attention. Could it
be that prions were more unusual than we originally thought? Were they
responsible for the appearance of both hereditary and transmissible
illnesses?

In 1988 Karen Hsiao in my laboratory and I uncovered some of the earliest
data showing that human prion diseases can certainly be inherited. We
acquired clones of a PrP gene obtained from a man who had Gerstmann-
Str...ussler-Scheinker disease in his family and was dying of it himself.
Then we compared his gene with PrP genes obtained from a healthy
population and found a tiny abnormality known as a point mutation.

To grasp the nature of this mutation, it helps to know something about the
organization of genes. Genes consist of two strands of the DNA building
blocks called nucleotides, which differ from one another in the bases they
carry. The bases on one strand combine with the bases on the other strand
to form base pairs: the "rungs" on the familiar DNA "ladder." In addition to
holding the DNA ladder together, these pairs spell out the sequence of
amino acids that must be strung together to make a particular protein.
Three base pairs together-a unit called a codon-specify a single amino
acid. In our dying patient, just one base pair (out of more than 750) had
been exchanged for a different pair. The change, in turn, had altered the
information carried by codon 102, causing the amino acid leucine to be
substituted for the amino acid proline in the man's PrP protein.

With the help of Tim J. Crow of Northwick Park Hospital in London and Jurg
Ott of Columbia University and their colleagues, we discovered the same
mutation in genes from a large number of patients with Gerstmann-
Str...ussler-Scheinker disease, and we showed that the high incidence in
the affected families was statistically significant. In other words, we
established genetic linkage between the mutation and the disease-a
finding that strongly implies the mutation is the cause. Over the past six
years work by many investigators has uncovered 18 mutations in families
with inherited prion diseases; for five of these mutations, enough cases
have now been collected to demonstrate genetic linkage.

The discovery of mutations gave us a way to eliminate the possibility that a
nucleic acid was traveling with prion proteins and directing their
multiplication. We could now create genetically altered mice carrying a
mutated PrP gene. If the presence of the altered gene in these "transgenic"
animals led by itself to scrapie, and if the brain tissue of the transgenic
animals then caused scrapie in healthy animals, we would have solid
evidence that the protein encoded by the mutated gene had been solely
responsible for the transfer of disease. Studies I conducted with Hsiao,
Darlene Groth in my group and Stephen J. DeArmond, head of a separate
laboratory at U.C.S.F., have now shown that scrapie can be generated and
transmitted in this way [see box on pages 56 and 57].

These results in animals resemble those obtained in 1981, when Gajdusek,
Colin L. Masters and Clarence J. Gibbs, Jr., all at the National Institutes of
Health, transmitted apparently inherited Gerstmann-Str...ussler-Scheinker
disease to monkeys. They also resemble the findings of Jun Tateishi and
Tetsuyuki Kitamoto of Kyushu University in Japan, who transmitted
inherited Creutzfeldt-Jakob disease to mice. Together the collected
transmission studies persuasively argue that prions do, after all, represent
an unprecedented class of infectious agents, composed only of a modified
mammalian protein. And the conclusion is strengthened by the fact that
assiduous searching for a scrapie-specific nucleic acid (especially by
Detlev H. Riesner of Heinrich Heine University in DYesseldorf) has
produced no evidence that such genetic material is attached to prions.

Scientists who continue to favor the virus theory might say that we still have
not proved our case. If the PrP gene coded for a protein that, when
mutated, facilitated infection by a ubiquitous virus, the mutation would lead
to viral infection of the brain. Then injection of brain extracts from the mutant
animal would spread the infection to another host. Yet in the absence of any
evidence of a virus, this hypothesis looks to be untenable.

