Current Insights into Combination Therapies with MAPK Inhibitors and Immune Checkpoint Blockade

Shin, Min Hwa; Kim, Jiyoung; Lim, Siyoung A.; Kim, Jeongsoo; Lee, Kyung Mi

doi:10.3390/ijms21072531

Cited by 61 publications

(45 citation statements)

References 79 publications

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“…ICIs resistance is divided into primary or adaptive resistance and acquired resistance. 79 The mechanisms of primary or adaptive resistance including (a) Alteration of signaling pathways: MAPK, PI3K, WNT/β-catenin, and IFN, which suppressed the process of tumor antigen expression, tumor antigen presentation, and T cell infiltration; [80][81][82][83] (b) Lack of antigenic mutations; 84 (c) loss of tumor antigen expression; (d) loss of HLA expression; 85 (e) up-regulation of constitutive PD-L1 expression. 86 The mechanisms of acquired resistance including (a) loss of target antigen; 87 (b) loss of T cell function; 87 (c) inhibitory immune checkpoints in T cells (eg, VISTA, LAG-3, TIM-3); 88,89 (d) T cell exhaustion; 90 (e) immunosuppressive cells (eg, TAMs, Tregs and MDSCs); 91,92 (d) intestinal dysbacteriosis; 93 (f) release of cytokines and metabolites in tumor microenvironment (eg, TGF-β, CSF-1, and adenylate).…”

Section: Clinical Study Of Combined Icis Therapy and Chemotherapy In mentioning

confidence: 99%

<p>Combination of Immune Checkpoint Inhibitors with Chemotherapy in Lung Cancer</p>

Liu¹,

Zhang²,

Xiu³

et al. 2020

OTT

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Tremendous progress has been achieved in the field of immune checkpoint inhibitors (ICIs) therapy in lung cancer in recent years. To generate robust, long-lasting anti-tumor immune responses in lung cancer patients, combinational ICI therapies have been explored deeply. Conventionally, chemotherapy was considered as immunosuppressive. It is now recognized that chemotherapy could also reinstate cancer cell immune-surveillance and enable the perception of cancer cells as dangerous. That is to say that chemotherapeutic drugs are not only a source of direct cytotoxic effects but also an adjuvant for anti-tumor immunity. Recently, multiple clinical studies of ICIs combined with chemotherapeutic drugs have been explored and proved effective. However, there are still crucial questions that are not well addressed, such as the optimal dose and schedule for a given combination may differ across disease indications, and the appropriate strategy of selecting patient population that can benefit from ICIs remains unclear. To facilitate more rational lung cancer ICIs therapy development, this review summarizes the immune-regulatory effects and related mechanisms of chemotherapeutic drugs and the clinical progress of ICIs and their combination with chemotherapies in lung cancer treatment.

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Section: Clinical Study Of Combined Icis Therapy and Chemotherapy In mentioning

confidence: 99%

<p>Combination of Immune Checkpoint Inhibitors with Chemotherapy in Lung Cancer</p>

Liu¹,

Zhang²,

Xiu³

et al. 2020

OTT

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“…35 One practicable way to overcome acquired drug-resistance, which is remarkably high in patients treated with ipilimumab monotherapy, is the combination of different drug and the combination with radiotherapy. 36 INCMGA00012 is a humanized IG4k monoclonal antibody against human PD-1, that has shown activity in solid tumors with an acceptable safety profile, is currently under investigation for metastatic MCC in a phase II trial (ClinicalTrials.gov Identifier: NCT03599713). [38][39][40] T A B L E 1 Recent trials on drug therapy of advanced or metastatic MCC…”

