POST-SURGERY RECOVERY
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Transcript POST-SURGERY RECOVERY
HISTORY - ? myopathy
Weakness
vs fatigue:
– Proximal vs distal (DM1, sIBM, FSH, nemaline rod,
distal myopathy (TCAP (telethonin), hIBM (GNE)).
– Exercise related (MG, metabolic, pseudometabolic).
– Daily “fatigue”, “trashed”, “tired all the time” are
not mainfestations of ANY NMD except DM1.
Pain:
– Joint vs muscle.
– Pain at rest is rarely neuromuscular disease (DM2,
rare myotonia congenita, statin myopathy).
– Most inflammatory myopathies are painless.
HISTORY - family
Multiple
systems involved?
– DM2, mitochondrial disease.
Family
history:
– AD – DM2, OPMD, FSHD,
LGMD, EDMD (lamin A/C).
– AR – GSD-II, SMA-IV.
– Maternal – mtDNA defects.
– XLR – BMD, EDMD.
Physical Exam
Complete
Neurological Exam.
MSK exam
– trochanteric bursitis may
mimic proximal leg
weakness/fatigue.
– FSHD may get rotator cuff
issues.
– Contractures.
Check the back (spinal stenosis
with radiculopathy can mimic
myopathy, lead to fatigue with
activity, and elevate CK).
Routine Bloodwork
CK
not aldolase.
Remember that AST and ALT are in skeletal muscle.
Cramps – Ca, Mg (cramps at rest are rarely significant
BUT they can increase the CK).
Make sure TSH is sent (commonly the CK will be
elevated).
Patients with motor neuropathy and motor
radiculopathy can have elevated CK (< 1,000 U/L).
Cause of HyperCKemia
Sarcolemma
leak/damage.
All cytoplasmic proteins.
Seen in many but not all
muscle disorders .
Huge variability between
people (men>women;
African > Caucasian).
EXERCISE: ~ 4h post and
up to 10 days.
CK
LDH
AST
ALT
Aldolase
Myoglobin
When to send for further testing.
No
cause for the high CK.
Neurological exam is abnormal (beyond radiculopathy
or diabetic neuropathy).
Any CK over 1,000 iU/L.
Positive family history of high CK or NMD or
arrhythmia/pacer or non-hypertensive cardiomyopathy
(lamin A/C, BMD)(HOCM screen @ CHEO).
SOBOE + weakness (Pompe, MG, LGMD, mito.).
– Sitting/supine FVC - > 20 % drop = diaphragm weak.
Needle EMG
Fibs./PSW
Myotonia
Myopathic
Potentials
Muscle Biopsy
Bourgeois and Tarnopolsky, Mitochondrion,
4:441-52, 2004.
Tarnopolsky, et al, Muscle Nerve, 2011.
Biopsy Patterns
Central Core
Ragged Red
Inflammation
Dennervation
Dystrophic
Pompe
EM Changes
Myopathies
Muscle
–
–
–
–
–
–
–
INFLAMMATORY.
DYSTROPHY.
TOXIC/INFECTIOUS.
METABOLIC.
CONGENITAL MYOPATHY.
ENDOCRINE.
CHANNELOPATHY.
Inflammatory Myopathies
Polymyositis.
Dermatomyositis.
Inclusion Body Myositis.
Myositis associated with
connective tissue
disorders (MCTD, RA,
lupus)
Rashes, etc.
Gottron’s
Papules
Rash on
knuckles –
Gottron’s Sign
Shawl Sign
Heliotrope
Rash
Calcinosis
Diagnosis – DM/PM.
proximal weakness.
CK activity.
+ EMG.
+ Biopsy.
Rash.
Definite
PM
all 4
DM
3 or 4 + R
Probable
3/4
2+R
Possible
2/4
1+R
Diagnosis-IBM
More common in older men.
Quadriceps and finger flexor
atrophy.
CK is elevated but mild/moderate.
EMG is often distinct from others.
Swallowing affected in about 70 %.
Biopsy shows rimmed vacuoles (+
αB crystallin, tau, APP) + COX –
ve.
Muscular Dystrophy
Dystrophinopathy
LGMD
OPMD
(AD, ptosis NOT
ophthalmoplegia, dysphagia,
onset 40 - 50 y)
Congenital
DM1/DM2
Distal (TCAP)/hIBM (GNE)
FSHD
Dx: ? Dystrophinopathy - gene first
(MLPA - HSC = 66 %) > biopsy.
