Identification of a novel putative pancreatic stem/progenitor cell marker DCAMKL-1 in normal mouse pancreas

Author:

May Randal12,Sureban Sripathi M.12,Lightfoot Stan A.32,Hoskins Aimee B.1,Brackett Daniel J.4,Postier Russell G.4,Ramanujam Rama5,Rao Chinthalapally V.16,Wyche James H.7,Anant Shrikant186,Houchen Courtney W.162

Affiliation:

1. Departments of Medicine,

2. Department of Veterans Affairs Medical Center, Oklahoma City, Oklahoma;

3. Pathology, University of Oklahoma Health Sciences Center;

4. Surgery,

5. ADNA Inc., Dublin, Ohio

6. OU Cancer Institute; and

7. Howard University, Washington, DC; and

8. Cell Biology, and

Abstract

Stem cells are critical in maintaining adult homeostasis and have been proposed to be the origin of many solid tumors, including pancreatic cancer. Here we demonstrate the expression patterns of the putative intestinal stem cell marker DCAMKL-1 in the pancreas of uninjured C57BL/6 mice compared with other pancreatic stem/progenitor cell markers. We then determined the viability of isolated pancreatic stem/progenitor cells in isotransplantation assays following DCAMKL-1 antibody-based cell sorting. Sorted cells were grown in suspension culture and injected into the flanks of athymic nude mice. Here we report that DCAMKL-1 is expressed in the main pancreatic duct epithelia and islets, but not within acinar cells. Coexpression was observed with somatostatin, NGN3, and nestin, but not glucagon or insulin. Isolated DCAMKL-1+ cells formed spheroids in suspension culture and induced nodule formation in isotransplantation assays. Analysis of nodules demonstrated markers of early pancreatic development (PDX-1), glandular epithelium (cytokeratin-14 and Ep-CAM), and isletlike structures (somatostatin and secretin). These data taken together suggest that DCAMKL-1 is a novel putative stem/progenitor marker, can be used to isolate normal pancreatic stem/progenitors, and potentially regenerates pancreatic tissues. This may represent a novel tool for regenerative medicine and a target for anti-stem cell-based therapeutics in pancreatic cancer.

Publisher

American Physiological Society

Subject

Physiology (medical),Gastroenterology,Hepatology,Physiology

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