 |
2nd
NM Convention
21-22 July, 2007 Barony Castle Hotel Eddleston, Scottish Borders |
| Friday | Guests arrival day and informal social evening. | |
| Saturday program | ||
| 07:30 - 09:00 | Breakfast served in dining room | |
| 09:30 | David McDougall | Welcome and introductions |
| 10:00 |
Dr. Anita Simonds - Consultant Respirologist |
Update in respiratory care |
| 11:00 | Break | |
| 11:30 | Marina Morrow - Senior Physiotherapist Glasgow |
Physiotherapy in Myopathies |
| 12:30 | Maggiorine de Muralt | Dolphin Therapy - Starring Philippe de Muralt |
| 13:00 | Buffet lunch | |
| 14:00 - 16:00 | Falconry Scotland | Falconry flying and static display |
| 16:00 - 16:30 | Official NMC07 group photogragh | |
| 16:00 - 19:00 | Trip to Kalzie Gardens (optional) | |
| 19:00 | Dinner and NM Community 8th Birthday Party | |
Sunday program |
||
| 07:30 - 09:00 | Buffet breakfast served in dining room | |
| 09:30 | Dr. Carina Wallgren-Pettersson Consultant in Medical Genetics Dept. of Medical Genetics University of Helsinki & Folkhalsan |
My nemaline story |
| 10:30 | Break | |
| 11:00 | Professor Nigel G Laing NH&MRC Principal Research Fellow Centre for Medical Research University of Western Australia M519 West Australian Institute for Medical Research |
"My journey with nemaline myopathy - from Alice Springs to testing potential therapy." (see abstract below) |
| 12:00 | Open Room Q & A | |
| 13:00 | Barony BBQ or buffet (weather dependant) | |
| 16:00 | Close |
| Abstract |
| "My journey with nemaline myopathy - from Alice Springs
to testing potential therapy."
Nigel G Laing, Centre for Medical Research, University of Western Australia, Western Australian Institute for Medical Research, B Block QEII Medical Centre, Nedlands, Western Australia 6009, Australia. My research into nemaline myopathy started in 1989 because of a large
South Australian family with dominant nemaline myopathy. This family
had ten living affected family members and was the first opportunity
to find any gene for nemaline myopathy. In 1992 we demonstrated that
the disease gene in the family was within an approximately 27 million
base pair region on chromosome 1. In 1995, we demonstrated that the
mutated gene in this family was the gene for slow alpha-tropomyosin
(TPM3). Tropomyosin is a protein component of the muscle thin filament
and this pioneering result moved the nemaline myopathy focus from the
Z-disc to the thin filament. We now know of 5 additional thin filament
protein genes which when mutated may cause nemaline myopathy: nebulin
(NEB - found in 1999); actin (ACTA1 -1999), beta tropomyosin (TPM2 -
2000); slow troponin T (TNNT1 - 2000); cofilin (CFL2 - 2007). Most nemaline
myopathy patients have mutations in nebulin, with mutations in actin
being the second most common cause of nemaline myopathy and the main
cause of the severe cases of nemaline myopathy. Actin mutations were
first found in my laboratory and we have over the last few years concentrated
on that gene. We now know of over 130 different mutations in actin associated
with congenital myopathies. Mutations in actin may cause dominant or
recessive diseases, but most patients have new mutations not present
in either parent. Since we first found mutations in skeletal actin,
we have thought that it might be possible to use cardiac actin, the
actin we normally have in our hearts and in our skeletal muscles before
we are born, to treat skeletal actin diseases. Recently we identified
a number of nemaline myopathy patients with recessive actin disease
who, because of the precise mutations they have in their actin gene,
have no skeletal actin at all. We showed that these patients have retained
cardiac actin instead of skeletal actin in their skeletal muscles and
that the patients with the most cardiac actin in their skeletal muscles
have done the best. This adds weight to our theory that cardiac actin
might be used to treat skeletal actin diseases and we have begun further
investigations to test if cardiac actin can replace skeletal actin in
experimental models of nemaline myopathy. |