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Saskatchewan Movement Disorders
Program
Ali H. Rajput, Alex Rajput

ABSTRACT: We review the Saskatchewan Movement Disorders Program, which started in 1968 and has had the dual goals of patient
care and research. The clinics are structured to collect research-worthy data including videos, longitudinal follow-up, and autopsy studies
of patients seen in the clinics. At every clinic visit, the patient is evaluated by one or both authors. A total of 25% to 30% of the deceased
come to autopsy. Frozen half-brain and formalin-fixed remnants from autopsy are preserved in our laboratories. Patients not seen in our clinic
are not included in research, which makes it different from brain banks. So far, 515 cases have come to autopsy. So far, there
have been 17 collaborating scientific teams from Canada, the United States, Europe, and Japan. The collaborators are not charged for access to
our resources. This program offers a unique opportunity to study multiple aspects of movement disorder patients seen in clinical practice.

RÉSUMÉ: Movement Disorders Program de la Saskatchewan. Nous avons revu le Movement Disorders Program de la Saskatchewan établi en 1968.
Son but est double, soit les soins aux patients et la recherche. Les cliniques sont structurées de telle sorte que des données de qualité soient générées à
des fins de recherche, incluant des vidéos, sur le suivi à long terme et l’autopsie de patients suivis à la clinique. À chaque visite à la clinique, le patient est
évalué par l’un des auteurs ou par les deux. Une autopsie est effectuée chez 25% à 30% des patients qui décèdent. Des demi-cerveaux congelés
provenant d’autopsies et des tissus conservés dans la formaline sont également conservés dans nos laboratoires. Les patients qui ne sont pas suivis à
notre clinique ne sont pas inclus dans notre recherche, contrairement aux banques de cerveaux. À ce jour, 515 autopsies ont été réalisées et 17 équipes de recherche
du Canada, des États-Unis, d’Europe et du Japon ont collaboré avec nous. Aucun frais n’est exigé des collaborateurs pour avoir accés à nos ressources. Ce
programme offre une opportunité unique d’étudier les multiples aspects des troubles du mouvement rencontrés en pratique clinique.

Keywords: Brain function, essential tremor, movement disorders, neuropathology, Parkinson disease

doi:10.1017/cjn.2015.13 Can J Neurol Sci. 2015; 42: 74-87

INTRODUCTION AND HISTORY

Ali Rajput joined the neurology faculty at the University
of Saskatchewan in July 1967 and Alex Rajput joined in 2000.
For the first 33 years of this history, the term “I” means Ali Rajput
and the subsequent term “we” means both neurologists.

I came to the University of Saskatchewan in July 1967 on a
one-year contract. In late September, I informed the department
head that I was looking for a position elsewhere after my contract
expired. He asked me to wait for two weeks before making the
final decision as he was going to the United States and wanted to
talk to me on his return. While there, he died suddenly. A new
department head was appointed, and I went to inform him
about my decision. The department head was highly distressed
because there were not many neurologists in Canada at that time.
During that meeting, I made a commitment to stay one more year
in Saskatoon. During that year (1968), I met my future wife.
Soon after we were married, our family circumstances changed
and the decision to move was postponed.

Movement disorders were of clinical interest to me during my
neurology training. Like most chronic neurological diseases,
treatment options for Parkinson disease (PD) were very
limited.

MAJOR BREAKTHROUGH

In 1960, Ehringer and Hornykiewicz reported marked striatal
dopamine loss in parkinsonism.1 One year later, Birkmayer and
Hornykiewicz reported 20 PD patients who improved in a dose-
dependent fashion on intravenous levodopa (LD).2 Those two
articles were published in German and the intravenous use of the
drug had limitations for ongoing treatment of PD. A brief report
of oral LD producing improvement in PD was presented by
Dr. André Barbeau at the International Congress of Neurology in
Rome in 1961,2 but received little attention. In 1967, Cotzias et al3

reported dramatic improvement of PD motor symptoms on a large
dose of oral D-L dopa. Most cases received 9 g or more—up to
16 g/day.3 Soon LD became available to some experts, but it was
expensive. There were many seriously disabled parkinsonian

Presented as Donald Calne Lecture for Parkinson Society Canada, Montreal May 26,
2014.
From the Saskatchewan Movement Disorders Program, Neurology Division, University
of Saskatchewan and Saskatoon Health Region.

Correspondence to: Ali Rajput, University of Saskatchewan, Royal University Hospital,
Div of Neurology, 103 Hospital Dr., Saskatoon, Saskatchewan, Canada S7N 0W8.
Email: ali.rajput@saskatoonhealthregion.ca

RECEIVED OCTOBER 14, 2014. FINAL REVISIONS SUBMITTED DECEMBER 19, 2014.

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patients in every community who needed urgent treatment. There
was no dose-finding study of LD, and the neurologists used the
dose that they felt comfortable with.

Impetus for the University of Saskatchewan Movement
Disorders Program

In early 1968, Dr. A. Barbeau visited the University of
Saskatchewan and presented his own observations and the work of
Cotzias’s group. He informed us that he was organizing a multi-
center LD drug trial in Canada, but that Saskatoon was not
included. At that time, the University of Saskatchewan had three
full-time neurologists—the third largest number of academic neu-
rologists at a Canadian university. I asked my senior colleagues
why we were not considered for the LD trial. I felt that our patients
deserved the best available treatment as much as anyone else in
Canada; they suggested that I consider providing that treatment.

Start of Special Clinics and Research

In 1968, LD was not approved for general use by Canadian
physicians; therefore, I needed approval from Health Canada to
use the drug. Health Canada asked for evidence that I would also
be pursuing research. I produced a research protocol and the
permission to use LD was granted. The requirement by Health
Canada made it necessary for my special clinics and research be
carried out simultaneously. The clinics were started in Saskatoon
in 1968, and because of patient requests we started similar
monthly clinics in Regina in 1999.

Initially I had to import LD powder from the United States. The
Royal University Hospital Pharmacy prepared 500-mg LD cap-
sules (without charge) and the medication was sold to patients at
cost. Several North American neurologists were already using the
drug and I was in the second wave of specialists to use LD. In the
early years, we admitted patients to the hospital to start LD
treatment. During hospitalization, other staff—nurses, occupa-
tional therapists, physiotherapists, psychologists, and physicians-
in-training—became interested in the new treatment and helped
perform detailed patient evaluations.

Our movement disorders clinics in the 1960s and early 1970s
included PD cases because many of those patients needed urgent
treatment; however, soon I started seeing patients with other
movement disorders. It was anecdotally known that essential tre-
mor (ET) patients improved on alcohol but it had never been
studied systematically; the effect of alcohol on action tremor in
other disorders was also unknown. With the help of occupational
therapists, I conducted a clinical pharmacology study. We
observed that a small quantity of oral alcohol improved action
tremor in the majority of ET cases as well as in other disorders.4,5

Basic Scientists and Clinician Scientist Teams

The three essential ingredients to pursue research are: (1)
appropriate topics to study; (2) material (resources); and (3)
proper methods. Basic scientists are trained in highly specialized
methodology that they use to answer scientific questions. Clin-
icians have many questions like: What is it? What caused it? How
does it evolve? What is the best treatment? These different ques-
tions require different methods to provide answers. Teams con-
sisting of clinicians and basic scientists are therefore an ideal
combination for research. My research was based on many

questions requiring special tools to provide answers; thus, I nee-
ded expert collaborators using specific methodology but had to
provide them with adequate material. With time, many questions
were also raised by the collaborators, which in turn needed our
resource to answer.

