Intermittent PI3Kδ inhibition sustains anti-tumour immunity and curbs irAEs

Eschweiler, Simon; Ramírez-Suástegui, Ciro; Li, Yingcong; King, Emma V.; Chudley, Lindsey; Thomas, Jaya; Wood, Oliver; Witzleben, Adrian von; Jeffrey, D. Lifson; McCann, Katy J.; Simon, Hayley; Mondal, Monalisa; Wang, Alice; Dicker, Martina; Lopez-Guadamillas, Elena; Chou, Ting-Fang; Dobbs, Nicola; Essame, Louisa; Acton, Gary D; Kelly, Fiona; Halbert, Gavin; Sacco, Joseph J.; Schache, Andrew; Shaw, Richard; McCaul, James; Paterson, C.; Davies, Joseph H.; Brennan, Peter A.; Singh, Rabindra Prasad; Loadman, Paul M.; Wilson, William T.; Hackshaw, Allan; Seumois, Grégory; Okkenhaug, Klaus; Thomas, Gareth J.; Jones, Terry M.; Ay, Ferhat; Friberg, Greg; Kronenberg, Mitchell; Vanhaesebroeck, Bart; Vijayanand, Pandurangan; Ottensmeier, Christian

doi:10.1038/s41586-022-04685-2

Cited by 42 publications

(28 citation statements)

References 38 publications

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“…72 The PI3K signaling pathway is also involved in regulating the immune system, so PI3Kis were found to act as immunomodulatory agents, which decreased the number of regulatory T (Treg) cells and enhanced CD8 + cytotoxic T cells in the tumor microenvironment. 73,74 In this study, we formulated mPEGylated NCs to simultaneously encapsulate DTX and PIC to achieve a synergistic anticancer effect. Anti-HER2-IV/mPEG and anti-HER2-II/mPEG BsAbs were successfully prepared to non-covalently decorate NCs via the anti-mPEG fragment, which endowed the NCs with a HER2-targeting ability and dual-HER2 blockade via the anti-HER2-IV and anti-HER2-II fragments.…”

Section: Discussionmentioning

confidence: 99%

Combined Docetaxel/Pictilisib-Loaded mPEGylated Nanocarriers with Dual HER2 Targeting Antibodies for Synergistic Chemotherapy of Breast Cancer

Cheng¹,

Lin²,

Chuang³

et al. 2022

IJN

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Introduction: Approximately 15%~30% of breast cancers have gene amplification or overexpression of the human epidermal growth factor receptor 2 (HER2), resulting in the chemotherapy resistance, a more-aggressive phenotype and poor prognosis. Methods: We propose a strategy of nanocarriers co-loaded with docetaxel (DTX) and pictilisib (PIC) at a synergistic ratio and noncovalently bound with dual anti-HER2 epitopes bispecific antibodies (BsAbs: anti-HER2-IV/methoxy-polyethylene glycol (mPEG) and anti-HER2-II/methoxy-PEG) for synergistic targeting to overcome the therapeutic dilemmas of the resistance for HER2-targetable chemodrugs. DTX/PIC-loaded nanocarriers (D/P_NCs) were prepared with single emulsion methods and characterized using dynamic light scattering analysis, and the drug content was assayed by high-performance liquid chromatographic method. The integrity and function of BsABs were evaluated using sodium dodecylsulfate polyacrylamide gel electrophoresis (SDS-PAGE) and enzyme-linked immunosorbent assay (ELISA). The in vitro cell studies and in vivo breast tumor-bearing mice model were used to evaluate the anticancer effect and biosafety of formulations. Results: D/P_NCs optimally prepared exhibited a spherical morphology with small particle sizes (~140 nm), high drug loading (~5.5%), and good colloidal stability. The synergistic tumor cytotoxicity of loading DTX and PIC at 2:1 ratio in D/P_NCs was discovered. The BsAbs are successfully decorated on mPEGylated DTX/PIC-loaded nanocarriers via anti-mPEG moiety. In vitro studies revealed that non-covalent decoration with dual BsAbs on D_P-NCs significantly and synergistically increased cellular uptake, while with loading DTX and PIC at a synergistic ratio of 2:1 in D/P_NCs further resulted in synergistic cytotoxicity. In vivo tumor inhibition studies showed the comparable results for synergistic antitumor efficacy while minimizing systemic toxicity of chemodrugs. Conclusion: Non-covalent modification with dual distinct epitopes BsAbs on the nanocarriers loaded with dual chemodrugs at a synergistic ratio was expected to be a promising therapeutic platform to overcome the chemoresistance of various cancers and warrants further development for future therapy in the clinical.

