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![Immunotherapy the Present and Future of
Cancer Treatment
Soto Vega E*
Medicine School, Anahuac University Puebla, México
Introduction
During many years’ cancer treatments was restricted to surgery, chemotherapy or
radiotherapy. The advances in cancer knowledge have revealed an interaction between
malignant cells, their microenvironment and the immune system, which is crucial during
oncogenesis and cancer progression; consequently, immunotherapy was developed, and it
seems to work when other treatments do not. The main problem of immunotherapy is the
tumor immunosuppressive microenvironment which is a dynamic status and is coordinated
by multiple immunosuppressive signals. Personalized medicine is essential during
immunotherapy to ensure the success of the treatment, it is necessary to consider tumor
biomarkers, microenvironment, patient genetics, immune profile, and the general patient
status [1]. Anticancer immunotherapies are classified as “passive” or “active” based on their
ability to activate the host immune system against malignant cells.
Passive Immunotherapy
Tumor-targeting monoclonal antibodies
The tumor targeting monoclonal antibodies (mAb) can act by the following three ways:
a) Altering the signaling of receptors expressed on malignant cells,
b) Neutralizing trophic signals produced by malignant cells or by stromal components
of neoplastic lesions,
c) 3) Recognizing selectively tumor associated antigen and then activate antibody-
dependent cellular cytotoxicity or complement dependent cytotoxicity, o well interfering with
pathways of tumorigenesis (triggering apoptosis, inhibiting cells proliferation or blocking
angiogenesis).
Clinical trials are being carried out to assess the safety or efficacy of tumor-targeting
mAbs, engineered humanized or chimeric mAbs have been recently approved by the FDA. The
mAbs are also being used combined with radioisotopes to attack selectively cancer cells [2,3].
Adoptive T cell transfer
The objective of the adoptive T cell transfer is to generate a vigorous immune mediated
antitumor response, T cells are harvested from blood or tumor and manipulated ex vivo for
its expansion and then re-infused into the patient, where they will mediate tumor destruction.
The mechanism can be divided in two:
Crimson Publishers
Wings to the Research
Opinion
*Corresponding author: Soto Vega E,
Medicine School, Puebla, México
Submission: March 28, 2019
Published: April 02, 2019
Volume 2 - Issue 3
How to cite this article: Soto Vega E.
Immunotherapy the Present and Future
of Cancer Treatment. Nov Appro in Can
Study. 2(3). NACS.000539.2019.
DOI: 10.31031/NACS.2019.02.000539
Copyright@ Soto Vega E, This article is
distributed under the terms of the Creative
Commons Attribution 4.0 International
License, which permits unrestricted use
and redistribution provided that the
original author and source are credited.
ISSN: 2637-773X
192Novel Approaches in Cancer Study
Abstract
Immunotherapy is based in reactivating the patient immune system specifically against the neoplasia,
tumors have immunosuppression mechanisms that allow them to control and evade the immune
response.
There are different immunotherapy approaches like tumor-targeting monoclonal antibodies, adoptive
T cell transfer, anticancer vaccines, checkpoint inhibitors, most of these in important clinical trials in
which the effects and toxicities are still evaluated. They are also beginning tested on a combination of
immunotherapies and other non-immunological therapies in order to increase the survival of patients.
Immunotherapy is still a young area and it needs to reach its peak, but it will surely be a great tool to treat
and cure cancer.](https://image.slidesharecdn.com/nacs-200925134312/75/Immunotherapy-the-Present-and-Future-of-Cancer-Treatment-1-2048.jpg)
![193
Nov Appro in Can Study Copyright © : Soto Vega E
NACS.000539. 2(3).2019
A. The isolation of tumor infiltrating lymphocytes; T
cells and Natural killer are present in any solid tumor, but in an
immunosuppressive tumor microenvironment, ex vivo T cell
stimulation with cytokines enhance their efficacy. This therapy is
actually used in melanoma patients.