START OF LOW-DOSE LD THERAPY

LD had created much publicity and optimism in physicians,
patients, and families. Before the start of the Movement Disorder
Clinic Saskatchewan (MDCS), some Saskatchewan patients had
travelled to other provinces and the United States for treatment
with LD. Expenses of the physician and hospital services outside
the province were the responsibility of patients, unless they sought
prior written approval from the provincial government. When
patients that had their LD treatment initiated outside Canada
reapplied for an out-of-province return visit, the government
directed them to my clinic. Thus I saw patients who were already
receiving LD. Based on observations in those cases and my own
early experience, I recognized that the large doses of LD used by
most neurologists at the time produced early and sometimes dis-
abling dyskinesias. I pondered the benefit and adverse effects
profile and concluded that in some PD cases, the quality of life on
LD was not much better than the untreated disease. My observa-
tion on dyskinesias was confirmed by others at a symposium
organized by Barbeau in Val David, Quebec, in 1969. Therefore,
on my own, I decided to use a lower dose of LD (up to 3 g, the
equivalent 600 mg levodopa/carbidopa).6 We hospitalized the
patients for slow titration and monitored the side effects. Our
patients had slower improvement, but at the end of several months
they were doing as well as those on the higher LD dose and had
fewer side effects. One adverse effect of LD was postural hypo-
tension, which was the topic of an early clinical pathological
study.7 Low-dose LD has remained standard practice at the
MDCS. In 1984, we published a 12-year experience. Dyskinesia
and motor response fluctuations were between 10% and 20%8

compared with those reported9 on higher LD dose. We also found
that dementia was not related to the duration of LD therapy8

(Figure 1).
At every MDCS patient visit, we used the newly described

Webster10 motor symptom measurement scale and Global Dis-
ability Scale described by Hoehn and Yahr.11 When the Unified
Parkinson’s Disease Rating Scale became available in 1987,12 we
started using that. The differences between the older.10,11 and
new12 scales were small and we could successfully convert old
data to the new scale for publications.13

WHAT SHOULD I STUDY AND HOW DO I DO THAT?

In the late 1960s and early 1970s, two main topics of PD
research were: (1) clinical observations on LD therapy and (2)
biochemical studies of PD brains. I was just getting started when,
in 1969, one New York group reported 100 patients treated with
LD. Naturally, their data would be more credible than the obser-
vations I could report on a much smaller number of patients.
Dr. Hornykiewicz pioneered the biochemistry in PD brains,1

which proved vital for future developments, but many more
questions needed to be answered. We had neither the brain
material nor the expertise for such studies.

I had to also consider the local realities. There was a major
mismatch between my research interest and the institutional

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situations. There were no funds for clinician-driven research, no
manpower dedicated to support research, no special equipment for
such studies, and no culture of clinician-driven research at the
University of Saskatchewan. We had no natural advantage to study
movement disorders, based on population ethnicity or the occupa-
tion in the province. My job involved full-time teaching and clinical
service with no protected time for research. Because I was unknown
and from an unknown institution, I had to produce high-quality
work that my peers would consider worthy of publication.

I realized that my research needed to progress beyond the
clinical observations on the patients and had to settle on topics that
were important but were not attractive to larger and faster research
teams. I recognized that some such studies could be pursued in
Saskatchewan. To do that, I needed the support of other experts;
however, I had nothing special to offer to attract well-known
collaborators. The research topics that I could tackle also required
a long time to study. Because research was my choice, I had to
find my own way to pursue it.

There was also a lingering doubt in my mind whether PD
research was a good academic career option. In 1963, Poskanzer
and Shwab.14 had reported that most PD cases were consequent to
the von Economo encephalitis epidemic of 1917-1930s and pos-
tulated that when the population exposed to that epidemic passed
away, PD would come to a natural end. It was published by a
reputable group from a highly prestigious institution (Harvard), so
we had to pay attention.

Taking Advantage of the Local Situation and Building
Alliances

My first major support came from my future wife, Karla.
Before we got married, I told her that my salary was only $14,000
per year (the lowest for neurologists in Canada), but I could earn

three times that amount in private practice. She asked me, “Do you
like what you do?” I said yes. She responded, “Do not worry; we
will make do”. She has done that for more than 40 years. Although
she has been my longest and unwavering supporter—she worked
in my laboratory as a volunteer for three years and as an employee
for the next 15 years—her name does not appear on our papers.

The low salary was a mixed blessing because there was no
pressure to generate large clinical billing income. The fees were
(and still are) based on seeing a new or a return-visit patient and
are significantly lower for a return visit. In my case, the fee
structure did not matter and I decided to follow patients at inter-
vals of my choice and spend as much time as I needed to perform
clinical assessments that could be used for future research. When I
could afford it, my first investment was a Super 8 movie camera.
Anyone who could look through the lens and press the button took
the video and every patient who consented had a movie made.
Many patients had movies made before and on LD treatment.
Soon after that, I purchased a Super 8 movie projector.

As the news of LD treatment for PD spread, invitations for
lectures started to come and I never turned down an opportunity.
The local media were very generous and showed the movies as
part of public service. After a lecture to nurses’ alumni of the
Saskatoon City Hospital, a lady said she wanted to work with me.
I thanked her and told her that I had no money to pay her, to which
she responded, “Did I ask you for money?” She was my first
research assistant and her two sons, who were land surveyors,
helped us free of charge to do a major study on the environmental
cause of PD. Following a lecture to the Kinsmen’s Club of Sas-
katoon in 1972, I joined them for lunch. After the lunch, their
executive members asked if they could borrow my film. They
wanted to show the film to other provincial chapters to establish a
foundation for the handicapped. The privacy regulations were not
stringent at that time and without much thought I agreed to loan

Figure 1: Adapted from Rajput et al, Neurology 1984.8

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them the film. They established a highly successful annual charity
event called TeleMiracle Saskatchewan. The first TeleMiracle
was organized in 1977 with me and a dopa-responsive dystonia
patient, whose film was used to motivate formation of the Foun-
dation, as special guests. (My children, aged six and four, got their
own thrills from meeting the Sesame Street actor, Bob McGrath,
and even had their picture in the local newspaper.)

Early Collaborating Scientists

My first effort to enlist scientific collaboration was to ask
Dr. Bohdan Rozdilsky, the neuropathologist at the Royal University
Hospital, to perform autopsies on my patients. He was trained by
Dr. Olszewski (of Steele-Richardson-Olszewski fame), who was
on our faculty in the 1950s. Dr. Rozdilsky was a thorough neu-
ropathologist and a very nice man; together, we produced some
30 articles.