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Section: Discussionmentioning

confidence: 99%

Combined Docetaxel/Pictilisib-Loaded mPEGylated Nanocarriers with Dual HER2 Targeting Antibodies for Synergistic Chemotherapy of Breast Cancer

Cheng¹,

Lin²,

Chuang³

et al. 2022

IJN

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“…This suggests an opportunity to combine PI3K inhibition with dietary or pharmacological interventions to lower blood glucose levels. Other approaches to moderate toxicity could be through intermittent dosing, as PI3Kδ inhibition in solid tumours has been hampered by severe immune-related adverse events; however, these events could be minimized by a modified treatment regimen with PI3Kδ inhibitor intermittent dosing 286 .…”

Section: Class I Pi3ks As Therapeutic Targetsmentioning

confidence: 99%

Beyond PI3Ks: targeting phosphoinositide kinases in disease

Burke

Triscott

Emerling

et al. 2022

Nat Rev Drug Discov

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Lipid phosphoinositides are master regulators of almost all aspects of a cell's life and death and are generated by the tightly regulated activity of phosphoinositide kinases. Although extensive efforts have focused on drugging class I phosphoinositide 3-kinases (PI3Ks), recent years have revealed opportunities for targeting almost all phosphoinositide kinases in human diseases, including cancer, immunodeficiencies, viral infection and neurodegenerative disease. This has led to widespread efforts in the clinical development of potent and selective inhibitors of phosphoinositide kinases. This Review summarizes our current understanding of the molecular basis for the involvement of phosphoinositide kinases in disease and assesses the preclinical and clinical development of phosphoinositide kinase inhibitors.

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“…However, combining PI3K inhibitors with ICI has been challenging as PI3K inhibitors may alter antitumor immunity or lead to immune-related adverse events. This obstacle could be overcome by adopting a modified treatment regimen with intermittent, rather than daily, dosing of PI3K inhibitors [ 191 , 192 ]. Notably, a phase-I/II trial with copanlisib combined with nivolumab and/or ipilimumab is ongoing in patients with advanced solid cancers who have genomic alterations in PIK3CA and PTEN (NCT04317105).…”

Section: Immunotherapy For Head and Neck Cancermentioning

confidence: 99%

Novel Systemic Treatment Modalities Including Immunotherapy and Molecular Targeted Therapy for Recurrent and Metastatic Head and Neck Squamous Cell Carcinoma

Ghosh

Shah

Johnson

2022

IJMS

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Head and neck squamous cell carcinomas (HNSCCs) are the sixth most common cancers worldwide. More than half of patients with HNSCC eventually experience disease recurrence and/or metastasis, which can threaten their long-term survival. HNSCCs located in the oral cavity and larynx are usually associated with tobacco and/or alcohol use, whereas human papillomavirus (HPV) infection, particularly HPV16 infection, is increasingly recognized as a cause of oropharyngeal HNSCC. Despite clinical, histologic, and molecular differences between HPV-positive and HPV-negative HNSCCs, current treatment approaches are the same. For recurrent disease, these strategies include chemotherapy, immunotherapy with PD-1-inhibitors, or a monoclonal antibody, cetuximab, that targets epidermal growth factor; these therapies can be administered either as single agents or in combination. However, these treatment strategies carry a high risk of toxic side effects; therefore, more effective and less toxic treatments are needed. The landscape of HNSCC therapy is changing significantly; numerous clinical trials are underway to test novel therapeutic options like adaptive cellular therapy, antibody-drug conjugates, new targeted therapy agents, novel immunotherapy combinations, and therapeutic vaccines. This review helps in understanding the various developments in HNSCC therapy and sheds light on the path ahead in terms of further research in this field.

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Intermittent PI3Kδ inhibition sustains anti-tumour immunity and curbs irAEs

Cited by 42 publications

References 38 publications

Combined Docetaxel/Pictilisib-Loaded mPEGylated Nanocarriers with Dual HER2 Targeting Antibodies for Synergistic Chemotherapy of Breast Cancer

Combined Docetaxel/Pictilisib-Loaded mPEGylated Nanocarriers with Dual HER2 Targeting Antibodies for Synergistic Chemotherapy of Breast Cancer

Beyond PI3Ks: targeting phosphoinositide kinases in disease

Novel Systemic Treatment Modalities Including Immunotherapy and Molecular Targeted Therapy for Recurrent and Metastatic Head and Neck Squamous Cell Carcinoma

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