Blood retinal barrier and ocular pharmacokinetics: Considerations for the development of oncology drugs

Williamson, Beth; Reddy, Venkatesh Pilla

doi:10.1002/bdd.2276

Cited by 6 publications

(6 citation statements)

References 57 publications

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“…On one hand, transporter-mediated DDIs at the BRB due to concomitant treatment with drugs which inhibit ABCB1 and/or ABCB2 could contribute to enhanced ocular and in particular retinal toxicity of drugs that normally penetrate poorly into the eye, such as imatinib ( Ho et al, 2013 ), other tyrosine kinase inhibitors ( Williamson and Reddy, 2021 ), ciprofloxacin ( Ramirez et al, 2011 ), tamoxifen ( Griffin and Garnick, 1981 ; Noureddin et al, 1999 ; Grzybowski et al, 2015 ) and methotrexate ( Balachandran et al, 2002 ; Iqbal et al, 2005 ; Sbeity et al, 2006 ; Sharma and Sharma, 2011 ; Grzybowski et al, 2015 ) (see Supplementary Table S3 ). On the other hand, DDIs could generate therapeutic benefits by enhancing the ocular penetration of systemic treatments for retinal disorders struggling to cross the BRB, which represents so far a major challenge for ocular drug delivery ( Jordán and Ruíz-Moreno, 2013 ; Agrahari et al, 2016 ; Pascual-Pasto et al, 2017 ; Kim and Woo, 2021 ).…”

Section: Discussionmentioning

confidence: 99%

ABCB1 and ABCG2 Together Limit the Distribution of ABCB1/ABCG2 Substrates to the Human Retina and the ABCG2 Single Nucleotide Polymorphism Q141K (c.421C> A) May Lead to Increased Drug Exposure

et al. 2021

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The widely expressed and poly-specific ABC transporters breast cancer resistance protein (ABCG2) and P-glycoprotein (ABCB1) are co-localized at the blood-brain barrier (BBB) and have shown to limit the brain distribution of several clinically used ABCB1/ABCG2 substrate drugs. It is currently not known to which extent these transporters, which are also expressed at the blood-retinal barrier (BRB), may limit drug distribution to the human eye and whether the ABCG2 reduced-function single-nucleotide polymorphism (SNP) Q141K (c.421C > A) has an impact on retinal drug distribution. Ten healthy male volunteers (five subjects with the c.421CC and c.421CA genotype, respectively) underwent two consecutive positron emission tomography (PET) scans after intravenous injection of the model ABCB1/ABCG2 substrate [11C]tariquidar. The second PET scan was performed with concurrent intravenous infusion of unlabelled tariquidar to inhibit ABCB1 in order to specifically reveal ABCG2 function.In response to ABCB1 inhibition with unlabelled tariquidar, ABCG2 c.421C > A genotype carriers showed significant increases (as compared to the baseline scan) in retinal radiotracer influx K1 (+62 ± 57%, p = 0.043) and volume of distribution VT (+86 ± 131%, p = 0.043), but no significant changes were observed in subjects with the c.421C > C genotype. Our results provide the first evidence that ABCB1 and ABCG2 may together limit the distribution of systemically administered ABCB1/ABCG2 substrate drugs to the human retina. Functional redundancy between ABCB1 and ABCG2 appears to be compromised in carriers of the c.421C > A SNP who may therefore be more susceptible to transporter-mediated drug-drug interactions at the BRB than non-carriers.

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Section: Discussionmentioning

confidence: 99%

ABCB1 and ABCG2 Together Limit the Distribution of ABCB1/ABCG2 Substrates to the Human Retina and the ABCG2 Single Nucleotide Polymorphism Q141K (c.421C> A) May Lead to Increased Drug Exposure

et al. 2021

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“…Hence, understanding the relationship between efflux ratio and ocular exposure is crucial for PK understanding. As previously discussed (Williamson and Pilla Reddy 2021 ), melanin binding must be considered to accurately assess the free ocular exposure. However, differences in melanin levels across species and the localization of melanin within ocular tissues including the RPE layer (Jakubiak et al 2018 ; Leblanc et al 1998 ) hinders the interpretation of the free levels.…”