The first few autopsies were done on patients who had died in
the hospital. Later, we decided to perform an autopsy on every
patient if the family consented. That was a major undertaking in a

large province of more than 652,000 square kilometers (251,700
square miles) but only one million population. We devised a plan
such that patients/families would experience the least hardship.
Patients interested in autopsy study for research would sign the
Declaration of Desire for Autopsy Study form (Figure 2). A copy
of the form was provided to each family member and to the family
physician. The patients also signed a more detailed consent
approved by the University of Saskatchewan Bio-Ethics Board
allowing storage and use of brains for research. The final decision
for autopsy was always made by the next-of-kin after death of the
patient. Using local pathologists to perform brain autopsy was not
suitable and frequently there was no local pathologist; therefore, it
was decided to transport the body to Saskatoon for autopsy to
ensure uniformity of the autopsy procedure. We concluded early
on that for most of the movement disorders, one-half of the brain
was sufficient for pathological studies and the other half could be
frozen for future research. The autopsy had to be done within
24 hours of death to prevent major biochemical changes. The
need for autopsy could arise at any time; therefore, I had to be
available around the clock to arrange that. Initially, it took me a

Figure 2: This form is provided to patients to decide on autopsy for research. A copy is
provided to each family member and the family physician.

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long time to get an autopsy organized, but the procedure has been
streamlined—a typical autopsy now takes between 2 to 4 hours of
neurologist’s time (though at times up to 12 hours).

Outside Collaborators

We are a small institution and there was limited neurosciences
expertise to study human brains. In 1967, Dr. O. Hornykiewicz
had moved to Clarke Institute in Toronto, and by the mid-1970s
we established collaboration with his team. Dr. S. Kish was his
postdoctoral fellow and later a faculty member. We collected
frozen half-brains in our freezer locally; when there was a suffi-
cient number of specimens, they were shipped to Toronto.

I was also collecting cerebrospinal fluid and urine samples
from PD patients untreated and on LD treatment. In 1981, my
freezer was accidentally unplugged, resulting in the loss of more
than 50 cerebrospinal fluid samples, several dozen urine samples,
and about ten frozen half-brains—irreplaceable specimens. I was
already a tenured full professor and research was not part of my
job requirement. Devastated by the loss, I opted to discontinue this
research. After three to six months of soul searching, I decided to
give it one more try.

We made arrangements to have our freezers connected to the
emergency power of the Royal University Hospital and to the
hospital security alarm system. With the new arrangement, I had
to be available 24/7 for any freezer mishap. There were several
occasions when I had to come to the hospital at night or over the
weekend to relocate frozen brains. After that, we started to keep all
frozen half-brains in Saskatoon and sent brain samples to Toronto
for specific research projects only.

By the mid-1990s, we had a sufficient number of frozen
brains in Saskatoon to pursue several large studies. By then,
Dr. Hornykiewicz had returned to Vienna. In 1996, while attending
a meeting in Vienna, I asked Dr. Hornykiewicz to recommend
someone who could help us process the frozen brains for research.
He said, “Would you like me to come to Saskatoon and do it for
you?” Before I could say yes, he said, “I know you do not have
money; you do not have to pay me.” That was far more generous
than I had expected. Soon he was appointed Distinguished
Professor of Brain Disorders Research at the University of Sas-
katchewan with no salary or stipend. He came to Saskatoon once
or twice a year for approximately a week at a time. He dissected
the frozen brains and guided us in research. He could dissect
brains for only three days per visit and approximately three new
brains each day. Together with Dr. Hornykiewicz and his Toronto
and new Vienna team, we have published more than 20 high-
impact articles. Our first collaborative study was published in
1978.15 Dr. C. Pifl of the Vienna team is our new collaborator and
together we have recently published a groundbreaking paper on
the pathogenesis of PD.16

Dr. Alex Rajput joined the College of Medicine faculty in 2000.
The next time Dr. Hornykiewicz came to Saskatoon, he spent the
entire visit providing hands-on training to Alex. All the frozen brain
dissections are now performed by Dr. Alex Rajput. With that
development, our options to collaborate increased substantially.

SABBATICAL LEAVE

The cohort hypothesis14 (of PD and its relation to von Econ-
omo encephalitis infection) was stuck in my mind. When I could

not convince anyone else to study that, I took a one-year sabba-
tical leave (1980-1981) to study the epidemiology of PD in
Rochester, MN. They had previously reported two incidence
studies from 1935 to 1966. If the cohort hypothesis were correct,14

it was expected that the incidence of PD would start to decline by
the late 1960s. Using the same methodology as in the previous
studies, I decided to study the incidence of PD in Rochester
between 1967 and 1979. Our study17 showed no decline in the
incidence of PS; thus, the cohort hypothesis14 was put to rest.

The sabbatical leave experience was wonderful academically
but financially disastrous. My salary was reduced by 35% and we
had to maintain two residences—Saskatoon and in Rochester for
part of the year. The Canadian dollar went down to 65 cents and
interest rates climbed to more than 20%. My host and mentor,
Dr. Len Kurland, was very generous to me and our family. Mayo
also helped me analyze my own clinical data, which by now were
voluminous.

I pursued an analytic epidemiology study to identify environ-
mental cause(s) of PD. It was like looking for a needle in a hay-
stack—because clinical onset of PD is later in life, one has to
consider numerous environmental factors. I decided on having a
smaller haystack for the search. We included only those patients
that had PD onset by age 40 years and further restricted the
environmental consideration to the first 15 years of life (because at
age 16 children can leave home). Twenty-one early-onset PD
patients in Saskatchewan were identified; all except one were born
and raised in small communities or on a farm and they had all
consumed well water for the first 15 years of life.18 We decided to
analyze the well water from those locations. Most old wells were
not operational, so we identified the nearest functioning wells.
Water samples were collected and compared with Saskatoon tap
water—there was no difference.19 We sent those water samples to
Dr. W. Langston in California for possible 1- methyl -4- phenyl
-1,2,3,6-tetrahydro pyridine (MPTP) or related substance, but
none was identified (unpublished).

Saskatchewan is a major agricultural province where herbi-
cides and pesticides have been used for as long as they have been
commercially available in Canada. We did not find an association
between the use of any of the herbicides or pesticides and higher
incidence of early onset PD.20

Considering my limited resources, I did not pursue population
epidemiology further.

THE SECOND PHASE OF RESEARCH

The two phases of our research are arbitrary because there is
much overlap. The dividing line for me was excluding the cohort
hypothesis; I could now focus on clinical and pathological studies
of movement disorder brains.

By contemporary standards, we had devised a new model of
research that had a distinct set of needs. This model was dictated
to a considerable extent by the local circumstances. We had major
weaknesses, but there were several strengths as well. There was a
need for research support at multiple levels, especially because
our research was based on human subjects. The major clinical
focus was longitudinal follow-up of the MDCS patients and
autopsy studies of their brains. That required strong patient/
family/public involvement. Saskatchewan was the home of the
cooperative movement that started during the Depression years. In
1962, Saskatchewan became the first Canadian province to

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introduce general tax-funded universal health care system, and I
wanted to capitalize on that public spirit. Personally, I needed to
go beyond the usual duties of a physician—to lead by example.
Building the trust and support of the public required different
skills than the practice of medicine; we have succeeded at that and
much credit goes to the people of Saskatchewan.

