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Author: Charles Richert
Date: 03/14/97
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<HEAD><title>Consult Report - Case 29</title></HEAD>
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<IMG SRC="/tpis/icons/purpball.gif"><i> Contributed by Anthony
Demetris, M.D.</A></i>
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<b>PATIENT HISTORY:</b>
Per referral letter, the patient is a 57-year-old Saudi male with
end stage liver disease due to Hepatitis B who was transplanted
on 12/2/96. He has had good liver functions until quite
recently. He developed a persistent fever which has defied every
work up. He has been cultured from every site, scanned from head
to toe, surgically explored, and biopsied in multiple locations.<P>
An excisional biopsy of a supraclavicular lymph node turned out
to be a localized area of necrosis within the subcutaneous
tissue. There is no real granuloma formation or evidence of a
pre-existing lymph node. All cultures have been negative. No
evidence of PTLD. He has been imperically treated with numerous
antibiotics, anti-fungal agents, and anti-tuberculous agents--all
without result. Currently, his serum chemistries are TB 15.9; AP
255; GGT 345; AST 340; ALT 276, ALB 2.9; PT 13.8. His
immunosuppression has been discontinued. Review of outside
material.
<hr>
<a name="final"></a>
<H4>Final Diagnosis (Case 29) [D808-97]</H4>
LIVER ALLOGRAFT, NEEDLE BIOPSY -<BR>
<ol type=A>
<li>MILD ACUTE CELLULAR REJECTION WITH PROMINENT CENTRAL
VENULITIS AND FOCAL HEPATOCELLULAR DROPOUT.
<li>LOBULAR DISARRAY, KUPFFER CELL HYPERTROPHY AND HEPATOCYTE
REACTIVE CHANGES; HEPATITIS B VIRUS INFECTION AND SEPSIS
SHOULD BE EXCLUDED (SEE MICROSCOPIC DESCRIPTION).
<li>PORTAL AND PERIPORTAL HEMORRHAGE, CAUSE UNCERTAIN.
</ol><p>
<i><b>Previous Biopsies on this Patient:</b></i><br>
NONE<p>
<i><b>TPIS Related Resources:</b></i><br>
<a href="/tpislibrary/schema/BanffRej.html">Liver Allograft Rejection Grading</a><br>
<a href="/tpislibrary/liver/index.html">Liver Transplant Topics</a><p>
<a name="gross"></a>
<hr><H4>Gross Description - Case 29 [D808-97]</H4>
The specimen consists of three (3) consult slides labeled D808-97
(2) and D50-97 (1). No surgical pathology
report is received with the specimen.
<p>
<a name="micro"></a>
<HR><H4>Microscopic Description - Case 29 [D808-97]</H4>
<A HREF="/tpis/images/H00056a.jpg"><IMG
SRC="/tpis/images/tnails/H00056a.jpg" width=133 height=100></a>
<A HREF="/tpis/images/H00056b.jpg"><IMG
SRC="/tpis/images/tnails/H00056b.jpg" width=133 height=100></a>
<A HREF="/tpis/images/H00056c.jpg"><IMG
SRC="/tpis/images/tnails/H00056c.jpg" width=133 height=100></a>
<A HREF="/tpis/images/H00056d.jpg"><IMG
SRC="/tpis/images/tnails/H00056d.jpg" width=133 height=100></a>
<P>
The normal lobular architecture is distorted by portal expansion
because of edema and focal hemorrhage. There is also a mild
focal, predominantly mononuclear portal infiltrate and focal bile
duct infiltration and damage are identified.<P>
The most striking changes are in the lobule. There is zonal
centrilobular hepatocellular dropout, lymphoplasmacytic
inflammation, congestion and hemorrhage. Focal central venulitis
is also appreciated. Mild perivenular fibrosis is seen.
However, there is also marked Kupffer cell hypertrophy, and
reactive changes of hepatocytes including an increased
nuclear:cytoplasmic ratio, spotty acidophilic necrosis of
hepatocytes, and macronucleoli.<P>
Compared to the previous biopsy there has been a marked increase
in the centrilobular dropout and inflammation along with the
congestion and hemorrhage.<P>
Overall, the histopathological changes suggest that more than one
process is contributing to the pathologic changes. First, the
zonal centrilobular dropout with central plasmacytic inflammation
and focal lymphocytic duct damage suggests a component of acute
cellular rejection with central venulitis. However, it is
difficult to explain the panlobular disarray, marked hepatocyte
reactive changes, and Kupffer cell hypertrophy on the basis of
rejection alone. These changes can be seen with hepatitis B
viral infection of the liver, sepsis and reactive/regenerative
change from vascular compromise, which last of which appears to
have been excluded by imaging studies. Immunohistochemical
stains to exclude HBV infection are suggested.<P>
Lastly, the cause of the portal and periportal hemorrhage is
uncertain. I have seen this change in intra-operative needle
biopsies after vigorous manipulation of the liver for operative
access, which presumably causes torsion between the portal tracts
and the surrounding, less rigid, parenchyma. Other causes of
portal and periportal hemorrhage include DIC and humoral
rejection. However, none of these possibilities appear to be
viable options based on the clinical profile and other
histopathological findings.
<P>
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