--part1_f4.890d304.27f7e511_boundary
Content-Type: text/plain; charset="US-ASCII"
Content-Transfer-Encoding: 7bit

Peggy et. al.,
Our protocol (from Dr. Sumi @ U. of W. neuropath) requests the following for 
optimal
neuropathathology workup on a muscle biopsy:
       1.  One biopsy "unclamped" for muscle enzyme histochemistry (Note, for 
the           reasons of clamp artifact and the desired uncrushed relaxation 
of  the fibers, as you noted.)  This portion is snap frozen in a relaxed 
state @ -160 degrees C. in  Isopentane cooled by liquid nitrogen.
       2.  A 2nd biopsy in a clamp and allowed to fix in this state in 10% 
NBF for 24 hours before resection of the "uncrushed" portion of the biopsy 
from between the tines of the clamp(for routine L.M. if needed).
       3.  A 3rd biopsy (as in #2 above) but in Trump's fixative for E.M. if 
needed.
Our feeling is that if the patient is going to undergo an open biopsy 
procedure we should harvest all materials necessary for a complete and 
definitve neuropathology assessment.  The only time we compromise on these 
specimen requirements are when the patient is a pediatric or a Shriner's 
patient when there is concern for the amount of the muscle compromise to the 
young patients.  I understand that often not all three of these specimens are 
necessary for diagnosis, but after getting the patient all the way into an 
invasive surgical procedure, which is for the sole purpose of obtaining a 
tissue diagnosis,  I would advocate a multiple bx/fixative approach.
Greg Luck
Anat.Path. Sup.
Deaconess Med Center
Spokane, WA

--part1_f4.890d304.27f7e511_boundary
Content-Type: text/html; charset="US-ASCII"
Content-Transfer-Encoding: 7bit

<HTML><FONT FACE=arial,helvetica><FONT  SIZE=2>Peggy et. al.,
<BR>Our protocol (from Dr. Sumi @ U. of W. neuropath) requests the following for 
<BR>optimal
<BR>neuropathathology workup on a muscle biopsy:
<BR>       1.  One biopsy "unclamped" for muscle enzyme histochemistry (Note, for 
<BR>the           reasons of clamp artifact and the desired uncrushed relaxation 
<BR>of  the fibers, as you noted.)  This portion is snap frozen in a relaxed 
<BR>state @ -160 degrees C. in  Isopentane cooled by liquid nitrogen.
<BR>       2.  A 2nd biopsy in a clamp and allowed to fix in this state in 10% 
<BR>NBF for 24 hours before resection of the "uncrushed" portion of the biopsy 
<BR>from between the tines of the clamp(for routine L.M. if needed).
<BR>       3.  A 3rd biopsy (as in #2 above) but in Trump's fixative for E.M. if 
<BR>needed.
<BR>Our feeling is that if the patient is going to undergo an open biopsy 
<BR>procedure we should harvest all materials necessary for a complete and 
<BR>definitve neuropathology assessment.  The only time we compromise on these 
<BR>specimen requirements are when the patient is a pediatric or a Shriner's 
<BR>patient when there is concern for the amount of the muscle compromise to the 
<BR>young patients.  I understand that often not all three of these specimens are 
<BR>necessary for diagnosis, but after getting the patient all the way into an 
<BR>invasive surgical procedure, which is for the sole purpose of obtaining a 
<BR>tissue diagnosis,  I would advocate a multiple bx/fixative approach.
<BR>Greg Luck
<BR>Anat.Path. Sup.
<BR>Deaconess Med Center
<BR>Spokane, WA</FONT></HTML>

--part1_f4.890d304.27f7e511_boundary--