Funding

Funding for clinician-driven movement disorders research in
Canada is mainly from local private sources. The researchers
procure funds with their own efforts. A lot of our work was done
on “please and thank you,” much personal unpaid time, and sig-
nificant in-kind support from the hospital. In spite of that, we still
needed funds to pay our small dedicated research staff, and for
equipment and consumables. Saskatchewan does not have many
wealthy people who could make large donations. Some patients/
families offered small amounts of money for special clinics and
research. I was not sure how to handle those funds and consulted a
senior colleague; he recommended against personally handling
any donations. Four of my patients/friends and I applied for a
registered charity status and in 1972 we received approval for the
Saskatchewan Parkinson’s Disease Foundation (SPDF). The pri-
mary stated objective in the application was to raise funds for
special clinics and research. Anyone who wanted to donate
towards my work was directed to the SPDF. The donations were
usually small. I observed early on that I would prefer receiving
one dollar from a million people as opposed to a million dollars
from one person (million-dollar single donations were not forth-
coming anyway). The donors of one dollar I hoped would be able
to give another dollar the following year. The large number of
small donors also started to identify with our program and con-
tinued to support it in many other ways, notably in getting the
brain autopsies. The SPDF contributed financially to the running
of special clinics and research, from those donations. The SPDF
was subsequently renamed as Parkinson’s Society Saskatchewan.

In the early 1990s, a group of patients/families organized an
annual curling tournament in Regina to support our clinics and
research. Soon, another group organized a golf tournament in
Regina with the same objectives. Those two events have been held
regularly for more than 22 years and have raised millions of
dollars for the program. Both are strictly volunteer-run events.
Some other smaller provincial groups have organized independent
fundraising events to support our work. We have received money
from multicenter drug trials (including some funded by the
National Institutes of Health in the United States); all funds left
over from the drug studies were kept for other research and the
special clinics. Even after I (Ali) retired from my position at the
University of Saskatchewan in 2002 (when mandatory retirement
at the University of Saskatchewan was still in place), I did not take
residual research funds for myself. We have received research
grants from Parkinson’s Society Canada and small amounts from
the International Essential Tremor Foundation and from Canadian
Institutes of Health Research joint grants. In 2008, an anonymous
donor established a one million dollar Trust for the Movement
Disorders Research and later donated $600,000 more. Our model
of program funding is similar to that at other major movement
disorders programs in Canada. Since my (Ali) retirement from the
University, the provincial government has provided financial
support towards Movement Disorder Clinics.

ADDITIONAL COLLABORATIONS

After Dr. Alex Rajput was trained in processing the frozen
brains in 2000, the number of collaborators has increased. So far,
we have had 17 different collaborating teams from Canada, the
United States, Europe, and Japan. We will not go over the con-
tributions made by all of them and instead will restrict our com-
ments to two major Canadian teams that are currently active.

Quebec City – Laval University Group

In 1997, Dr. Paul Bédard, Professor of Neurology, Laval
University, Quebec City, visited Saskatoon for the Canadian
Congress of Neurological Sciences. Paul was pursuing high-
quality work on a primate model of MPTP-induced Parkinson
syndrome (PS). The MPTP model has served well for studies of
major motor features of PS, but does not fully represent the
naturally occurring disease.16 I asked Paul to consider enlarging
his scope of work to include studies of human movement disorder
brains and later that year I invited him as a Visiting Professor to
the University of Saskatchewan. We showed him our setup and he
was convinced that we could develop a useful collaboration. He
recommended inclusion of his younger colleague, Dr. Thérèse Di
Paolo, who had done considerable work on MPTP monkeys. She
visited Saskatoon the following year and our collaboration began.
She introduced us to her younger colleague, Dr. Frédéric Calon.
All three of them have honorary Adjunct Professor appointments
at the University of Saskatchewan. This collaboration has pro-
duced more than ten very high-quality papers. They have studied
PD brains including LD-induced dyskinesia.21 Our recent paper in
Brain22 on the GABAergic system in ET brains was chosen as
one of the ten best scientific developments in the Province of
Quebec in 2012. We should note that Quebec is a powerhouse for
neurosciences research in Canada. Our collaboration continues
with Drs. Calon and Di Paolo, but unfortunately Dr. Bédard is no
longer active.

MAYO CLINIC JACKSONVILLE, FL/UNIVERSITY OF BRITISH
COLUMBIA

In 2002, I (Ali) was introduced to Dr. Matthew Farrer who was
pursuing genetic studies of PD at the Mayo Clinic, Jacksonville,
FL. We invited him to Saskatoon and quickly realized that we
would benefit from each other’s expertise. Dr. Farrer and his team,
including Dr. C. Vilariño-Gűell, moved to the University of
British Columbia in 2010. Our University of British Columbia
collaboration team has enlarged and now includes two leading
movement disorders and positron emission tomography scan
experts, Drs. Jon Stoessl and Silke Cresswell. Together, we have
published more than 25 articles dealing with the genetics of
movement disorders and more recently with functional imaging
(positron emission tomography). We have reported on the LRRK2
gene mutation with autopsy verification in one PD family; inter-
estingly, the pathology showed a tauopathy with no evidence
of Lewy bodies.23 Dr. Farrer and his group have identified
DNAJC13 mutation in a large multi-incident Mennonite family
from Saskatchewan, with autopsy verification of Lewy body
PD.24 This observation has the potential to significantly enhance
our understanding of the pathogenesis of PD. There are several
other articles accepted or in the pipeline.

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STUDENTS AND FUTURE SCIENTISTS

As the research in movement disorders at the University of
Saskatchewan progressed, several students worked with me dur-
ing the summers. Even students joining our program for a short
time have been able to present and publish articles based on our
resources. Some of them now occupy prominent academic posi-
tions in Canada and the United States. Notable in that group are
Drs. Ryan J. Uitti and Alex Rajput. Ryan started working with me
in the summer after his first year of medical college and then
continued to be involved throughout his medical college years and
beyond. He graduated in 1988 and is now Professor of Neurology
at the Mayo Clinic, Jacksonville, FL. Dr. Alex Rajput started
working with me in the summer when he was 15 years old and I
paid him from my own pocket. My motive was more personal
than academic—I wanted to know where my son was so he would
not be bored and get into trouble. He did his neurology training at
the University of Iowa and moved back to Saskatoon in 1998 as he
was on a J1 visa in the United States. He needed a postgraduate
year-5 of residency training to qualify for the FRCP(C) Neurology
Examination and following that he did a one year movement
disorder fellowship in Saskatoon. He had an offer for a position at
the University of Saskatchewan but was seriously considering
moving back to Iowa. I did not want to get involved in that
decision nor did I participate in his appointment to the faculty at
the University of Saskatchewan. Once he was here, I asked
Dr. Hornykiewicz to train him in the methods of frozen brain
dissection in 2000. Alex also did special training in 2003 on the
rotenone rat model of PD at Emory University, Atlanta, in
Dr. J. Timothy Greenamyre’s laboratory. In our laboratory, the
mortality in those animals was high and we determined that early
death was associated with brain hemorrhage.25 We concluded that
this model was not suitable for our research. Dr. Alex Rajput is now
the Director of the Saskatchewan Movement Disorders Program,
including the clinics, research, and all related laboratories.

MAIN COMPONENTS OF SASKATCHEWAN MOVEMENT
DISORDERS PROGRAM

There are two inseparably linked components: (1) clinical
services for Saskatchewan patients and (2) research. That dual
objective was the foundation of this program in 1968. The data
collected in the clinics are not driven by any one research protocol
but are research-worthy. The clinical data are regularly used in
conjunction with videos, pathology, biochemistry, and genetics
information in our research. Longitudinal follow-up of the
patients is a major feature of the MDCS. All Saskatchewan resi-
dents carry general tax-supported health care insurance and access
to MDCS is equal to all provincial residents. There is a provincial
plan to support drug costs.

