Evaluating and Reporting the Immunogenicity Impacts for Biological Products—a Clinical Pharmacology Perspective

Wang, Yow‐Ming; Wang, Jie; Hon, Yuen Yi; Zhou, Lin; Fang, Lanyan; Ahn, Hyun Soo

doi:10.1208/s12248-015-9857-y

Cited by 78 publications

(78 citation statements)

References 20 publications

(31 reference statements)

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“…The exposure–response and PK–pharmacodynamic models for tildrakizumab estimated EC 50 values at 0·36 μg mL −1 (90% confidence interval 0·22–0·61) and 0·25 μg mL −1 , respectively, implying that at these exposure levels at least half of the maximum effect in PASI 75 can be expected . The finding that the effects of ADAs on PK are more sensitive than the effects on clinical response has also been observed with other biologics …”

Section: Discussionmentioning

confidence: 61%

Assessment of the effects of immunogenicity on the pharmacokinetics, efficacy and safety of tildrakizumab

et al. 2019

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Summary Background We evaluated antidrug antibody (ADA) development in patients with chronic plaque psoriasis from three clinical trials of tildrakizumab, a humanized anti‐interleukin‐23p19 monoclonal antibody (P05495, reSURFACE 1 and reSURFACE 2). Objectives To determine the effects of immunogenicity on the pharmacokinetics, efficacy and safety of tildrakizumab. Methods In 1400 (weeks 12–16) and 780 (weeks 52–64) evaluable patients randomized to tildrakizumab 100 or 200 mg, treatment‐emergent ADA‐positive (TE‐POS) patients were identified and characterized for neutralizing antibodies (NAbs). Pharmacokinetics, safety and efficacy were evaluated by ADA status. Results In patients treated with tildrakizumab 100 or 200 mg continuously, < 7% were inconclusive at 52–64 weeks. In long‐term data through 52–64 weeks, the incidence of TE‐POS was 6·5% (100 mg) and 8·2% (200 mg) and the incidence of TE‐POS NAb‐POS was 2·5% (100 mg) and 3·2% (200 mg). TE‐POS NAb‐POS patients had modestly increased median tildrakizumab clearance (36·5%) compared with ADA‐NEG patients. Percentage Psoriasis Area and Severity Index improvements in TE‐POS NAb‐POS vs. ADA‐NEG patients on continuous treatment through week 52 were 76% (n = 10) vs. 91% (n = 342) for 100 mg and 77% (n = 12) vs. 87% (n = 299) for 200 mg. The incidence of potential immunogenicity‐related adverse events did not indicate a clear trend in any positive ADA patient category compared with ADA‐NEG patients through weeks 52–64. The effects of ADA on pharmacokinetics, efficacy and safety at 12–16 weeks were also summarized. Conclusions ADA development with tildrakizumab treatment for 52–64 weeks was low; around 3% of patients developed TE‐POS NAb‐POS ADAs and showed lower serum concentrations and corresponding reduced efficacy. No relationship between ADAs and safety was observed. What's already known about this topic? Unwanted immune responses – for example immunogenicity and antidrug antibodies (ADAs) – have been observed with therapeutic monoclonal antibodies and can affect efficacy and safety. Tildrakizumab is a humanized monoclonal antibody targeting interleukin‐23 and is currently approved for patients with plaque psoriasis. What does this study add? ADA development in tildrakizumab‐treated patients with psoriasis over 52 weeks was low. The small proportion of patients who had treatment‐emergent ADAs and had neutralizing antibodies experienced lower serum tildrakizumab concentrations and reduced efficacy. No relationship between ADAs and safety events was observed.

