Dose dependence of treatment-related adverse events for immune checkpoint inhibitor therapies: a model-based meta-analysis

Шульгин, Б. В.; Kosinsky, Yuri; Omelchenko, A. V.; Chu, Lulu; Mugundu, Ganesh; Aksenov, Sergey; Pimentel, Rodrigo; DeYulia, Garrett; Kim, Geoffrey; Peskov, Kirill; Helmlinger, Gabriel

doi:10.1080/2162402x.2020.1748982

Cited by 24 publications

(29 citation statements)

References 93 publications

(119 reference statements)

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“…There is a dose-dependent increase in the frequency of irAEs secondary to ipilimumab and combination immunotherapy in particular. 14,27 With approval of ipilimumab at higher doses by the US Food and Drug Administration, the frequency of ICI-induced AA could increase. 14 Alternatively, ICI therapy may reveal or amplify pathology preferentially in those patients with pre-existing compromise of the hair follicle immune privilege.…”

Section: Discussionmentioning

confidence: 99%

“…Additionally, the ICI dosage used may be too low to induce collapse of the immune privilege at the hair follicle. There is a dose‐dependent increase in the frequency of irAEs secondary to ipilimumab and combination immunotherapy in particular 14,27 . With approval of ipilimumab at higher doses by the US Food and Drug Administration, the frequency of ICI‐induced AA could increase 14…”

Section: Discussionmentioning

confidence: 99%

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Alopecia areata as an immune‐related adverse event of immune checkpoint inhibitors: A review

Antoury

Maloney

Bach

et al. 2020

Dermatologic Therapy

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Immune checkpoint inhibitors (ICI) improve the ability of the immune system to target cancer cells by blocking signaling through either the cytotoxic T-lymphocyteassociated antigen 4 (CTLA-4), programmed cell death (PD-1) receptor, or its ligand (PD-L1). They have been found to cause a variety of immune-related adverse events (irAEs) including a form of nonscarring alopecia that resembles alopecia areata (AA) in presentation and histology. Clinical features of ICI-induced AA are poorly described. We queried the Pubmed database for cases of AA secondary to ICI use reporting on extent of hair loss, treatments attempted, alopecia outcome, and time of follow-up with 13 cases identified. Although most patients had localized hair loss with subsequent regrowth, four of them experienced extensive and persistent AA, lasting up to a year. All but one patient continued ICI after the onset of hair loss. Many used topical corticosteroids with varying outcomes. Possible prognostic factors for severe and persistent disease may include young age and male sex. However, the low number of reported cases limits the generalizability of these findings. Tumor response was positive in every case of immune-induced AA where it was reported. Further investigation will be needed to better characterize clinical features of this irAE, risk factors for persistent disease, and determine its optimal management.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Alopecia areata as an immune‐related adverse event of immune checkpoint inhibitors: A review

Antoury

Maloney

Bach

et al. 2020

Dermatologic Therapy

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“…Although anti-CTLA4 treatment allowed to the overall survival of melanoma to be reached, with even cure of metastatic disease, for about 20% of the patients [ 46 , 47 , 50 , 51 ], nevertheless clinical application is limited because of its AIEs [ 52 , 53 ]. It is likely that CTLA-4 blockade can promote recruitment of peripheral T cells, thus enhancing the probability of autoimmune reaction [ 54 ]. A correlation between dose and both efficacy and toxicity has been highlighted.…”

Section: Immune Checkpoint Blocker Delivery With Nanocarriersmentioning

confidence: 99%

Advanced Nanotechnology for Enhancing Immune Checkpoint Blockade Therapy

et al. 2021

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Immune checkpoint receptor signaling pathways constitute a prominent class of “immune synapse,” a cell-to-cell connection that represses T-lymphocyte effector functions. As a possible evolutionary countermeasure against autoimmunity, this strategy is aimed at lowering potential injury to uninfected cells in infected tissues and at minimizing systemic inflammation. Nevertheless, tumors can make use of these strategies to escape immune recognition, and consequently, such mechanisms represent chances for immunotherapy intervention. Recent years have witnessed the advance of pharmaceutical nanotechnology, or nanomedicine, as a possible strategy to ameliorate immunotherapy technical weaknesses thanks to its intrinsic biophysical properties and multifunctional modifying capability. To improve the long-lasting response rate of checkpoint blockade therapy, nanotechnology has been employed at first for the delivery of single checkpoint inhibitors. Further, while therapy via single immune checkpoint blockade determines resistance and a restricted period of response, strong interest has been raised to efficiently deliver immunomodulators targeting different inhibitory pathways or both inhibitory and costimulatory pathways. In this review, the partially explored promise in implementation of nanotechnology to improve the success of immune checkpoint therapy and solve the limitations of single immune checkpoint inhibitors is debated. We first present the fundamental elements of the immune checkpoint pathways and then outline recent promising results of immune checkpoint blockade therapy in combination with nanotechnology delivery systems.

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“…Hingegen könnte bei einer Uveitis anterior (Grad-2-Nebenwirkung) die Therapie mit dem Checkpoint-Inhibitor fortgeführt werden [9]. Bei der Therapie mit PD1-Inhibitoren konnte ein Zusammenhang der Nebenwirkungen mit der verabreichten Medikamentendosis nicht nachgewiesen werden, sodass eine Dosisreduktion beim Auftreten von Nebenwirkungen vorerst keine Alternative darstellt [10]. Insgesamt zeigen sich die meisten in der Literatur beschriebenen Uveitiden, welche durch die Therapie mit Checkpoint-Inhibitoren ausgelöst werden, unter der Therapie mit topischen, periokulären oder systemischen Steroiden rückläufig [1,4].…”

Section: Diskussionunclassified

Beidseitige Nivolumab-assoziierte Vogt-Koyanagi-Harada-artige Uveitis bei einem Patienten mit metastasiertem Nierenzellkarzinom

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Wawrzynów

Chamalis

et al. 2021

Klin Monbl Augenheilkd

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Mit dem vermehrten Einsatz von Immun-Checkpoint-Inhibitoren in der Behandlung verschiedener, häufig bisher nicht therapierbarer Tumorerkrankungen treten immer häufiger autoimmune Nebenwirkungen auf. Hierzu zählt auch die Uveitis. Die medikamenteninduzierte Uveitis stellt somit ein seltenes, jedoch zunehmend auftretendes Krankheitsbild dar. ▶ Abb. 1 (a = rechts, b = links): Spaltlampenfotografie des Glaskörpers. Es finden sich beidseits Entzündungszellen und "snow balls".

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Dose dependence of treatment-related adverse events for immune checkpoint inhibitor therapies: a model-based meta-analysis

Cited by 24 publications

References 93 publications

Alopecia areata as an immune‐related adverse event of immune checkpoint inhibitors: A review

Alopecia areata as an immune‐related adverse event of immune checkpoint inhibitors: A review

Advanced Nanotechnology for Enhancing Immune Checkpoint Blockade Therapy

Beidseitige Nivolumab-assoziierte Vogt-Koyanagi-Harada-artige Uveitis bei einem Patienten mit metastasiertem Nierenzellkarzinom

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