Clinical Data

Every patient seen at the MDCS is regarded as a potential
candidate for inclusion in research studies. The clinics in Saska-
toon and Regina are identical. At every clinic, there are two or
three support staff members assisting the clinicians. Video
recordings are made on all consenting subjects at and rarely on
consenting family members who may be of research interest. After
initial MDCS assessment, a brochure outlining the disorder, the
nature of the disease, and management options is provided. The

expected outcome is discussed with the patient/family. Those
discussions are not restricted by time. Patients are provided with
our office telephone numbers, and have an unlimited access to the
two (AHR/AR) neurologists between clinic visits. We (AHR, AR)
answer our patients’ telephone calls, and considerable neurologist
time is spent on the telephone with patients. We are interested in
knowing of changes in the patient’s status; when appropriate, we
initiate treatment changes that may include phone calls or faxes to
the patient’s pharmacy—that information is entered into the
patient record and used for patient care and research.

At an opportune time, we ask patients to consider if they wish
to have an autopsy be done after death (Figure 2). We prefer to
give that form to the patient/family to take home and discuss with
family members before signing. If the patient is comfortable and
intends to proceed with the autopsy, the form is signed and
returned to us. There is no expense to the family and the body is
not disfigured for viewing. They are also assured that regardless of
the decision on autopsy, there would be no impact on the ongoing
care. In case the patient is not comfortable with the declaration,he
or she is asked to write “no” on the form and return it to us. Once a
patient has said “no,” we do not ask again for autopsy declaration.
In those cases where the patient has declared the desire to have an
autopsy, a copy of the signed form is provided to each family
member and to the family physician. Patients that sign the
declaration also sign consent for use of brain tissue for research
and allow us access to their clinical information from all sources.
If we come across a suitable normal control subject, we offer a
similar autopsy option.

AUTOPSY PROCEDURE

Typically a call comes to the neurologist from a family mem-
ber, nursing home, or hospital personnel that the patient has died
and the family wishes to have an autopsy performed for research.
The two of us (AHR, AR) are on 24/7 call (Figure 2). We make
autopsy arrangements with the family, care home, funeral home,
morgue attendant, etc. and are available from the time of initial
call until the body is released back to the funeral home. Autopsies
are performed in Saskatoon. The cost of transporting the body
to and from Saskatoon is our responsibility. Saskatchewan is a
large geographical area so there can be long distances to transport
the body. We also pay for the time of extra morgue attendants
when they are needed after hours. The average immediate cost for
body transport and the autopsy procedure is now approximately
$2,000. In rare situations, for patients that have died out of pro-
vince we are grateful to have received support from local
neuropathologists.

Between 30% and 35% of our Parkinson’s patients and a
smaller percentage of ET cases come to autopsy. The decision to
have an autopsy performed rests with the next-of-kin; there are
rare examples in which the patient did not sign the declaration but
the family decided on autopsy. On other occasions, patients not
seen at MDCS also come to autopsy. A call would come at night
indicating that someone in a nursing home who had PD has died,
but neither the caller nor the neurologist is certain if the patient
was ever evaluated at the MDCS. The autopsy will proceed and
when we discover later that the patient was never seen in our
clinic, the brain is not used for research because of lack of our own
clinical information. Some normal controls not seen at the MDCS
also come to autopsy.

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Immediately after removal, the brain is divided at midline into
two halves. Half is frozen at −80°C for future studies and the other
half is fixed in formalin for pathology studies. (There is no parti-
cular side that is chosen when the brain is grossly normal. For those
cases in which there is a known structural lesion, that hemisphere is
fixed in formalin.) The neuropathologist produces a detailed report
that is attached to the patient’s clinical record and a copy is sent to
the next-of-kin, with an offer to discuss the diagnosis.

Figure 3 shows summary of Saskatchewan Movement Dis-
orders Program.

INFORMATION AND MATERIAL STORAGE

Figure 4 shows different laboratories where patient records and
material are stored.

Videos made with older technology need updating. There are
more than 3500 patient videos and some patients have had several
videos. One member of our staff is responsible for the video
library. The videos are updated regularly to ensure compatibility
with the most recent technology and catalogued.

As noted previously, the freezers are connected to the hospital
auxiliary power and the alarm system monitored by Royal Uni-
versity Hospital security department. The two of us (AHR, AR)
are on 24/7 call for any freezer mishap.

Figure 3: Flow chart of Saskatchewan Movement Disorders Program
operations.

Figure 4: Pictures of Saskatchewan Movement Disorders program storage of patient records and research material. (A) Filing cabinet containing
hard copies of patient clinical records. (B) −80°C freezers. Currently there are nine freezers. (C) Cardboard boxes, each containing half-frozen brain
from a patient. Each box has patient identification at four places—two with only the number and two with name and number. (D) Formalin-fixed
remains of the brain tissue after pathology has been completed. (E) Paraffin blocks and glass slides stored in our laboratory. (F) Video library.

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Each frozen brain is kept in a separate box. The frozen brains are
dissected (by AR) in another special room and only one brain is
brought to that room at a time.

The formalin-fixed tissue and paraffin blocks are being used
for research with increasing frequency as new investigative tools
become available. One member of our staff has the primary
responsibility for the brain tissue storage laboratories, though
other members are familiar with that.

Major Movement Disorders Studied at MDCS

The disorders studied at MDCS are those prevalent in the
Saskatchewan population. The three most common disorders in
our clinic population are parkinsonism, ET, and dystonia (mostly
focal or segmental). Figure 5 shows the latest autopsy count and
the broad diagnostic groups. In some cases, a final pathology
report was not available at the time of this article’s preparation.
Most of our collaborations are based on deidentified frozen half-
brains. Numbered brain tissue samples are provided to the
collaborators.

OUR RESOURCE IS NOT A BRAIN BANK

Since we started publishing human brain studies, interest in
this field has increased. Several institutions are now pursuing
studies of movement disorder–autopsied brains. Each program
uses the strategy appropriate to the local circumstances and each
has its own strengths and weaknesses. Following are the common
models of such programs.

1. Patients receiving a certain drug treatment regimen are enrolled
in research; thus, they are evaluated by the researchers at regular
intervals using specific research protocol and autopsy studies are
performed.26 The patients, however, are cared for by their own
physicians. The strength of such programs is that research-
specific data are collected prospectively. The weakness is that
only the specially selected cases are included and the clinical
data collected by treating physicians are heterogenous.

2. Studies based on individuals from defined communities who
express a desire to have autopsy studies for research.27-30

Strengths of such programs are that patients are periodically
evaluated in detail by movement disorders experts. They can
collect large amounts of detailed data and a large number of
autopsied brains, including control brains for research. The
autopsy can be obtained soon after death and expert patholo-
gists study every brain. The weaknesses are that the cases
included are all elderly and not representative of the general
population.29,30 and in many cases the medical care is provided
by other physicians.

3. National Parkinson’s Disease Brain Bank.31 Brains from all
parts of the country are forwarded to a centralized brain bank.
The strength is that a large number of brains can be collected.
The weaknesses are that there are many (more than 70)
physicians including neurologists and geriatricians who
look after these patients and collect the clinical data.32 The
autopsies are performed locally at multiple sites, thus there is
a lack of uniformity of the clinical data and the brain
harvesting.

