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KMID : 0371320000590020254
Journal of the Korean Surgical Society
2000 Volume.59 No. 2 p.254 ~ p.262
Solid and Papillary Neoplasm and Nonfunctioning Islet Cell Tumor Differential Diagnosis and Study of Histopathogenesis by Immunohistochemical Staining
±è´ë°â/Dae-Kyum Kim
ÀÌ»ó´Þ/¹ÚÇظ°/³ë»óÀÍ/ÇãÁø¼®/³ëÀçÇü/¼Õżº/³²¼®Áø/ÃÖ¼ºÈ£/¾çÁ¤Çö/±è¿ëÀÏ/¿À¿µ·û/Sang-Dal Lee/Hai-Lin Park/Sang-Ik Noh/Jin-Seok Heo/Jae-Hyung Noh/Tae-Sung Sohn/Seok-Jin Nam/Seong-Ho Choi/Jung-Hyun Yang/Yong-Il Kim/Young-Lyun Oh
Abstract
Purpose: Solid and papillary neoplasms and nonfunctioning islet cell tumors are both rare pancreatic tumors, and their clinical and pathological features are similar which makes it hard to differentiate between them. Because both tumors have
different
prognoses, it is important to have precise diagnosis. The etiology of solid and papillary neoplasm is not precisely known. The role of sexual hormone has been debated as this tumor occurs mostly in women. Methods: We retrospectively reviewed the
medical
records of 13 patients with solid and papillary neoplasm and 11 patients with nonfunctioning islet cell tumors who had been treated by surgical resection between October 1994 and May 1999 at Samsung Medical Center. Immunohistochemical stainings
were
performed for neuron-specific enolase (NSE), chromogranin, somatostatin, alpha 1-antitrypsin, estrogen (ER), and progesterone (PR) receptors. Results: The average ages of the patients with solid and papillary neoplasms and nonfunctioning islet
cell
tumors were 39.5 and 47.8 respectively. The male to female ratio was 2 to 11 and 6 to 5, respectively and solid and papillary neoplasms were more common in women. CT showed a cystic mass in 76.9% (10/13) of the solid and papillary neoplasm
patients
and
20% (2/10) of nonfunctioning islet cell tumor patients. Lymphadenopathy was noted in 0% (0/13) of the solid and papillary neoplasm cases and in 50% (5/10) of the nonfunctioning islet cell tumor cases, and calcifications were present in 46.2%
(6/13)
and
0% (0/10) of those cases, respectively. The solid and papillary neoplasms were located most commonly in the tail of the pancreas (7 cases), and nonfunctioning islet cell tumors were located most commonly in the head of the pancreas (5 cases). No
malignancies were detected in the solid and papillary neoplasms. Seven cases of the nonfunctioning islet cell tumors (63.6%) were malignant. Both solid and papillary neoplasms and nonfunctioning islet cell tumors stained positive for NSE and
alpha
1-antitrypsin in all cases and they were chromogranin positive in 25% (3/12) and 100% (10/10) and somatostatin positive in 25% (3/12) and 60% (6/10) of the cases, respectively. A solid and papillary neoplasm stained positive for ER in 1 case and
for PR
in 5 cases. However, only 1 case of a nonfunctioning islet cell tumor stained positive for PR. Conclusion: A nonfunctioning islet cell tumor is more malignant tumor than a solid and papillary neoplasm, and age, presence of cysts, lymphadenopathy,
calcification, and chromogranin staining can all be used for differential diagnoses of these tumors. Both the solid and papillary neoplasms and the nonfunctioning tumors are thought to originate from a stem cell capable of differentiating into
endocrine
cells. The sexual hormone seems to have a role in the development of solid and papillary neoplasms.
KEYWORD
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