Section: Drug-resistance To Checkpoint Inhibitorsmentioning

confidence: 99%

Advanced Merkel cell carcinoma—A focus on medical drug therapy

Wollina

Koch

Cardoso

2020

Dermatologic Therapy

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Merkel cell carcinoma (MCC) is a rare but aggressive non‐melanoma skin cancer with significant morbidity and mortality. Treatment of choice for primary and locoregional MCC is complete surgical removal with sentinel lymphonodectomy and postsurgical radiotherapy of tumor basin and locoregional lymph nodes. In nonresectable and advanced tumors, drug therapy is indicated. While cytotoxic chemotherapy has resulted in higher response rates, overall survival remained nearly unaffected. With a better insight into tumor development and biology, new treatment s became available. Immune checkpoint inhibitors result in durable responses with a better safety profile that classical combined chemotherapy. Combinations of immune checkpoint inhibitors with and without radiotherapy help to overcome acquired drug‐resistance. New compounds for vaccination and oral use are on the horizon. Despite all progress, treatment of MCC remains a challenge that needs close interdisciplinary teamwork.

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“…Moreover, MAPK may also control inflammatory cytokine production and cellular apoptosis upon viral infection, integrating signals from complex intracellular networks in performing cellular functions, thus being a rather obvious target to fight against viral infection. Due to the initial discovery of the core elements of the MAPK pathways nearly four decades ago, considerable effort has been focused on development of MAPK inhibitors which have shown promising clinical responses in cancer patients, both as single inhibitors or in combination [7]. The pandemic crisis imposes to think about high-throughput molecular approaches to moving from operational to scientifically-driven pharmacovigilance.…”

Section: Mapk Activation In Severe Covid-19 Diseasementioning

confidence: 99%

“…Members of the Ras family of proteins, including K-Ras, H-Ras, and N-Ras, play a key role in transmission of extracellular signals into thecells [4]. Since decades, intense work is under way to develop and evaluate compounds that target components of MAPK pathways, for the treatment of inflammatory and neurodegenerative diseases, and of cancer [5], [6], [7]. CQ (N4-(7-Chloro-4-quinolinyl)-N1,N1-diethyl-1,4-pentanediamine) has long been used to treat malaria and amebiasis.…”

Section: Introductionmentioning

confidence: 99%

Molecular Insights on Potential Combination of Mapk Inhibitors Together with HCQ and HCQs Analogs in Viral Infection

Mohanta¹,

Sharma²,

Arina³

et al. 2020

Preprint

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The outbreak of coronavirus disease-19 (COVID-19) has infected more than 11 million people and has claimed more than 530.000 deaths world-wide. In July 2020, still, there is no specific treatment for disease caused by the novel coronavirus. In the search to curb the global pandemic COVID-19, some eastern and developing countries have approved various treatment with controversial efficacy, among that the use of the antimalarial Hydroxychloroquine (HCQ), so far with inconclusive clinical evidence of effectiveness. On the other hand, computer-based screening suggest that HCQs analog are promising molecules, to impair viral replication in vitro[1]. Therefore, what is emerging from this complex background, is the need to understand molecular mechanism beyond drugs that can be helpful against viral infection for this and future pandemic. The intent of this Brief Report is to highlight: i) the involvement of the Mitogen Activated Protein Kinase (MAPK) cascade in viral infection and ii) the urgent need to have molecular data on the effectiveness of the combination of MAPK inhibitors together with HCQ and HCQs analogs in curbing viral infection. We are convinced that a better understanding of the patterns of elicited molecular mechanisms will be critical for new molecular approaches to this severe disease

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Current Insights into Combination Therapies with MAPK Inhibitors and Immune Checkpoint Blockade

Cited by 61 publications

References 79 publications

<p>Combination of Immune Checkpoint Inhibitors with Chemotherapy in Lung Cancer</p>

<p>Combination of Immune Checkpoint Inhibitors with Chemotherapy in Lung Cancer</p>

Advanced Merkel cell carcinoma—A focus on medical drug therapy

Molecular Insights on Potential Combination of Mapk Inhibitors Together with HCQ and HCQs Analogs in Viral Infection

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