PD w/wo
Other Dx

PSP
w/wo

Other Dx

MSA
w/wo

Other Dx

ET w/wo
Other Dx

CBD
w/wo

Other Dx

ALS
w/wo

Other Dx
Controls

AD w/wo
Other Dx

Other Normal Diseased

Autopsies 292 54 27 57 7 6 18 28 46 Autopsies 15 1

Frozen 245 50 16 46 7 4 13 22 28 Frozen 13 0

Formalin 197 41 13 34 6 3 4 17 24 Formalin 4 1

Paraffin 240 51 16 43 7 5 13 22 30 Paraffin 11 1

Cases with Tissue Available Used as Controls

Total Number of Autopsies with Pathology
Report and/or Tissue Available

(July 2014)

570

Number of Cases Seen in Our Clinic
(Alex or Ali )

Number of Cases Not
Seen in Our Clinic

515 55

Figure 5: Summary of autopsy studies performed at Saskatchewan Movement Disorders Program and available samples. PD = Parkinson
disease; PSP = progressive supranuclear palsy; MSA = multiple system atrophy; ET = essential tremor; CBD = corticobasal degeneration;
ALS = amyotrophic lateral sclerosis; AD = Alzheimer disease.

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4. National Essential Tremor repository in the United States.33-35

Neurologists—mostly movement disorders experts from
across the country—provide the brains from their own patients.
The strengths are that a large number of ET brains are available
for research and there is very good team of neuropathologists
that study those brains. The weaknesses are that the patients are
looked after by many different neurologists and the autopsies
are performed at multiple sites before the tissue is transported
to the central repository.

5. Our program is based on our own clinical practice of movement
disorders. For research, we include patients that we (AHR, AR)
have evaluated at the MDCS. Our cases include a representative
sample of the provincial population—all ages and all forms of
treatment. The autopsies are done at one centralized location.
All patients are looked after by us (AHR, AR), which ensures
consistency of the clinical data. The treatment regimen is fully
documented and the autopsy procedure is standardized. All
patient records including videos and brain material are pre-
served in our laboratories. Research is based on movement
disorder patients seen in our clinic and controls. The main
weaknesses are that it is a slow process to collect large number
of brains and the clinical data are not based on any specific
research protocol. Over the years, we have collected several
hundred brains from patients with diverse movement disorders
(Figure 5) and the clinical data are of adequate quality to
complement other major research studies.8,13,36-38

After visiting Saskatoon, Dr. Andres Lozano, Professor and
Head of Neurosurgery, University of Toronto, called it a “Safety
deposit—world heritage site unmatched anywhere.” Dr. Horny-
kiewicz observed, “I consider that collection the most valuable in
the world. There is nothing else like it, and I know about every
such lab. He collected the whole thing in Saskatoon very patiently,
and now it is unique. He has very rare material and has meticulous
records of the patients.” To distinguish from a brain bank, we call
our resource the Brain Safety Deposit.

SELECTED WORK OF THE SASKATCHEWAN MOVEMENT
DISORDERS PROGRAM

For space reasons, we cannot comment on most of our articles
and will exclude the epidemiological studies noted previously.
We briefly describe some of our work in chronological order to
illustrate the evolution of the research over time.

1. 1973. Specificity of Tremorilytic Effects of Alcohol and
Propranolol.4 Improvement of ET after an alcoholic drink
has been anecdotally known for a long time and that infor-
mation was passed by the neurologists from one generation to
the next, but it was never established scientifically. This was
first ever literature report on systematically studied effect of
oral alcohol on the ET.

2. 1975. Relative efficacy of alcohol and propranolol in action
tremor.5 This was the first published study on the effect of
1 oz (30 mL) oral alcoholic on the action tremor in several
different disorders. We reported on 39 cases, including 21
with ET and 15 with PD. Action tremor improved 30 minutes
after 1 oz of alcohol ingestion in 62% of ET and 47% of PD
cases; action tremor of some other rare disorders also
improved. The blood alcohol levels did not correlate with the
tremor benefit. More patients improved on propranolol than

with a single alcoholic drink. To our knowledge, this is the
only study on the effect of oral alcohol in action tremor in
multiple disorders. The symptomatic benefit of alcohol on
action tremor is neither specific nor restricted to ET.

3. 1976. Dysautonomia in parkinsonism: a clinicopathological
study.7 Autonomic dysfunction in PD was recognized by
early 1960s, but the anatomical basis of that was unknown.
Most pathology studies were limited to brain and the spinal
cord. This study included eight patients that had detailed intra-
arterial blood pressure assessments in supine and upright
positions, and the autopsy study included the brain, spinal
cord, and the sympathetic ganglia. The orthostatic hypotension
correlated with the sympathetic ganglia pathology—neuronal
loss and Lewy body inclusions. This is the only study to our
knowledge that looked histologically at central as well as
the peripheral autonomic nervous system for the autonomic
dysfunction in PD.

4. 1978. Receptor basis for dopaminergic supersensitivity in
Parkinson’s disease.15 This included 14 normal controls,
6 untreated PD, and 5 LD-treated PD patient brains. The
dopamine receptors were supersensitive in the untreated PD
and the sensitivity declined after treatment with LD. This is
one of the earliest studies, if not the earliest study of its kind.

5. 1982. Reversible drug-induced parkinsonism.39 Drug induced
parkinsonism has been well known since the 1950s, but there
were no pathological studies to determine the underlying
mechanisms of parkinsonian manifestation. This was a clinical
and pathological study of two cases. On neuroleptics, each
patient manifested parkinsonism. At autopsy, each case had
pathological evidence of premotor PD. The neuroleptic stress
needed to unmask parkinsonism was inversely related to the
underlying PD pathology.

6. 1984. Chronic low dose levodopa therapy .8 High dose of LD
was a common practice in the 1960s-1970’s. We observed that
this resulted in early onset of dyskinesias in many cases and
decided to use a lower dose of LD. This was a 12-year clinical
study of 195 cases on low dose—3 g or less plain (600 mg LD/
carbidopa)/day. Low-dose LD was effective and resulted in
considerably lower incidence of dyskinesia and motor
response fluctuations.8,40 compared with most literature
reports.9 Those observations were confirmed 29 years later by
Olanow et al.41 Our practice of using lower dose resulted in
lower drug costs, less common need for medical service for LD
complications, and a better quality of life for patients.

7. 1990. Levodopa efficacy and pathological basis of Parkinson
syndrome.36 LD was known to be effective in most PD cases,
but the information was based on clinical observations. Some
patients in those studies likely included other variants of PS.
This is a 22-year clinicopathological study of 59 cases. It
shows that all PD patients receiving an adequate LD dose
improve, all patients with Substantia Nigra (SN) restricted
pathology also improve, and 33% of multiple system atrophy
cases have some benefit on LD. This is the first published
autopsy verified report on LD efficacy in PS.

8. 1991. Accuracy of clinical diagnosis in parkinsonism—a
prospective study.42 This was the first study comparing clinical
diagnosis with autopsy verification in parkinsonism. At the
first visit, a neurologist correctly diagnosed PD in 65%,
whereas at the final assessment before death, diagnosis by
a movement disorder neurologist was accurate in 76% (as

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verified by brain histological studies). This article was very
well-received and was considered the best original article in the
Canadian Journal of Neurological Sciences in 1991. In 2014,
Adler et al28 reported a virtually identical accuracy rate—68%
of the initial and 77% of the final clinical diagnosis accuracy.
Thus, predicting the pathology, based on the clinical diagnosis
of PD, has remained unchanged for more than two decades.43

Our study helped include clinical diagnostic inaccuracy when
considering PD case selection for drug trials.