In addition to showing that a protein can multiply and cause disease without
help from nucleic acids, we have gained insight into how scrapie PrP
propagates in cells. Many details remain to be worked out, but one aspect
appears quite clear: the main difference between normal PrP and scrapie
PrP is conformational. Evidently, the scrapie protein propagates itself by
contacting normal PrP molecules and somehow causing them to unfold and
Bip from their usual conformation to the scrapie shape. This change
initiates a cascade in which newly converted molecules change the shape
of other normal PrP molecules, and so on. These events apparently occur
on a membrane in the cell interior.

We started to think that the differences between cellular and scrapie forms
of PrP must be conformational after other possibilities began to seem
unlikely. For instance, it has long been known that the infectious form often
has the same amino acid sequence as the normal type. Of course,
molecules that start off being identical can later be chemically modified in
ways that alter their activity. But intensive investigations by Neil Stahl and
Michael A. Baldwin in my laboratory have turned up no differences of this
kind.

One Protein, Two Shapes

How, exactly, do the structures of normal and scrapie forms of PrP differ?
Studies by Keh-Ming Pan in our group indicate that the normal protein
consists primarily of alpha helices, regions in which the protein backbone
twists into a specific kind of spiral; the scrapie form, however, contains
beta strands, regions in which the backbone is fully extended. Collections
of these strands form beta sheets. Fred E. Cohen, who directs another
laboratory at U.C.S.F., has used molecular modeling to try to predict the
structure of the normal protein based on its amino acid sequence. His
calculations imply that the protein probably folds into a compact structure
having four helices in its core. Less is known about the structure, or
structures, adopted by scrapie PrP.

The evidence supporting the proposition that scrapie PrP can induce an
alpha-helical PrP molecule to switch to a beta-sheet form comes primarily
from two important studies by investigators in my group. Mar'a Gasset
learned that synthetic peptides (short strings of amino acids)
corresponding to three of the four putative alpha-helical regions of PrP can
fold into beta sheets. And Jack Nguyen has shown that in their beta-sheet
conformation, such peptides can impose a beta-sheet structure on helical
PrP peptides. More recently Byron W. Caughey of the Rocky Mountain
Laboratories and Peter T. Lansbury of the Massachusetts Institute of
Technology have reported that cellular PrP can be converted into scrapie
PrP in a test tube by mixing the two proteins together.

PrP molecules arising from mutated genes probably do not adopt the
scrapie conformation as soon as they are synthesized. Otherwise, people
carrying mutant genes would become sick in early childhood. We suspect
that mutations in the PrP gene render the resulting proteins susceptible to
Bipping from an alpha-helical to a beta-sheet shape. Presumably, it takes
time until one of the molecules spontaneously Bips over and still more time
for scrapie PrP to accumulate and damage the brain enough to cause
symptoms.

Fred Cohen and I think we might be able to explain why the various
mutations that have been noted in PrP genes could facilitate folding into the
beta-sheet form. Many of the human mutations give rise to the substitution
of one amino acid for another within the four putative helices or at their
borders. Insertion of incorrect amino acids at those positions might
destabilize a helix, thus increasing the likelihood that the affected helix and
its neighbors will refold into a beta-sheet conformation. Conversely,
Hermann Sch...tzel in my laboratory finds that the harmless differences
distinguishing the PrP gene of humans from those of apes and monkeys
affect amino acids lying outside of the proposed helical domains-where the
divergent amino acids probably would not profoundly inBuence the stability
of the helical regions.

Treatment Ideas Emerge

No one knows exactly how propagation of scrapie PrP damages cells. In
cell cultures, the conversion of normal PrP to the scrapie form occurs inside
neurons, after which scrapie PrP accumulates in intracellular vesicles
known as lysosomes. In the brain, filled lysosomes could conceivably burst
and damage cells. As the diseased cells died, creating holes in the brain,
their prions would be released to attack other cells.

We do know with certainty that cleavage of scrapie PrP is what produces
PrP fragments that accumulate as plaques in the brains of some patients.
Those aggregates resemble plaques seen in Alzheimer's disease,
although the Alzheimer's clumps consist of a different protein. The PrP
plaques are a useful sign of prion infection, but they seem not to be a major
cause of impairment. In many people and animals with prion disease, the
plaques do not arise at all.