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Section: Discussionmentioning

confidence: 61%

Assessment of the effects of immunogenicity on the pharmacokinetics, efficacy and safety of tildrakizumab

et al. 2019

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“…86,87 ADAs against therapeutic mAbs can appear transiently or throughout the entire treatment period; can cause immune reactions such as anaphylaxis, cytokine release, and hypersensitivity; and may lead to complete or partial loss of efficacy because of target neutralization. The presence of ADAs can alter the PK of the drug, which in turn can influence safety and efficacy.…”

Section: Immunogenicitymentioning

confidence: 99%

Clinical Pharmacology Considerations for the Development of Immune Checkpoint Inhibitors

Sheng

Srivastava

Sanghavi

et al. 2017

The Journal of Clinical Pharma

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Immuno-oncology works through activation of the patient's immune system against cancer, with several advantages over other treatment approaches, including cytotoxic agents and molecular-targeted therapies. The most notable feature of immuno-oncology treatments is the nature of the patient responses achieved, which can be more durable and sustained than with other modalities. Increased understanding of immune system complexity has provided a number of opportunities to advance several strategies for the development of immuno-oncology therapies. This review outlines the clinical pharmacology characteristics and development challenges for the 6 approved immunomodulatory monoclonal antibodies that target 2 immune checkpoint pathways: ipilimumab (an anti-cytotoxic T-lymphocyte antigen-4 antibody) and, more recently, nivolumab and pembrolizumab (both anti-programmed death-1 antibodies) and atezolizumab, avelumab, and durvalumab (all anti-programmed death ligand-1 antibodies). These agents have revealed much about the clinical pharmacology features of immune checkpoint inhibitors as a class, as well as the pharmacometric approaches used to support their clinical development and regulatory approval. The development experiences with these pioneering immuno-oncology agents are likely to serve as useful guides in the discovery, progression, and approval of future drugs or combination of drugs in this class. This review includes summaries of the pharmacokinetics and exposure-response of the immune checkpoint inhibitors approved to date, as well as an overview of some quantitative systems pharmacology approaches. The ability of immuno-oncology to meet its full potential will depend on overcoming development challenges, including the need for clear strategies to determine optimal dose and scheduling for monotherapy as well as combination approaches. Keywords immunopharmacology, oncology, clinical pharmacology, clinical trials, pharmacology, immunotherapy, checkpoint inhibitorsIt could be said that if there were a book chronicling the history and progression of cancer treatment, we are now moving on from the chapter describing the time of sole reliance on chemotherapy, the chapter outlining the advent of targeted therapy is partially completed, and a new chapter on immuno-oncology is just beginning. The past few years have seen the regulatory approval of several immuno-oncology agents (Figure 1), including 6 immune checkpoint inhibitors: ipilimumab (Yervoy; Bristol-Myers Squibb), pembrolizumab (Keytruda; Merck), nivolumab (Opdivo; Bristol-Myers Squibb), atezolizumab (Tecentriq; Genentech), avelumab (Bavencio; EMD Serono), and durvalumab (Imfinzi; AstraZeneca). 1,2Immunotherapy in oncology is a switch from the cell-killing modality using relatively nonspecific cytotoxic methods (chemotherapy) or therapies that target cancer-specific pathways to methods that employ the patients' immune system to attack cancer. The immuno-oncology approach calls on the understanding of complex signaling processes of effector and regulatory...

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“…However, not all ADAs affect the efficacy and/or safety of the biologic: the titer (ie, amount), binding affinity, and ability to neutralize the biologic's activity also determine whether ADA formation is detrimental to therapy with the affected biologic. Humanized biologics have a low incidence of antidrug antibodies, and most do not neutralize the activity of the drug . The incidence reporting for immunogenicity is highly variable and dependent on the assay measuring the antidrug–antibody.…”

Section: Common Characteristics Of Biologicsmentioning

confidence: 99%

Core Entrustable Professional Activities in Clinical Pharmacology for Entering Residency: Biologics

Donnenberg

Mandić

Rhee

et al. 2017

The Journal of Clinical Pharma

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Evaluating and Reporting the Immunogenicity Impacts for Biological Products—a Clinical Pharmacology Perspective

Cited by 78 publications

References 20 publications

Assessment of the effects of immunogenicity on the pharmacokinetics, efficacy and safety of tildrakizumab

Assessment of the effects of immunogenicity on the pharmacokinetics, efficacy and safety of tildrakizumab

Clinical Pharmacology Considerations for the Development of Immune Checkpoint Inhibitors

Core Entrustable Professional Activities in Clinical Pharmacology for Entering Residency: Biologics

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