BMD
NORM
Gene Seq.
DMD
WESTERN BLOTTING
I.H.C.
Dystrophinopathies
Duchenne:
–
–
–
–
–
XLR, 1/3500 live male births.
weakness age 3 – 4 y.
CK – 10,000’s.
W/C by teens.
Death resp. failure in 20’s.
Becker’s:
– Less common.
– Milder phenotype.
– CLINICAL - ++ calf hypertrophy, quads affected (atrophy)
with relative preservation of upper extremeties.
Myotonic Dystrophy-1.
AD
trinucleotide disorder
(CTG), ch. 19.
~1.4/10,000 live birth.
Disease affects multiple
systems (somnolent, cataracts,
dysphagia, conduction blocks,
GI issues, distal weakness).
Rough correlation with size of
CTG expansion. (CHEO).
Anticipation (females).
Myotonic Dystrophy-2.
Chr.
3, AD.
No congenital form.
CCTG repeat in ZNF9 (Zn finger)(CHEO).
Weakness is mainly proximal (“PROMM”).
Usually not suspected until the EMG.
Cataracts are very common, conduction block risk is
similar to DM1 (~ 50 % will get at least a 1st degree).
Muscle pain is common.
LGMD
Sarcoglycanopathies
(α,β,γ,δ –
sarcoglycan)
– 60 % of kids; 10 % adults.
Calpainopathy
(Calpain 3)
– 10 – 30 % of late-childhood/adult.
Bethlem/Ullrich
Myopathy
– Early contractures (elbows, Achilles).
– COL6A1,2,3 mutations.
Dysferlinopathy
– Very high CKs/inflammation on Bx.
FSHD
AD
condition (variable).
Type 1 = Chr. 4q33
deletion (CHEO).
Early adult onset.
FSH distribution.
Dorsi-flexion and
asymmetrical weakness
are common.
Usually normal lifespan.
No significant cardiac
Pompe Disease
• First described in 1932 by Dutch pathologist J.C.
Pompe
• Also known as acid maltase deficiency (AMD) or
GSD-II.
• Characterised by the deficiency of
a lysosomal enzyme, acid alpha-glucosidase (GAA)
• Results in progressive intracellular accumulation of
glycogen, primarily in muscle cells
• Signs and symptoms begin anywhere from early
infancy through adulthood
Onset of Pompe Disease in Adults
Age-specific distribution of events in a Dutch cohort of mean age 48.6 years
Black line = mean age for event
First complaints
n=54
Running problems
n=31
Diagnosis
n=54
Problems going up and down staircase
n=46
Problems rising from armchair
n=45
Problems rising from lying position
n=37
Walking problems
n=41
Problems with dressing
n=32
Problems going to toilet
n=18
Start of walking aid use
n=23
Start of wheelchair use
n=26
Start use of artificial ventilation
(n=54)
n=20
0
10
20
30
40
50
60
Figure from Hagemans ML, Winkel LP, Van Doorn PA, et al. Clinical manifestation and natural course of late-onset Pompe's disease in 54 Dutch patients. Brain 2005;
128:671-7, by permission of Oxford University Press.
70
yrs
Pompe – diagnosis.
form (AR) – shortness of breath, proximal
weakness, contractures.
CK usually up.
EMG – fibs, PSW, myotonia – paraspinals.
EM – membrane bound glycogen, autophagic
vacuoles.
LM – PAS increase (blebs), acid phosphatase +ve,
vacuolar myopathy.
Fibroblasts/muscle/blood spot –
reduction of -glucosidase.
Adult
Biopsy Patterns
ADULT
INFANT
Drugs associated with myopathy
AZT – mitochondrial.
Corticosteroids – type 2
atrophy; ICU – myosinolysis
+/- NDMBAs.
Ethanol – acute rhabdo.
Hydroxychoroquine.
Neuroleptics – NMS, CK.
d-penicillamine (MG,
inflammatory).
Lithium ( K+, rhabdo).
Retinoic acid (vitamin A).
Interferon.
Antibiotics (Macrolides)
Cholesterol lowering agents:
– HMG-CoA reductase inhibitors
(fibrates, cholchicine, cyclosporine).
