Journal article
The Penetratin Sequence in the Anticancer PNC-28 Peptide Causes Tumor Cell Necrosis Rather Than Apoptosis of Human Pancreatic Cancer Cells
Annals of surgical oncology, v 15(12), pp 3588-3600
01 Dec 2008
PMID: 18931881
Featured in Collection : UN Sustainable Development Goals @ Drexel
Abstract
Background: PNC-27 and PNC-28 are p53-derived peptides from the human double minute (hdm-2) binding domain attached to penetratin. These peptides induce tumor cell necrosis of cancer cells, but not normal cells. The anticancer activity and mechanism of PNC-28 (p53 aa17-26-penetratin) was specifically studied against human pancreatic cancer.
Methods: MiaPaCa-2 cells were treated with PNC-28. Necrosis was determined by measuring lactate dehydrogenase (LDH) and apoptosis as assayed for measuring elevation of proapoptotic proteins. PNC-29, an unrelated peptide, and hdm-2-binding domain p53 aa12-26 without penetratin (PNC-26) were used as controls. Since there is evidence that penetratin is required for tumor cell necrosis, we tested "naked'' p53 peptide without penetratin by transfecting a plasmid that encodes p53 aa17-26 segment of PNC-28 into MiaPaCa-2 and an untransformed rat pancreatic acinar cell line, BMRPA1. Time-lapse electron microscopy was employed to further elucidate anticancer mechanism.
Results: Treatment with PNC-28 does not result in the elevation of proapoptotic proteins found in p53-induced apoptosis, but elicits rapid release of LDH, indicative of tumor cell necrosis. Accordingly, we observed membrane pore formation and dose-dependent killing. In direct contrast, transfected MiaPaCa-2 cells underwent apoptosis, and not necrosis, as evidenced by expression of high levels of caspases-3 and 7 and annexin V with background levels of LDH.
Conclusion: These results suggest that PNC-28 may be effective in treating human pancreatic cancer. The penetratin sequence appears to be responsible for the fundamental change in the mechanism of action, inducing rapid necrosis initiated by membrane pore formation. Cancer cell death by apoptosis was observed in the absence of penetratin.
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Details
- Title
- The Penetratin Sequence in the Anticancer PNC-28 Peptide Causes Tumor Cell Necrosis Rather Than Apoptosis of Human Pancreatic Cancer Cells
- Creators
- Wilbur B. Bowne - SUNY Downstate Health Sciences UniversityKelley A. Sookraj - SUNY Downstate Health Sciences UniversityMichael Vishnevetsky - SUNY Downstate Health Sciences UniversityVictor Adler - College Station Medical CenterEhsan Sarafraz-Yazdi - SUNY Downstate Health Sciences UniversitySunming Lou - SUNY Downstate Health Sciences UniversityJesco Koenke - Columbia UniversityVadim Shteyler - SUNY Downstate Health Sciences UniversityKamran Ikram - VA NY Harbor Healthcare SystemMichael Harding - College Station Medical CenterMartin H. Bluth - Wayne State UniversityMou Ng - SUNY Downstate Health Sciences UniversityPaul W. Brandt-Rauf - Columbia UniversityRaqibul Hannan - SUNY Downstate Health Sciences UniversityStephan Bradu - SUNY Downstate Health Sciences UniversityMichael E. Zenilman - SUNY Downstate Health Sciences UniversityJosef Michl - SUNY Downstate Health Sciences UniversityMatthew R. Pincus - United States Department of Veterans Affairs
- Publication Details
- Annals of surgical oncology, v 15(12), pp 3588-3600
- Publisher
- Springer Nature
- Number of pages
- 13
- Grant note
- R01CA042500 / NATIONAL CANCER INSTITUTE; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Cancer Institute (NCI) CA42500 / NCI NIH HHS; United States Department of Health & Human Services; National Institutes of Health (NIH) - USA; NIH National Cancer Institute (NCI)
- Resource Type
- Journal article
- Language
- English
- Academic Unit
- School of Biomedical Engineering, Science, and Health Systems; Drexel University
- Web of Science ID
- WOS:000261617400033
- Scopus ID
- 2-s2.0-58149293618
- Other Identifier
- 991019323773104721
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- Collaboration types
- Domestic collaboration
- Web of Science research areas
- Oncology
- Surgery