Treatment with decitabine induces the expression of stemness markers, PD-L1 and NY-ESO-1 in colorectal cancer: potential for combined chemoimmunotherapy

Nassiba Taib; Maysaloun Merhi; Varghese Inchakalody; Sarra Mestiri; Shereena Hydrose; Karama Makni-Maalej; Afsheen Raza; Fairooz Sahir; Fouad Azizi; Parveen B Nizamuddin; Queenie Fernandes; Zeenath Safira K M Yoosuf; Salam Almoghrabi; Lobna Al-Zaidan; Alaaeldin Shablak; Shahab Uddin; Cristina Maccalli; Mohammed Ussama Al Homsi; Said Dermime

doi:10.1186/s12967-023-04073-y

Treatment with decitabine induces the expression of stemness markers, PD-L1 and NY-ESO-1 in colorectal cancer: potential for combined chemoimmunotherapy

J Transl Med. 2023 Mar 31;21(1):235. doi: 10.1186/s12967-023-04073-y.

Authors

Nassiba Taib^{1

2}, Maysaloun Merhi^{1

2}, Varghese Inchakalody^{1

2}, Sarra Mestiri^{1

2}, Shereena Hydrose^{1

2}, Karama Makni-Maalej^{1

2}, Afsheen Raza^{1

2}, Fairooz Sahir^{1

2}, Fouad Azizi³, Parveen B Nizamuddin³, Queenie Fernandes^{1

4}, Zeenath Safira K M Yoosuf^{1

5}, Salam Almoghrabi^{1

2}, Lobna Al-Zaidan^{1

2}, Alaaeldin Shablak², Shahab Uddin^{6

7}, Cristina Maccalli⁸, Mohammed Ussama Al Homsi², Said Dermime^{9

10

11}

Affiliations

¹ Translational Cancer Research Facility, National Center for Cancer Care and Research/Translational Research Institute, Hamad Medical Corporation, 2030, Doha, Qatar.
² National Center for Cancer Care and Research, Hamad Medical Corporation, 2030, Doha, Qatar.
³ Translational Research Institute, Academic Health System, Hamad Medical Corporation, 2030, Doha, Qatar.
⁴ College of Medicine, Qatar University, 2713, Doha, Qatar.
⁵ College of Health and Life Sciences, Hamad Bin Khalifa University, 34110, Doha, Qatar.
⁶ Translational Research Institute and Dermatology Institute, Academic Health System, Hamad Medical Corporation, 2030, Doha, Qatar.
⁷ Laboratory Animal Research Center, Qatar University, 2713, Doha, Qatar.
⁸ Laboratory of Immune and Biological Therapy, Human Immunology Department, Research Branch, Sidra Medicine, 26999, Doha, Qatar.
⁹ Translational Cancer Research Facility, National Center for Cancer Care and Research/Translational Research Institute, Hamad Medical Corporation, 2030, Doha, Qatar. sdermime@hamad.qa.
¹⁰ National Center for Cancer Care and Research, Hamad Medical Corporation, 2030, Doha, Qatar. sdermime@hamad.qa.
¹¹ College of Health and Life Sciences, Hamad Bin Khalifa University, 34110, Doha, Qatar. sdermime@hamad.qa.

Abstract

Background: The mechanism of tumor immune escape and progression in colorectal cancer (CRC) is widely investigated in-vitro to help understand and identify agents that might play a crucial role in response to treatment and improve the overall survival of CRC patients. Several mechanisms of immune escape and tumor progression, including expression of stemness markers, inactivation of immunoregulatory genes by methylation, and epigenetic silencing, have been reported in CRC, indicating the potential of demethylating agents as anti-cancer drugs. Of these, a chemotherapeutic demethylating agent, Decitabine (DAC), has been reported to induce a dual effect on both DNA demethylation and histone changes leading to an increased expression of target biomarkers, thus making it an attractive anti-tumorigenic drug.

Methods: We compared the effect of DAC in primary 1076 Col and metastatic 1872 Col cell lines isolated and generated from patients' tumor tissues. Both cell lines were treated with DAC, and the expression of the NY-ESO-1 cancer-testis antigen, the PD-L1 immunoinhibitory marker, and the CD44, Nanog, KLF-4, CD133, MSI-1 stemness markers were analyzed using different molecular and immunological assays.

Results: DAC treatment significantly upregulated stemness markers in both primary 1076 Col and meta-static 1872 Col cell lines, although a lower effect occurred on the latter: CD44 (7.85 fold; ***p = 0.0001 vs. (4.19 fold; *p = 0.0120), Nanog (4.1 fold; ***p < 0.0001 vs.1.69 fold; ***p = 0.0008), KLF-4 (4.33 fold; ***p < 0.0001 vs.2.48 fold; ***p = 0.0005), CD133 (16.77 fold; ***p = 0.0003 vs.6.36 fold; *p = 0.0166), and MSI-1 (2.33 fold; ***p = 0.0003 vs.2.3 fold; ***p = 0.0004), respectively. Interestingly, in the metastatic 1872 Col cells treated with DAC, the expression of both PD-L1 and NY-ESO-1 was increased tenfold (*p = 0.0128) and fivefold (***p < 0.0001), respectively.

Conclusions: We conclude that the upregulation of both stemness and immune checkpoint markers by DAC treatment on CRC cells might represent a mechanism of immune evasion. In addition, induction of NY-ESO-1 may represent an immuno-therapeutic option in metastatic CRC patients. Finally, the combination of DAC and anti-PD-1/anti-PD-L1 antibodies treatment should represent a potential therapeutic intervention for this group of patients.

Keywords: Chemoresistance; Colorectal cancer; Decitabine; Immune escape; NY-ESO-1; PD-L1; Stemness markers.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antigens, Neoplasm* / metabolism
Cell Line, Tumor
Colorectal Neoplasms* / drug therapy
Colorectal Neoplasms* / genetics
Decitabine / pharmacology
Decitabine / therapeutic use
Humans
Immunotherapy
Male
Membrane Proteins / genetics
Membrane Proteins / metabolism

Substances

Decitabine
Antigens, Neoplasm
Membrane Proteins