– Fibric acid derivatives
Statins and myopathy.
3
- 5 % of patients develop myalgias.
0.1 % = rhabdomyolysis (10 X ULN).
? direct toxicity (phrenylation, COQ10).
Recently there is evidence of delayed onset
necrotic myopathy responsive to
immunomodulation (Amato, M and N; Mammen,
AL, Arthritis and Rheum, 63:713-, 2011) =
statins induce expression of anti-HMGCR
autoanitbodies.
Statin myositis.
100
% of patients had myonecrosis.
20 % showed “inflammation”.
MOST of the patients in both studies responded
to MTX and prednisone.
27/28 of our patient IDed in past 4 years
responded to MTX and prednisone - one needed
pulse solu-medrol and IgG.
50 % of our patients had inflammation in biopsy.
Case # 1- Calf atrophy
26
y old male with difficulty getting up from
squat age 19 y > progressive.
Family history - parents are consanguinous
(paternal great grandmother is sister to his
maternal great grandmother), one sister with
similar phenotype and brother sister no weakness.
Examination: MS/CN = N; MOTOR = minimal
proximal UE weakness, profound calf > anterior
lower leg atrophy and weakness with hip flexors
= 2/5 and hamstrings 3/5.
Case # 1- Calf atrophy.
Muscle
biopsy = inflammation, N - dysferlin.
CK > 3,000 iU.
Dx: inflammatory myopathy - no response to
corticosteroids.
Rheumatologist wanted a second opinion.
Patient wanted to know about Rx options.
Case # 1= New mutation
Whole
DYS gene sequenced.
Mutation analysis = c.4747 T>G transversion
(homo); p.Tyr1583Asp.
Athena = “Since these types of sequence variants are similar to
those observed in both disease-associated mutations and benign
polymorphisms, the nature of this variation precluded clear
interpretation.”
in
silico evaluation:
– SIFT = “not tolerated”
– PolyPhen = “probably damaging”, score = 3.024.
– Tyr = tyrosine is highly conserved 46/46 vertebrata.
Case # 1 - Molecular issues
claims that they can detect 99 % of DYS
cases with a blood lyphocyte Western blot.
We found that the immunohistochemistry was
normal in this case and many others.
We ran Western blotting and found none,
reduced, normal and overexpression in 9 cases.
Athena
Muscle Nerve. 2013 May;47(5):740-7. Dysferlin aggregation
in limb-girdle muscular dystrophy type 2B/myoshi myopathy
necessitates mutational screen for diagnosis.
Nilsson MI, Laureano ML, Saeed M, Tarnopolsky MA.
Case # 2– Lumber Jack!
69 y RHD male.
PMHx:
Angioplasty – 1995
Meds: Simvastatin, ASA,
atenolol, terazocin, vits
B/C/E
HPI: tree cutting x 2 ++
DOMS w/ CK to 4869 then
dropping to 341 over 2 d
Case # 3: Fibromyalgia?
59
y old female.
Dx = fibromyalgia for 20 + y.
Hx: non-specific pains and weakness for > 20
years and fatigue with exercise + more recent
SOBOE - Dx = sleep apnea + obesity.
O/E: MS - N; CN - N; MOTOR - ~ 4/5 prox.
weakness; MSR - N; sensory -N.
CK = 678 U/L; EMG = fibs, PSW, small, brief
(incl. paraspinals).
Spirometry: FVC = 2.1 L/ FEV1 = 1.9 L/s
Case # 3- Testing
DBS
= low GAA activity
Biopsy =
Genetics
= c.692+5G>T (known - alters splicing
of mRNA in 3’ region of exon 3); c.1211A>G;
p.Asn404Gly).
The clinic:
Ms. L. Brandt
Ms. Erin Hatcher
Ms. L. Brady
Ms. D. Johnston
Ms. H. Vey
Ms. K. Scott
The lab:
Dr. M. Nilsson
Dr. M. Akhtar
Dr. L. MacNeill
Mr. D. Ogborn
Collaborators:
Dr. B. Lach
Dr. J. Provias
Dr. J. Bourgeois
Dr. T. Hawke
Dr. J. Schertzer
Thanks
• Warren Lammert and Family
• CIHR – Institute of aging.
• McMaster Children’s Hospital and
Hamilton Health Sciences Foundation.