B. The genetic modification of blood-derived T cells to allow
for specific recognition of tumor cells. There are two common
approaches for redirecting T cell specificity:
a) Gene modification with TCRs directed against tumor
associated antigens. Some clinical studies have been conducted
with modified TCR with limited efficacy and significant toxicity due
to the destruction of self-antigens and
b) T cell receptor modified through the expression of a
chimeric antigen receptor, CAR-T cell. The CAR-T cell has been used
successfully in hematological malignancies targeting specific cell
antigens; in solid tumors, the problem is the lack of specific tumor
antigen [4,5].
Active Immunotherapy
Anticancer vaccines
There are two types of anti-cancer vaccines, the first one
prophylactic anti-cancer vaccines that are developed to those
chronic infections that are involved in carcinogenesis. On the
other hand, non-prophylactic anti-cancer vaccines elaborated with
tumor antigens to elicit an immune response versus cancer, the
main obstacle is the identification of appropriate tumor antigen.
The first anti-cancer vaccine approved by the FDA was for prostate
cancer, it was done with autologous peripheral blood mononuclear
cells and incubated with a fusion protein of a tumor antigen
associated protein, and the objective is that dendritic cells present
the antigen as part of the major histocompatibility complex. The
most important prophylactic anti-cancer vaccine is the human
papillomavirus which causes cervical cancer [6].
Checkpoint inhibitors
Malignant cells promote an immunosuppressive
microenvironment with suppressive signal transduction; immune
checkpoints are responsible for the tolerance and immune
activation. Cancer uses those checkpoints for its own benefit,
inducing tolerance and evasion. The main checkpoints for cancer
treatments by now are PD-1/PD-1L (Programmed death-1/-
Ligand), CTLA-4 (cytotoxic T lymphocyte-associated antigen 4),
LAG-3 (lymphocyte activation gene 3), among others [7].
Conclusion
The immune system is very powerful against cancer, but
it controls the immunity by producing an immunosuppressive
microenvironment.Theobjectiveofimmunotherapyistore-activate
the patient immune system instead of attack cancer like other
therapies used. Immunotherapy is the area of medical sciences that
has advanced more in the last years but has not reached its peak,
it seems that there is finally a way to effectively treat or even cure
cancer, in the following years immunotherapy will complete change
and everything seems to indicate that it would be used combined
with other therapies to improve patient survival, but the studies are
just starting, and antitumor effects and toxicities have yet to be fully
explored.
References
1. Yu Y, Cui J (2017) Present and future of cancer immunotherapy: A tumor
microenviromental perspective. Oncology Letters 16(4): 4105-4113.
2. Candéias SM, Gaipl US (2016) The Immune system in cancer prevention,
development and therapy. Anti-Cancer Agents in Medicinal Chemistry
16(1): 101-107.
3. Vacchelli E, Pol J, Bloy N, Eggermont A, Cremer I, et al. (2015) Trial watch:
Tumor-targeting monoclonal antibodies for oncological indications.
Oncoimmunology 4(1): e985940.
4. Met O, Melgaard Jensen K, Aled Chamberlain C, Donia M, Svane IM (2018)
Principles of adoptive T cell therapy in cancer. Semin Immunopathol
41(1): 49-58.
5. Yee C (2018) Adoptive T cell therapy: Points to consider. Curr Opin
Immunol 51: 197-203.
6. Liberal JM, Ochoa de Olza M, Hierro C, Gros A, Rodon J, et al. (2017) The
expanding role of immunotherapy. Cancer treat Rev 54: 74-86.
7. Denis H, Davoine C, Bermudez E, Grosjean G, Schwager M, et al. (2019)
Les immunotherapies spécifiques dans le traitement des cancer. Bull
Cancer 106: 37-47.