Even though we do not yet know much about how PrP scrapie harms brain
tissue, we can foresee that an understanding of the three-dimensional
structure of the PrP protein will lead to therapies. If, for example, the four-
helix-bundle model of PrP is correct, drug developers might be able to
design a compound that would bind to a central pocket that could be
formed by the four helices. So bound, the drug would stabilize these helices
and prevent their conversion into beta sheets.

Another idea for therapy is inspired by research in which Weissmann and
his colleagues applied gene-targeting technology to create mice that
lacked the PrP gene and so could not make PrP. By knocking out a gene
and noting the consequences of its loss, one can often deduce the usual
functions of the gene's protein product. In this case, however, the animals
missing PrP displayed no detectable abnormalities. If it turns out that PrP
is truly inessential, then physicians might one day consider delivering so-
called antisense or antigene therapies to the brains of patients with prion
diseases. Such therapies aim to block genes from giving rise to unwanted
proteins and could potentially shut down production of cellular PrP [see
"The New Genetic Medicines," by Jack S. Cohen and Michael E. Hogan;
SCIENTIFIC AMERICAN, December 1994]. They would thereby block PrP
from propagating itself.

It is worth noting that the knockout mice provided a welcomed opportunity
to challenge the prion hypothesis. If the animals became ill after inoculation
with prions, their sickness would have indicated that prions could multiply
even in the absence of a preexisting pool of PrP molecules. As I expected,
inoculation with prions did not produce scrapie, and no evidence of prion
replication could be detected.

The enigma of how scrapie PrP multiplies and causes disease is not the
only puzzle starting to be solved. Another long-standing question-the
mystery of how prions consisting of a single kind of protein can vary
markedly in their effects-is beginning to be answered as well. Iain H.
Pattison of the Agriculture Research Council in Compton, England, initially
called attention to this phenomenon. Years ago he obtained prions from
two separate sets of goats. One isolate made inoculated animals drowsy,
whereas the second made them hyperactive. Similarly, it is now evident
that some prions cause disease quickly, whereas others do so slowly.

The Mystery of "Strains"

Alan G. Dickinson, Hugh Fraser and Moira E. Bruce of the Institute for
Animal Health in Edinburgh, who have examined the differential effects of
varied isolates in mice, are among those who note that only pathogens
containing nucleic acids are known to occur in multiple strains. Hence, they
and others assert, the existence of prion "strains" indicates the prion
hypothesis must be incorrect; viruses must be at the root of scrapie and its
relatives. Yet because efforts to find viral nucleic acids have been
unrewarding, the explanation for the differences must lie elsewhere.

One possibility is that prions can adopt multiple conformations. Folded in
one way, a prion might convert normal PrP to the scrapie form highly
eUciently, giving rise to short incubation times. Folded another way, it might
work less eUciently. Similarly, one "conformer" might be attracted to
neuronal populations in one part of the brain, whereas another might be
attracted to neurons elsewhere, thus producing different symptoms.
Considering that PrP can fold in at least two ways, it would not be
surprising to find it can collapse into other structures as well.

Since the mid-1980s we have also sought insight into a phenomenon
known as the species barrier. This concept refers to the fact that something
makes it diUcult for prions made by one species to cause disease in
animals of another species. The cause of this diUculty is of considerable
interest today because of the epidemic of mad cow disease in Britain. We
and others have been trying to find out whether the species barrier is strong
enough to prevent the spread of prion disease from cows to humans.

Breaking the Barrier

The barrier was discovered by Pattison, who in the 1960s found it hard to
transmit scrapie between sheep and rodents. To determine the cause of
the trouble, my colleague Michael R. Scott and I later generated transgenic
mice expressing the PrP gene of the Syrian hamster-that is, making the
hamster PrP protein. The mouse gene differs from that of the hamster gene
at 16 codons out of 254. Normal mice inoculated with hamster prions rarely
acquire scrapie, but the transgenic mice became ill within about two
months.

