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Tumor immune escape πŸ”Ž

➑️ P2X7R is expressed in most solid and haematological cancer.

πŸ“Œ P2X7R:
1. Promotes proliferation.
2. Promotes metabolism.
3. Facilitates tumor invasion and metastatic dissemination.

πŸ“ P2X7R showed different roles of anti-tumor response in various preclinical studies.

πŸ₯ˆTwo oposite role of P2X7R:

1. Genetic deletion of P2X7R shown adverse effect on tumor infiltrating T cells and promotes tumor growth.

2. Systemic P2X7R antagonism in same tomor model shown positive effect and reduce tumor burden.

πŸ’₯ Mechanism of P2X7R in detail:

1⃣. Sustained exposure of high concentrations of extracellular ATP, produced in the tumor microenvironment (TME), is recognized by the P2X7R on tumor infiltrating lymphocytes cause the ATP-induced cell death (AICD) and also Expression of ART1 by tumor cells can utilize extracellular NAD+ in TME on tumor-infiltrating lymphocytes (TILs) in trans resulting in NAD-induced cell death (NICD).

2⃣. Modified P2X7R is Expressed by tumor cells with low affinity for AICD and NICD allows them to avoid cell death while still exploiting P2X7R-mediated proliferation and growth signalling.

3⃣. CD38 and CD39 mediated catabolism of extracellular NAD and ATP into ADPR and ADP/AMP respectively,

4⃣. CD73 convert ADPR and ADP/AMP into adenosine. CD73 is frequently overexpressed by tumor cells, resulting in polarization of intratumoural immune cells towards a regulatory phenotype (including Tregs and macrophages) as well as reduced proliferation, cytokine production and cytotoxic function of effector lymphocytes.

πŸ“„ Reference: https://doi.org/10.3389%2Ffimmu.2023.1287310

πŸ†” Follow us:
@Oncologylearn
@ResearchGroup1401
Frontiers
Frontiers | Tumour immune escape via P2X7 receptor signalling
While P2X7 receptor expression on tumour cells has been characterized as a promotor of cancer growth and metastasis, its expression by the host immune system...
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Tumor immune escape πŸ”Ž

➑️ P2X7R is expressed in most solid and haematological cancer.

πŸ“Œ P2X7R:
1. Promotes proliferation.
2. Promotes metabolism.
3. Facilitates tumor invasion and metastatic dissemination.

πŸ“ P2X7R showed different roles of anti-tumor response in various preclinical studies.

πŸ₯ˆTwo oposite role of P2X7R:

1. Genetic deletion of P2X7R shown adverse effect on tumor infiltrating T cells and promotes tumor growth.

2. Systemic P2X7R antagonism in same tomor model shown positive effect and reduce tumor burden.

πŸ’₯ Mechanism of P2X7R in detail:

1⃣. Sustained exposure of high concentrations of extracellular ATP, produced in the tumor microenvironment (TME), is recognized by the P2X7R on tumor infiltrating lymphocytes cause the ATP-induced cell death (AICD) and also Expression of ART1 by tumor cells can utilize extracellular NAD+ in TME on tumor-infiltrating lymphocytes (TILs) in trans resulting in NAD-induced cell death (NICD).

2⃣. Modified P2X7R is Expressed by tumor cells with low affinity for AICD and NICD allows them to avoid cell death while still exploiting P2X7R-mediated proliferation and growth signalling.

3⃣. CD38 and CD39 mediated catabolism of extracellular NAD and ATP into ADPR and ADP/AMP respectively,

4⃣. CD73 convert ADPR and ADP/AMP into adenosine. CD73 is frequently overexpressed by tumor cells, resulting in polarization of intratumoural immune cells towards a regulatory phenotype (including Tregs and macrophages) as well as reduced proliferation, cytokine production and cytotoxic function of effector lymphocytes.

πŸ“„ Reference: https://doi.org/10.3389%2Ffimmu.2023.1287310

πŸ†” Follow us:
@Oncologylearn
@ResearchGroup1401

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