For possible submissions Click below:
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Uploaded byCrimsonpublishersCancer
Immunotherapy the Present and Future of Cancer Treatment
Immunotherapy is an innovative approach to cancer treatment that reactivates the immune system against tumors, which often create immunosuppressive environments. Various strategies such as monoclonal antibodies, adoptive T cell transfer, anticancer vaccines, and checkpoint inhibitors are currently being explored, with ongoing clinical trials assessing their efficacy and safety. This field is rapidly evolving, and while it shows promise for significantly improving cancer treatment outcomes, the potential for combination therapies and further research is essential for maximizing patient survival.
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Immunotherapy the Present and Future of Cancer Treatment
- 1. Immunotherapy the Presentand Future of Cancer Treatment Soto Vega E* Medicine School, Anahuac University Puebla, México Introduction During many years’ cancer treatments was restricted to surgery, chemotherapy or radiotherapy. The advances in cancer knowledge have revealed an interaction between malignant cells, their microenvironment and the immune system, which is crucial during oncogenesis and cancer progression; consequently, immunotherapy was developed, and it seems to work when other treatments do not. The main problem of immunotherapy is the tumor immunosuppressive microenvironment which is a dynamic status and is coordinated by multiple immunosuppressive signals. Personalized medicine is essential during immunotherapy to ensure the success of the treatment, it is necessary to consider tumor biomarkers, microenvironment, patient genetics, immune profile, and the general patient status [1]. Anticancer immunotherapies are classified as “passive” or “active” based on their ability to activate the host immune system against malignant cells. Passive Immunotherapy Tumor-targeting monoclonal antibodies The tumor targeting monoclonal antibodies (mAb) can act by the following three ways: a) Altering the signaling of receptors expressed on malignant cells, b) Neutralizing trophic signals produced by malignant cells or by stromal components of neoplastic lesions, c) 3) Recognizing selectively tumor associated antigen and then activate antibody- dependent cellular cytotoxicity or complement dependent cytotoxicity, o well interfering with pathways of tumorigenesis (triggering apoptosis, inhibiting cells proliferation or blocking angiogenesis). Clinical trials are being carried out to assess the safety or efficacy of tumor-targeting mAbs, engineered humanized or chimeric mAbs have been recently approved by the FDA. The mAbs are also being used combined with radioisotopes to attack selectively cancer cells [2,3]. Adoptive T cell transfer The objective of the adoptive T cell transfer is to generate a vigorous immune mediated antitumor response, T cells are harvested from blood or tumor and manipulated ex vivo for its expansion and then re-infused into the patient, where they will mediate tumor destruction. The mechanism can be divided in two: Crimson Publishers Wings to the Research Opinion *Corresponding author: Soto Vega E, Medicine School, Puebla, México Submission: March 28, 2019 Published: April 02, 2019 Volume 2 - Issue 3 How to cite this article: Soto Vega E. Immunotherapy the Present and Future of Cancer Treatment. Nov Appro in Can Study. 2(3). NACS.000539.2019. DOI: 10.31031/NACS.2019.02.000539 Copyright@ Soto Vega E, This article is distributed under the terms of the Creative Commons Attribution 4.0 International License, which permits unrestricted use and redistribution provided that the original author and source are credited. ISSN: 2637-773X 192Novel Approaches in Cancer Study Abstract Immunotherapy is based in reactivating the patient immune system specifically against the neoplasia, tumors have immunosuppression mechanisms that allow them to control and evade the immune response. There are different immunotherapy approaches like tumor-targeting monoclonal antibodies, adoptive T cell transfer, anticancer vaccines, checkpoint inhibitors, most of these in important clinical trials in which the effects and toxicities are still evaluated. They are also beginning tested on a combination of immunotherapies and other non-immunological therapies in order to increase the survival of patients. Immunotherapy is still a young area and it needs to reach its peak, but it will surely be a great tool to treat and cure cancer.
