Understanding the clinical impact of MUC5AC expression on pancreatic ductal adenocarcinoma

A Manne, A Esnakula, L Abushahin, A Tsung - Cancers, 2021 - mdpi.com
A Manne, A Esnakula, L Abushahin, A Tsung
Cancers, 2021mdpi.com
Simple Summary Management of pancreatic cancer is challenging as there are limited
treatment options, and most cases are diagnosed at advanced stages. In addition, there are
no dependable tests available to predict bad outcomes or treatment responses in current
clinical practice. Here, we shed light on the available evidence on mucin, MUC5AC in
predicting the outcome of pancreatic cancers. We also discuss variants of MUC5AC
believed to have a role in the malignant transformation of pancreatic tissues. Abstract Mucin …
Simple Summary
Management of pancreatic cancer is challenging as there are limited treatment options, and most cases are diagnosed at advanced stages. In addition, there are no dependable tests available to predict bad outcomes or treatment responses in current clinical practice. Here, we shed light on the available evidence on mucin, MUC5AC in predicting the outcome of pancreatic cancers. We also discuss variants of MUC5AC believed to have a role in the malignant transformation of pancreatic tissues.
Abstract
Mucin-5AC (MUC5AC) is a heavily glycosylated gel-forming secreted mucin with a reliable prognostic value when detected in multiple malignancies. It is highly prevalent (70%) in PDA and is nonexistent in normal pancreatic tissues. Retrospective studies on PDA tumor tissue (detected by immunohistochemistry or IHC)) have investigated the prognostic value of MUC5AC expression but were equivocal. Some studies associated it with poor outcomes (survival or pathological features such as lymph node disease, vascular/neural invasion in resected tumors), while others have concluded that it is a good prognostic marker. The examination of expression level threshold (5%, 10%, or 25%) and the detected region (apical vs. cytoplasmic) were variable among the studies. The maturation stage and glycoform of MUC5AC detected also differed with the Monoclonal antibody (Mab) employed for IHC. CLH2 detects less mature/less glycosylated versions while 45M1 or 21-1 detect mature/more glycosylated forms. Interestingly, aberrantly glycosylated variants of MUC5AC were detected using lectin assays (Wheat Germ Agglutinin-MUC5AC), and Mabs such as NPC-1C and PAM4 have are more specific to malignant pancreatic tissues. NPC-1C and PAM4 antibody reactive epitopes on MUC5AC are immunogenic and could represent specific changes on the native MUC5AC glycoprotein linked to carcinogenesis. It was never studied to predict treatment response.
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