Departments of *Pathology ∥Surgery, University of Pittsburgh Medical Center, Pittsburgh, PA Departments of †Pathology ‡Oncology §Surgery, The Sol Goldman Pancreatic Cancer Research Center, Johns Hopkins University School of Medicine, Baltimore, MD.
Am J Surg Pathol. 2013 Sep;37(9):1329-35. doi: 10.1097/PAS.0b013e3182a1ad72.
Acinar cell cystadenoma (ACA) of the pancreas was initially described as a non-neoplastic cyst of the pancreas and, at that time, referred to as "acinar cystic transformation." In subsequent studies, these lesions were given the designation of "-oma," despite the relative lack of evidence supporting a neoplastic process. To characterize these lesions further, we examined the clinical, pathologic, and immunohistochemical features of 8 ACAs. The majority of patients were female (7 of 8, 88%) and ranged in age from 18 to 57 years (mean, 43 y). Grossly, the cysts involved the head (n=5), body (n=1), or the entire pancreas (n=2). ACAs were either multilocular (n=4) or unilocular (n=4) and ranged in size from 1.8 to 15 cm (mean, 6.8 cm). Histologically, multilocular ACAs were lined by patches of acinar and ductal epithelium. Immunolabeling, including double-labeling for cytokeratin 19 and chymotrypsin, highlighted the patchy pattern of the ductal and acinar cells lining the cysts. In some areas, the cysts with patches of acinar and ductal differentiation formed larger locules with incomplete septa as they appeared to fuse with other cysts. In contrast, the unilocular cases were lined by 1 to 2 cell layers of acinar cells with little intervening ductal epithelium. Nuclear atypia, mitotic figures, necrosis, infiltrative growth, and associated invasive carcinoma were absent in all cases. In addition, we assessed the clonal versus polyclonal nature of ACAs, occurring in women, using X-chromosome inactivation analysis of the human androgen receptor (AR) gene. Five of 7 cases were informative and demonstrated a random X-chromosome inactivation pattern. Clinical follow-up information was available for all patients, and follow-up ranged from 10 months to 7.8 years (mean, 3.6 y), with no evidence of recurrence or malignant transformation. We hypothesize that early lesions are marked by acinar dilatation that expands into and incorporates smaller ductules and later larger ducts. As the cysts increase in size, they fuse forming larger cysts. Later lesions demonstrate a unilocular cyst lined by predominantly acinar epithelium with scattered ductal cells. The term cystadenoma, with its neoplastic connotation, does not seem to accurately reflect the histologic, immunohistochemical, or molecular features of these lesions. We suggest readopting the term "acinar cystic transformation" until the non-neoplastic versus neoplastic origin of these lesions can be resolved.
胰腺腺泡细胞囊腺瘤(ACA)最初被描述为胰腺的非肿瘤性囊肿,当时称为“腺泡囊性转化”。在随后的研究中,尽管缺乏支持肿瘤过程的相对证据,但这些病变被指定为“-oma”。为了进一步描述这些病变,我们检查了 8 例 ACA 的临床、病理和免疫组织化学特征。大多数患者为女性(8 例中的 7 例,88%),年龄在 18 至 57 岁之间(平均 43 岁)。大体上,囊肿累及头部(n=5)、体部(n=1)或整个胰腺(n=2)。ACA 为多房性(n=4)或单房性(n=4),大小为 1.8 至 15 cm(平均 6.8 cm)。组织学上,多房性 ACA 由腺泡和导管上皮的斑块组成。免疫标记,包括细胞角蛋白 19 和糜蛋白酶的双重标记,突出了囊壁上皮中腺泡和导管细胞的斑块状模式。在某些区域,具有腺泡和导管分化斑块的囊肿形成较大的腔室,不完全分隔,因为它们似乎与其他囊肿融合。相比之下,单房性病例由 1 至 2 层细胞的腺泡细胞组成,其间有很少的导管上皮。所有病例均无核异型性、有丝分裂象、坏死、浸润性生长和相关浸润性癌。此外,我们使用人类雄激素受体(AR)基因的 X 染色体失活分析评估了发生在女性中的 ACA 的克隆与多克隆性质。7 例中有 5 例信息丰富,表现出随机的 X 染色体失活模式。所有患者均获得临床随访信息,随访时间从 10 个月到 7.8 年(平均 3.6 年),无复发或恶性转化证据。我们假设早期病变的特征是腺泡扩张,扩张并纳入较小的小管,然后是较大的导管。随着囊肿的增大,它们融合形成更大的囊肿。后期病变表现为主要由腺泡上皮组成的单房性囊肿,伴有散在的导管细胞。囊腺瘤一词带有肿瘤学的含义,似乎不能准确反映这些病变的组织学、免疫组织化学或分子特征。我们建议重新采用“腺泡囊性转化”一词,直到这些病变的非肿瘤性与肿瘤性起源得到解决。