- 2. 193 Nov Appro inCan Study Copyright © : Soto Vega E NACS.000539. 2(3).2019 A. The isolation of tumor infiltrating lymphocytes; T cells and Natural killer are present in any solid tumor, but in an immunosuppressive tumor microenvironment, ex vivo T cell stimulation with cytokines enhance their efficacy. This therapy is actually used in melanoma patients. B. The genetic modification of blood-derived T cells to allow for specific recognition of tumor cells. There are two common approaches for redirecting T cell specificity: a) Gene modification with TCRs directed against tumor associated antigens. Some clinical studies have been conducted with modified TCR with limited efficacy and significant toxicity due to the destruction of self-antigens and b) T cell receptor modified through the expression of a chimeric antigen receptor, CAR-T cell. The CAR-T cell has been used successfully in hematological malignancies targeting specific cell antigens; in solid tumors, the problem is the lack of specific tumor antigen [4,5]. Active Immunotherapy Anticancer vaccines There are two types of anti-cancer vaccines, the first one prophylactic anti-cancer vaccines that are developed to those chronic infections that are involved in carcinogenesis. On the other hand, non-prophylactic anti-cancer vaccines elaborated with tumor antigens to elicit an immune response versus cancer, the main obstacle is the identification of appropriate tumor antigen. The first anti-cancer vaccine approved by the FDA was for prostate cancer, it was done with autologous peripheral blood mononuclear cells and incubated with a fusion protein of a tumor antigen associated protein, and the objective is that dendritic cells present the antigen as part of the major histocompatibility complex. The most important prophylactic anti-cancer vaccine is the human papillomavirus which causes cervical cancer [6]. Checkpoint inhibitors Malignant cells promote an immunosuppressive microenvironment with suppressive signal transduction; immune checkpoints are responsible for the tolerance and immune activation. Cancer uses those checkpoints for its own benefit, inducing tolerance and evasion. The main checkpoints for cancer treatments by now are PD-1/PD-1L (Programmed death-1/- Ligand), CTLA-4 (cytotoxic T lymphocyte-associated antigen 4), LAG-3 (lymphocyte activation gene 3), among others [7]. Conclusion The immune system is very powerful against cancer, but it controls the immunity by producing an immunosuppressive microenvironment.Theobjectiveofimmunotherapyistore-activate the patient immune system instead of attack cancer like other therapies used. Immunotherapy is the area of medical sciences that has advanced more in the last years but has not reached its peak, it seems that there is finally a way to effectively treat or even cure cancer, in the following years immunotherapy will complete change and everything seems to indicate that it would be used combined with other therapies to improve patient survival, but the studies are just starting, and antitumor effects and toxicities have yet to be fully explored. References 1. Yu Y, Cui J (2017) Present and future of cancer immunotherapy: A tumor microenviromental perspective. Oncology Letters 16(4): 4105-4113. 2. Candéias SM, Gaipl US (2016) The Immune system in cancer prevention, development and therapy. Anti-Cancer Agents in Medicinal Chemistry 16(1): 101-107. 3. Vacchelli E, Pol J, Bloy N, Eggermont A, Cremer I, et al. (2015) Trial watch: Tumor-targeting monoclonal antibodies for oncological indications. Oncoimmunology 4(1): e985940. 4. Met O, Melgaard Jensen K, Aled Chamberlain C, Donia M, Svane IM (2018) Principles of adoptive T cell therapy in cancer. Semin Immunopathol 41(1): 49-58. 5. Yee C (2018) Adoptive T cell therapy: Points to consider. Curr Opin Immunol 51: 197-203. 6. Liberal JM, Ochoa de Olza M, Hierro C, Gros A, Rodon J, et al. (2017) The expanding role of immunotherapy. Cancer treat Rev 54: 74-86. 7. Denis H, Davoine C, Bermudez E, Grosjean G, Schwager M, et al. (2019) Les immunotherapies spécifiques dans le traitement des cancer. Bull Cancer 106: 37-47. For possible submissions Click below: Submit Article