9. 1993. Significance of parkinsonian manifestations in essen-
tial tremor.37 Tremor is the major manifestation in both PD
and ET, but resting tremor is considered characteristic of PD.
There is no widely available biological marker to clinically
distinguish between those two disorders. In this clin-
icopathological study of nine ET patients, three (33%) had
resting tremor as part of the natural evolution of ET. This was
first pathologically confirmed report on the presence of rest-
ing tremor in ET patients. We also recommended that in a
well-established ET case, all three parkinsonism motor fea-
tures—resting tremor, bradykinesia, and rigidity (preferably
asymmetrical)—must be present before making the additional
diagnosis of PS.

10. 1993. Prognostic significance of the onset mode in parkin-
sonism.44 It was widely known that parkinsonian cases have
different modes of motor onset, but the reasons for that were
not known. This clinicopathological study of 70 autopsied
patients over 29 years showed that most patients with tremor
onset had PD, whereas the postural instability and gait diffi-
culty onset was most common in multiple system atrophy and
progressive supranuclear palsy. The prognosis is most
favorable in the tremor onset cases.

11. 1994. Dopa-responsive dystonia: pathological and bio-
chemical observations in a case.45 Dramatic and sustained
response on a small dose of LD is well-known in dopa-
responsive dystonia. This was a detailed clinical, pathologi-
cal, and brain biochemical study of a 19-year-old woman who
died after 14 years of dystonia symptoms. She had marked
improvement on LD initiated at age 8 years and died in an
automobile accident at age 19. The number of pigmented
substantia nigra neurons was normal, but there was a marked
reduction in the neuronal pigmentation. There was marked
reduction in striatal dopamine levels. This patient was sub-
sequently reported in a genetic study showing GCH1 gene
mutation as the first example in a Caucasian subject.46 Her
brother, who had mild symptoms from childhood but did not
come to medical attention until age 49 years with mild fea-
tures of parkinsonism and dystonia, has responded very well
to a small dose of LD.

12. 1997. Is levodopa toxic to human substantia nigra?.47 Toxicity
of levodopa to the human SN was vigorously debated based on
laboratory studies, especially after dopamine agonist drugs
became available. We reported five cases including two
autopsies. In one patient, a total of 24 kg (plain LD) was used
over 26 years without evidence of nigral damage. This was the
first pathologically verified study to show that levodopa is not
toxic to human SN. We have now collected 21 LD-treated
autopsied cases that have normal SN (unpublished).

13. 1997. Timely levodopa (LD) administration prolongs survi-
val in Parkinson’s disease.48 There was an ongoing debate if
LD increased life expectancy in PD; however, it could not be

verified because all the contemporary PD patients are treated
with LD and untreated controls needed for comparison are not
available. This clinical study included 934 cases observed
over 22 years. Cases were divided into those with delayed
access to LD at first assessment at MDCS (1968 to the end of
1973) with those having unrestricted access to LD (if needed)
at first assessment (1974 and later). To our knowledge, this is
the only study comparing PD patients that had highly
restricted access to LD with patients that had unrestricted LD
access. The survival in parkinsonism remains shorter than
expected, but it has increased significantly since unrestricted
access to LD. Survival benefit, however, is restricted to those
that receive LD therapy before onset of postural instability
(stage 3 Hoehn and Yahr, or modified Hoehn and Yahr stage
2.5). We also noted that epidemiological studies comparing
PD survival with the general population that start from the
retrospectively identified PD onset date artificially inflate PD
survival. Such survival comparisons should start from the
date of PD patient entry in the study (i.e. first visit).

14. 2002. Clinical-pathological study of levodopa complica-
tions.38 LD motor complications are known to increase with
longer duration of treatment; however, most studies are based
on clinical observations of heterogenic PS cases that have
different responses to LD.36 This was a 28-year study of 42
autopsied Lewy body PD cases. The most common LD motor
complication was dyskinesia. Cumulative incidence of dys-
kinesia (observed at some time during the course) over the
20-year study interval was 80%, of wearing-off 50% and of
on-off 25%. To our knowledge, this is the only study based on
autopsy-verified PD cases on this subject.

15. 2004. Human brain dopamine metabolism in levodopa-
induced dyskinesia and wearing-off.49 Some PD patients on
long-term LD treatment develop wearing off but no dyski-
nesia, whereas others on comparable LD dose/duration
manifest dyskinesia but no wearing off. The reason for that
difference was not known. This study compared nine PD
brains of cases with different LD motor complication profiles
followed over 21 years with four neurologically normal
control brains. This is the first autopsy study to show that
patients with wearing-off metabolize dopamine more rapidly
than the patients with dyskinesia.

16. 2004. Essential tremor course and disability: a clin-
icopathological study of 20 cases.50 ET patients have a vari-
able course—in some cases there is no significant progression
and in others the symptoms worsen with time. In 20 autopsied
ET cases seen at MDCS over 32 years, we observed pro-
gressively wider anatomical sites of tremor involvement and
increasing functional disability with time. The risk of devel-
oping PD in the ET cases was comparable to that in the
general population. This is the first autopsy study of long-
itudinally followed autopsied ET cases.

17. 2008. Globus pallidus dopamine and Parkinson motor sub-
types: clinical and brain biochemical correlation.51 Some PD
patients manifest dominant tremor, whereas others have
dominant bradykinesia and rigidity, and many more have
equal severity of those motor features. There was no expla-
nation for those clinical differences. This study of eight PD
cases that had different motor subtypes (determined when the
entire clinical course of disease was considered) and five
normal control brains found striatal dopamine loss was more

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pronounced in the akinetic-rigid compared with tremor
dominant cases. In the globus pallidus interna, dopamine loss
was the most pronounced in the akinetic-rigid and the least in
the tremor-dominant cases. These data indicate that akinetic-
rigid cases have a more widespread pathology than the tremor
dominant cases.

18. 2009. Course in Parkinson’s disease subtypes: a 39-year
clinicopathological study.13 Having established that the
akinetic-rigid cases have more advanced pathology,51 we
chose to determine the course of disease in different PD motor
subtypes. This study included 166 autopsied PD cases seen at
MDCS during 39 years. Motor subtypes were based on the
entire course of disease. The outcome was most favorable in
those who had tremor-dominant and the worst in akinetic
rigid cases. This is the longest followed autopsy-verified
study of PD motor subtypes reported to date.

19. 2011. Significance of cerebellar Purkinje cell loss to patho-
genesis of essential tremor.52 The pathological basis of ET
remains unknown but some studies.33-35 reported that cere-
bellar Purkinje cell (PC) loss was the specific pathology in a
large majority of ET cases. This study of seven ET, six
tremor-dominant PD and two normal control brains, found no
difference in PC counts between ET, PD, and normal con-
trols. Literature evidence supporting that PC loss is not spe-
cific to ET and the conclusion was discussed. Because some
criticized the study due to small numbers, in 2012 we reported
on 59 autopsy cases including 12 ET, 41 PD, and 6 normal
control brains.53 The PC counts were done by a neuro-
pathologist blinded to the clinical diagnosis. It revealed that
the PC counts were marginally higher in the ET cases com-
pared with the control groups. A recent large, independent
study has confirmed our observations.54 It is concluded that
PC loss is not the pathological basis of ET.

