Chapter 1 Introduction
The disease
1.1
Chronic and clinically significant adhesive arachnoiditis is a painful
condition caused by long term scarring of the arachnoid membrane, one of the
membranes that surround and protect the nerves of the spinal cord and spinal
nerves. Inflammation from medical intervention or infection can lead to the
formation of scar tissue, which causes the spinal nerves to ‘stick’ together,
hence the descriptive term ‘adhesive’ arachnoiditis which is used in this
report. This ‘tethering’ of the spinal nerves can prevent them from moving
freely as an individual moves, triggering pain and other symptoms.
1.2
Sufferers of adhesive arachnoiditis experience a range of symptoms,
including:
- pain, particularly
affecting the lower back and legs, often intense and leading to decreased
mobility or in severe cases paralysis;
- bladder and bowel
dysfunction; and
- impaired sexual
function.
1.3
There are no reliable data on the prevalence or incidence of adhesive
arachnoiditis in Australia (or apparently elsewhere) as the necessary clinical
data do not exist.[1] However, it was clear to
the Committee at the roundtable that the impact of adhesive arachnoiditis on
the lives of sufferers and their families can be devastating.
1.4
The aetiology (i.e. clinical cause) of adhesive arachnoiditis is
complex. Causes and risk factors associated with the development of adhesive
arachnoiditis include:
- complications of
bacterial and viral infections;
- degenerative back
conditions such a disc herniation or spinal stenosis;
- trauma to the back or
spine due to injury or multiple surgical procedures; and
- exposure of the
spinal cord and surrounding membranes to a range of therapeutic and diagnostic
agents.
1.5
Reports on the relative contribution of these factors to the development
of adhesive arachnoiditis vary. It is often very difficult to establish a
single causative event for individuals with adhesive arachnoiditis, as many
sufferers will have experienced more than one risk factor.
1.6
For those with a diagnosis with adhesive arachnoiditis, treatment
options are limited and the prognosis is poor. There is no cure for adhesive
arachnoiditis and treatment is primarily pain management and assistance with
functional impairment.
Context of the Committee’s inquiry
1.7
Adhesive arachnoiditis was first brought to the attention of the House
of Representatives Standing Committee on Health and Ageing (the Committee) by a
member of the Committee in the context of constituent concerns raised by affected
individuals and/or their carers.
1.8
On 19 September 2011, during the grievance debate, the Committee’s
deputy Chair Mr Steve Irons MP, called for the Committee to inquire into specific
matters associated with adhesive arachnoiditis. A key issue raised by Mr Irons
was the extent to which certain diagnostic agents, specifically the oil-based
contrast media marketed as Myodil by the UK product manufacturers and
Pantopaque by the USA product manufacturers[2], caused adhesive
arachnoiditis. These oil-based contrast media, containing iophendylate dye as
the main active ingredient, were used to help clinicians determine the causes
of chronic back conditions in affected individuals. The contrast media were injected
into the cerebrospinal fluid (CSF) in a process known as myelography. This allowed
details of the spinal cord and spinal nerves to be visualised by X-ray.
1.9
The oil-based contrast media Myodil and Pantopaque were used in
myelography from the 1950s to the 1980s in Australia and elsewhere, including
the UK and USA. As a consequence, often many years post-procedure, some
individuals have developed adhesive arachnoiditis.
1.10
A number of those affected have subsequently litigated seeking compensation
from the product manufacturers. The basis of many of their claims for
compensation is that the product manufacturers provided insufficient warnings
about product safety and did not appropriately react to the evolving scientific
literature. While the outcomes of litigation have varied according to
individual circumstances, it is clear that some individuals in Australia and
overseas have received out of court settlements from product manufacturers.[3]
These out of court settlements were made by the product manufacturers without
admission of guilt. The Committee comments further on litigation in Chapter 2
of the report.
1.11
Mr Irons’ speech is not the first time that adhesive arachnoiditis has
been debated in the House. In 2002 several Members of Parliament debated the condition,
and matters relating to adhesive arachnoiditis were subject to questions on
notice directed to the then Minster for Health.[4] While all speakers on the
issue acknowledged the seriousness of the condition and its impact on sufferers,
opinions differed on the whether a committee inquiry into adhesive arachnoiditis
was warranted.[5]
Scope and conduct of the inquiry
1.12
On 22 May 2012 the Committee resolved to investigate the issue of
adhesive arachnoiditis further.[6] To assist the Committee
to determine the nature and scope of its investigations it initially received a
private briefing on 14 August 2012 from a clinical neurologist and a
representative of the Therapeutic Goods Administration. On the basis of
information from that briefing the Committee undertook to focus on the
aetiology, diagnosis, treatment and prognosis of adhesive arachnoiditis.
1.13
As noted, the Committee is aware of litigation relating to exposure to
Myodil and/or Pantopaque and the development of adhesive arachnoiditis. In conducting
its inquiry into adhesive arachnoiditis the Committee is of course mindful that
the courts are independent of the Parliament. The Committee also emphasises
that it does not have the authority to order compensation with respect to the
use of Myodil or Pantopaque. Individuals who are considering such legal action
should obtain their own independent medical assessment and legal advice. It is
in this context that the Committee has sought to investigate issues associated
with adhesive arachnoiditis with a view to assisting sufferers by raising the
profile of the condition and considering practical options for support.
1.14
To progress its investigations into adhesive arachnoiditis the Committee
resolved to hold a public roundtable in Canberra on 21 September 2012. The
Committee invited a range of participants with experience of adhesive arachnoiditis.
The roundtable opened with introductory statements by teleconference from Professor
Marcus Stoodley, Professor of Neurosurgery, Macquarie University in New South
Wales (NSW) and from Professor Michael Cousins, Royal Australasian College of
Physicians. Other participants at the roundtable were:
- Ms Ruth Ahrens, Vice
President, Australian Arachnoiditis Sufferers Association and sufferer;
- Professor Chris
Baggoley, Chief Medical Officer, Department of Health and Ageing;
- Ms Bernadette Clarke,
sufferer;
- Dr Tony Gill, Acting
Principal Medical Adviser, Therapeutic Goods Administration;
- Mr Joern Hagemann, sufferer;
- Ms Maureen McLean,
President/Secretary, Australian Arachnoiditis Sufferers Association (NSW) and
sufferer;
- Professor Michael
Sage, Royal Australian and New Zealand College of Radiologists;
- Mr Max Scott, sufferer
(teleconference); and
- Mrs Erika Zorzit, daughter
and carer of Mr Hagemann.
1.15
Following the roundtable, the Committee also took ‘in-camera’ evidence
from representatives of GlaxoSmithKline (GSK), the product manufacturer of Myodil.
On the same day as the roundtable GSK posted a press release on its website
outlining its position on the use of Myodil and the development of adhesive
arachnoiditis (at Attachment A). Subsequently GSK also provided the Committee
with a range of information in correspondence to the Committee, including product
information sheets for Myodil from the 1970s.[7]
1.16
The Committee very much appreciates the contributions of all participants
to its inquiry. The roundtable made clear to the Committee how debilitating adhesive
arachnoiditis can be to sufferers. The Committee very much sympathises and
hopes that the recommendations in the report will help to improve quality of
life for sufferers, and their families and carers.