Cancers (Mar 2022)

Conversion of a Non-Cancer-Selective Promoter into a Cancer-Selective Promoter

  • Praveen Bhoopathi,
  • Anjan K. Pradhan,
  • Amit Kumar,
  • Santanu Maji,
  • Padmanabhan Mannangatti,
  • Xiaoyan Deng,
  • Dipankar Bandyopadhyay,
  • Devanand Sarkar,
  • Xiang-Yang Wang,
  • Joseph W. Landry,
  • Swadesh K. Das,
  • Luni Emdad,
  • Paul B. Fisher

DOI
https://doi.org/10.3390/cancers14061497
Journal volume & issue
Vol. 14, no. 6
p. 1497

Abstract

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Progression-elevated gene-3 (PEG-3) and rat growth arrest and DNA damage-inducible gene-34 (GADD34) display significant sequence homology with regulation predominantly transcriptional. The rat full-length (FL) and minimal (min) PEG-3 promoter display cancer-selective expression in rodent and human tumors, allowing for cancer-directed regulation of transgenes, viral replication and in vivo imaging of tumors and metastases in animals, whereas the FL- and min-GADD34-Prom lack cancer specificity. Min-PEG-Prom and min-GADD34-Prom have identical sequences except for two single-point mutation differences (at −260 bp and +159 bp). Engineering double mutations in the min-GADD34-Prom produce the GAPE-Prom. Changing one base pair (+159) or both point mutations in the min-GADD34-Prom, but not the FL-GADD34-Prom, results in cancer-selective transgene expression in diverse cancer cells (including prostate, breast, pancreatic and neuroblastoma) vs. normal counterparts. Additionally, we identified a GATA2 transcription factor binding site, promoting cancer specificity when both min-PEG-Prom mutations are present in the GAPE-Prom. Taken together, introducing specific point mutations in a rat min-GADD34-Prom converts this non-cancer-specific promoter into a cancer-selective promoter, and the addition of GATA2 with existing AP1 and PEA3 transcription factors enhances further cancer-selective activity of the GAPE-Prom. The GAPE-Prom provides a genetic tool to specifically regulate transgene expression in cancer cells.

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