20. 2012. Defective dentate nucleus GABA receptors in essential
tremor.22 This study of 10 ET, 10 PD, and 17 control brains
first time showed reduced GABA receptors in the dentate
nucleus in ET cases.

21. 2014. DNAJC13 mutation in Parkinson disease.24 This study
reports on a large multi-incident Mennonite family with three
autopsy-confirmed Lewy body PD that had DNAJC13
mutation. The first case was seen nearly 30 years before
publication, but took this long to evaluate other family
members and for some affected persons to come to autopsy.
Other seemingly unrelated persons from four different
families of Mennonite ancestry were identified; all but
one family can trace their roots to the Chortitza Mennonite
colony of the Ukraine. The DNAJC13 mutation leads to
toxic gain of function resulting in impaired endosome
transport. This observation furthers our understanding of the
pathogenesis of PD.

22. 2014. Is Parkinson’s disease a vesicular dopamine storage
disorder? Evidence from a study in isolated synaptic vesicles
of human and nonhuman primate striatum.16 The molecular
mechanism of onset and progression of PD pathology
remains unknown. This study included six PD, four normal
control brains, and seven MPTP treated and eight normal
control monkey brains. There was markedly reduced dopa-
mine vesicular uptake and binding in the human PD, but not
in the MPTP-treated monkey brains. This abnormality is
therefore specific to PD. This observation improves our

understanding of the pathophysiology of PD and reinforces
that despite the usefulness of the MPTP model of PD, it does
not represent fully what is going on in human PD.

WHAT MADE OUR RESEARCH MODEL SUCCESSFUL?

Compared with most other centers, we did not have any special
advantages of funding, equipment, manpower, or technical skills.
We believe the success of our research program can be attributed
to the following.

1. Fully integrated clinical and research programs since it was
started in 1968. A large number of cases can be studied
because the program includes all movement disorders seen at
the MDCS. We follow the patients longitudinally, make videos
on all consenting subjects, and perform autopsies wherever
possible. All patients are evaluated at each visit by the same
two neurologists, ensuring consistency of the clinical data.

2. A realistic plan, taking into account the local circumstances.
3. Building a long-term sustainable research program. It has

several components and each involves successful integration
of multiple individuals.

4. Slow but patient. In the earlier years, many of my (Ali)
contemporaries “appeared to be flying in supersonic jets, while
I was walking.”

5. Hard work. In the earlier years, I (Ali) took virtually no
holidays and the research was done over the weekends and
evenings. Although there are many other examples of extra-
ordinary efforts by Saskatchewan Movement Disorders neu-
rologists, one that is easy to understand is the availability. One
of us (AHR) has been on 24/7 autopsy call for 46 years and
emergency freezer call for 32 years, whereas the other (AR)
has been on each of those calls for 14 years, without financial
or academic reward.

6. The support of many others, including the hospital personnel,
who have contributed significantly to this program in their
own ways.

7. Saskatchewan public support. Saskatchewan people are prob-
ably the most generous anywhere, when the term “generosity”
is used in a broad sense. Not only has the public raised large
sums of money from many small donations to support this
work, they have also helped collect research-worthy data and
many families authorized autopsy on their loved ones—even
when there was no possibility of any gain to the family.

8. Cost-effectiveness. Not counting the many voluntary functions
performed by thousands of Saskatchewan people and neuro-
logists over the 46 years, this program has so far cost more than
$20 million. The cost was bearable as it was spread over a long
period.

There is an African saying: “If you want to go quickly, go
alone; if you want to go far, go together.” Together, the Sas-
katchewan public, neurologists, and our collaborators have indeed
traveled far—starting from nothing to being what is considered by
some experts in the field as the best program of its kind.

FUTURE

Our efforts were dictated by circumstances, and circumstances
change with time. The future of this program depends on the new
local realities—the desire of the new local expert neurologists in

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this field and the institution to pursue this model of research. If
handled properly, the future of the program is bright. We have one
of the best resources and have the mechanism in place for ongoing
replenishment. This program can expand to include many other
aspects of PD, ET, and dystonia and also include other movement
disorders.

FORESEEABLE NEEDS

We are not likely to receive a multimillion dollar donation or to
have a very large neurosciences manpower or technological
superiority over other major centers. This research program is
anchored to patient care and specialized research-worthy clinical
data collection. Those functions are performed by the specialty
trained neurologists. By the standards of this institution, it is a
fairly large program. The demands on our (AHR, AR) time are
numerous and we are frequently the bottleneck for the collabora-
tive studies. We appreciate the patience of our colleagues. The
program has reached a point that the two of us, with one (AHR)
retired from the university (though spending more than 50% of his
time on research), cannot take full advantage of the available
opportunities. There are many research options we cannot pursue
because of a lack of medical manpower. There is a need for three
fulltime academic movement disorder neurologists if we wish to
realize the full potential of this program. Appropriate recognition
and support for the multiple tasks which neurologists perform is
vital in order to attract and retain movement disorders experts.

Those who can contribute locally with specialized clinical or
imaging assessments as well as basic science research support are
also needed. New collaborators that bring state-of-the-art expertise
to take advantage of our unique resource are welcome. We are
highly optimistic about the continuing public generosity; however,
there is a need for a more sustained and reliable funding source.

ACKNOWLEDGEMENTS

We are grateful to Greystone Golf Classic, Regina Curling
Classic, and Royal University Hospital Foundation for the major
financial support of the Saskatchewan Movement Disorders
Program.

DISCLOSURES

Ali Rajput has received honoraria from and been a guest
speaker at Parkinson Society Canada.

Alex Rajput received research support from Greystone Golf
Classic, Regina Curling Classic, and Royal University Hospital
Foundation.

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	Outline placeholder
	Introduction and History
	Major Breakthrough
	Impetus for the University of Saskatchewan Movement Disorders Program
	Start of Special Clinics and Research
	Basic Scientists and Clinician Scientist Teams

	Start of Low-Dose LD Therapy
	What Should I Study and How Do I Do That?
	Taking Advantage of the Local Situation and Building Alliances

	Figure 1Adapted from Rajput et�al, Neurology 1984.8
	Early Collaborating Scientists

	Figure 2This form is provided to patients to decide on autopsy for research.
	Outside Collaborators

	Sabbatical Leave
	The Second Phase of Research
	Funding

	Additional Collaborations
	Quebec City – Laval University Group

	Mayo Clinic Jacksonville, Fl/University of British Columbia
	Students and Future Scientists
	Main Components of Saskatchewan Movement Disorders Program
	Clinical Data

	Autopsy Procedure
	Information and Material Storage
	Figure 3Flow chart of Saskatchewan Movement Disorders Program operations.
	Figure 4Pictures of Saskatchewan Movement Disorders program storage of patient records and research material.
	Major Movement Disorders Studied at MDCS

	Our Resource Is Not a Brain Bank
	Figure 5Summary of autopsy studies performed at Saskatchewan Movement Disorders Program and available samples.
	Selected Work of the Saskatchewan Movement Disorders Program
	What Made Our Research Model Successful?
	Future
	Foreseeable Needs
	Acknowledgements
	ACKNOWLEDGEMENTS