We thus concluded that we had broken the species barrier by inserting the
hamster genes into the mice. Moreover, on the basis of this and other
experiments, we realized that the barrier resides in the amino acid
sequence of PrP: the more the sequence of a scrapie PrP molecule
resembles the PrP sequence of its host, the more likely it is that the host
will acquire prion disease. In one of those other experiments, for example,
we examined transgenic mice carrying the Syrian hamster PrP gene in
addition to their own mouse gene. Those mice make normal forms of both
hamster and mouse PrP. When we inoculated the animals with mouse
prions, they made more mouse prions. When we inoculated them with
hamster prions, they made hamster prions. From this behavior, we learned
that prions preferentially interact with cellular PrP of homologous, or like,
composition.

The attraction of scrapie PrP for cellular PrP having the same sequence
probably explains why scrapie managed to spread to cows in England from
food consisting of sheep tissue: sheep and bovine PrP differ only at seven
positions. In contrast, the sequence difference between human and bovine
PrP is large: the molecules diverge at more than 30 positions. Because the
variance is great, the likelihood of transmission from cows to people would
seem to be low. Consistent with this assessment are epidemiological
studies by W. Bryan Matthews, a professor emeritus at the University of
Oxford. Matthews found no link between scrapie in sheep and the
occurrence of Creutzfeldt-Jakob disease in sheep-farming countries.

On the other hand, two farmers who had "mad cows" in their herds have
recently died of Creutzfeldt-Jakob disease. Their deaths may have nothing
to do with the bovine epidemic, but the situation bears watching. It may turn
out that certain parts of the PrP molecule are more important than others
for breaking the species barrier. If that is the case, and if cow PrP closely
resembles human PrP in the critical regions, then the likelihood of danger
might turn out to be higher than a simple comparison of the complete
amino acid sequences would suggest.

We began to consider the possibility that some parts of the PrP molecule
might be particularly important to the species barrier after a study related to
this blockade took an odd turn. My colleague Glenn C. Telling had created
transgenic mice carrying a hybrid PrP gene that consisted of human codes
Banked on either side by mouse codes; this gene gave rise to a hybrid
protein. Then he introduced brain tissue from patients who had died of
Creutzfeldt-Jakob disease or Gerstmann-Str...ussler-Scheinker disease
into the transgenic animals. Oddly enough, the animals became ill much
more frequently and faster than did mice carrying a full human PrP gene,
which diverges from mouse PrP at 28 positions. This outcome implied that
similarity in the central region of the PrP molecule may be more critical than
it is in the other segments.

The result also lent support to earlier indications-uncovered by Shu-Lian
Yang in DeArmond's laboratory and Albert Taraboulos in my group-that
molecules made by the host can inBuence the behavior of scrapie PrP. We
speculate that in the hybrid-gene study, a mouse protein, possibly a
"chaperone" normally involved in folding nascent protein chains,
recognized one of the two mouse-derived regions of the hybrid PrP protein.
This chaperone bound to that region and helped to refold the hybrid
molecule into the scrapie conformation. The chaperone did not provide
similar help in mice making a totally human PrP protein, presumably
because the human protein lacked a binding site for the mouse factor.

The List May Grow

An unforeseen story has recently emerged from studies of transgenic mice
making unusually high amounts of normal PrP proteins. DeArmond, David
Westaway in our group and George A. Carlson of the McLaughlin
Laboratory in Great Falls, Mont., became perplexed when they noted that
some older transgenic mice developed an illness characterized by rigidity
and diminished grooming. When we pursued the cause, we found that
making excessive amounts of PrP can eventually lead to
neurodegeneration and, surprisingly, to destruction of both muscles and
peripheral nerves. These discoveries widen the spectrum of prion
diseases and are prompting a search for human prion diseases that affect
the peripheral nervous system and muscles.

Investigations of animals that overproduce PrP have yielded another
benefit as well. They offer a clue as to how the sporadic form of Creutzfeldt-
Jakob disease might arise. For a time I suspected that sporadic disease
might begin when the wear and tear of living led to a mutation of the PrP
gene in at least one cell in the body. Eventually, the mutated protein might
switch to the scrapie form and gradually propagate itself, until the buildup of
scrapie PrP crossed the threshold to overt disease. The mouse studies
suggest that at some point in the lives of the one in a million individuals who
acquire sporadic Creutzfeldt-Jakob disease, cellular PrP may
spontaneously convert to the scrapie form. The experiments also raise the
possibility that people who become aUeicted with sporadic Creutzfeldt-
Jakob disease overproduce PrP, but we do not yet know if, in fact, they do.

All the known prion diseases in humans have now been modeled in mice.
With our most recent work we have inadvertently developed an animal
model for sporadic prion disease. Mice inoculated with brain extracts from
scrapie-infected animals and from humans afflicted with Creutzfeldt-Jakob
disease have long provided a model for the infectious forms of prion
disorders. And the inherited prion diseases have been modeled in
transgenic mice carrying mutant PrP genes. These murine representations
of the human prion aUeictions should not only extend understanding of how
prions cause brain degeneration, they should also create opportunities to
evaluate therapies for these devastating maladies.

Striking Similarities

Ongoing research may also help determine whether prions consisting of
other proteins play a part in more common neurodegenerative conditions,
including Alzheimer's disease, Parkinson's disease and amyotrophic
lateral sclerosis. There are some marked similarities in all these disorders.
As is true of the known prion diseases, the more widespread ills mostly
occur sporadically but sometimes "run" in families. All are also usually
diseases of middle to later life and are marked by similar pathology:
neurons degenerate, protein deposits can accumulate as plaques, and
glial cells (which support and nourish nerve cells) grow larger in reaction to
damage to neurons. Strikingly, in none of these disorders do white blood
cells-those ever present warriors of the immune system-infiltrate the brain. If
a virus were involved in these illnesses, white cells would be expected to
appear.

Recent findings in yeast encourage speculation that prions unrelated in
amino acid sequence to the PrP protein could exist. Reed B. Wickner of
the NIH reports that a protein called Ure2p might sometimes change its
conformation, thereby affecting its activity in the cell. In one shape, the
protein is active; in the other, it is silent.

The collected studies described here argue persuasively that the prion is
an entirely new class of infectious pathogen and that prion diseases result
from aberrations of protein conformation. Whether changes in protein
shape are responsible for common neurodegenerative diseases, such as
Alzheimer's, remains unknown, but it is a possibility that should not be
ignored.

FURTHER READING

Scrapie Disease In Sheep. Herbert B. Parry. Edited by D. R.
Oppenheimer. Academic Press, 1983.

Molecular Biology Of Prion Diseases. S. B. Prusiner in "Science," Vol.
252, pages 1515-1522; June 14, 1991.

Prion Diseases Of Humans And Animals. Edited by S. B. Prusiner, J.
Collinge, J. Powell and B. Anderton. Ellis Horwood, 1992.

Fatal Familial Insomnia: Inherited Prion Diseases, Sleep, And The
Thalamus. Edited by C. Guilleminault et al. Raven Press, 1994.

Molecular Biology Of Prion Diseases. Special issue of "Philosophical
Transactions of the Royal Society of London, Series B," Vol. 343, No.
1306; March 29, 1994.

Structural Clues To Prion Replication. F. E. Cohen, K.-M. Pan, Z. Huang,
M. Baldwin, R. J. Fletterick and S. B. Prusiner in "Science," Vol. 264,
pages 530-531; April 22, 1994.

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