Section: Discussionmentioning

confidence: 99%

Pharmacological inhibition of MERTK induces in vivo retinal degeneration: a multimodal imaging ocular safety assessment

et al. 2022

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The receptor tyrosine kinase, MERTK, plays an essential role in homeostasis of the retina via efferocytosis of shed outer nuclear segments of photoreceptors. The Royal College of Surgeons rat model of retinal degeneration has been linked to loss-of-function of MERTK, and together with the MERTK knock-out mouse, phenocopy retinitis pigmentosa in humans with MERTK mutations. Given recent efforts and interest in MERTK as a potential immuno-oncology target, development of a strategy to assess ocular safety at an early pre-clinical stage is critical. We have applied a state-of-the-art, multi-modal imaging platform to assess the in vivo effects of pharmacological inhibition of MERTK in mice. This involved the application of mass spectrometry imaging (MSI) to characterize the ocular spatial distribution of our highly selective MERTK inhibitor; AZ14145845, together with histopathology and transmission electron microscopy to characterize pathological and ultra-structural change in response to MERTK inhibition. In addition, we assessed the utility of a human retinal in vitro cell model to identify perturbation of phagocytosis post MERTK inhibition. We identified high localized total compound concentrations in the retinal pigment epithelium (RPE) and retinal lesions following 28 days of treatment with AZ14145845. These lesions were present in 4 of 8 treated animals, and were characterized by a thinning of the outer nuclear layer, loss of photoreceptors (PR) and accumulation of photoreceptor outer segments at the interface of the RPE and PRs. Furthermore, the lesions were very similar to that shown in the RCS rat and MERTK knock-out mouse, suggesting a MERTK-induced mechanism of PR cell death. This was further supported by the observation of reduced phagocytosis in the human retinal cell model following treatment with AZ14145845. Our study provides a viable, translational strategy to investigate the pre-clinical toxicity of MERTK inhibitors but is equally transferrable to novel chemotypes.

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“…This suggests that another potential application of PEGylation could be to modulate ocular biodistribution of systemically administered proteins or antibodies. We sought to investigate if PEGylation could impact the biodistribution of a full length antibody targeting MerTK, a therapeutic target of interest with risk of ocular toxicity …”

Section: Introductionmentioning

confidence: 99%

“…MerTK, a member of the Tyro3-Axl-Mer receptor tyrosine kinase family, plays an important role in tissue homeostasis, remodeling, preventing autoimmunity, and controlling inflammation. , MerTK recognizes externalized phosphatidylserine on apoptotic cells via the bridging molecules Gas6 or ProteinS, , and engulfs apoptotic cells in a process known as efferocytosis. , MerTK expressed on tumor associated macrophages (TAMs) is hypothesized to promote an immune suppressive tumor microenvironment, therefore inhibiting antitumor immunity . Several groups have published studies investigating antagonism of MerTK to promote antitumor immune response, showing promising results as a single agent as well as in combination with checkpoint immune therapy , and cytotoxic agents. − While MerTK is a target of interest for cancer immunotherapy, on-target ocular toxicity remains a key concern for clinical development . MerTK is expressed on retinal pigment epithelial cells (RPEs) and has an essential role in the diurnal phagocytosis of shed photoreceptor outer segments. , Mutation or knockout of MerTK in mice results in accumulation of cell debris and photoreceptor death leading to loss of vision. , Consistent with genetic studies, therapeutic blockade of MerTK has been shown to induce retinal degeneration in preclinical models with both a small molecule and an antibody …”

Section: Introductionmentioning

confidence: 99%

“…We sought to investigate if PEGylation could impact the biodistribution of a full length antibody targeting MerTK, a therapeutic target of interest with risk of ocular toxicity. 15 MerTK, a member of the Tyro3-Axl-Mer receptor tyrosine kinase family, plays an important role in tissue homeostasis, remodeling, preventing autoimmunity, and controlling inflammation. 16,17 MerTK recognizes externalized phosphatidylserine on apoptotic cells via the bridging molecules Gas6 or ProteinS, 18,19 and engulfs apoptotic cells in a process known as efferocytosis.…”

Section: ■ Introductionmentioning

confidence: 99%

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PEGylation of anti-MerTK Antibody Modulates Ocular Biodistribution

Vollmar¹,

Fei²,

Liang³

et al. 2022

Bioconjugate Chem.

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Here, we explore whether PEGylation of antibodies can modulate their biodistribution to the eye, an organ once thought to be immune privileged but has recently been shown to be accessible to IV-administered large molecules, such as antibodies. We chose to PEGylate an anti-MerTK antibody, a target with known potential for ocular toxicity, to minimize biodistribution to retinal pigment epithelial cells (RPEs) in the eye by increasing the hydrodynamic volume of the antibody. We used site-specific conjugation to an engineered cysteine on anti-MerTK antibody to chemically attach 40-kDa branched or linear PEG polymers. Despite reduced binding to MerTK on cells, site-specifically PEGylated anti-MerTK retained similar potency in inhibiting MerTK-mediated macrophage efferocytosis of apoptotic cells. Importantly, we found that PEGylation of anti-MerTK significantly reduced MerTK receptor occupancy in RPE cells in both naïve mice and MC-38 tumor-bearing mice, with the branched PEG exhibiting a greater effect than linear PEG. Furthermore, similar to unconjugated anti-MerTK, PEGylated anti-MerTK antibody triggered type I IFN response and exhibited antitumor effect in syngeneic mouse tumor studies. Our results demonstrate the potential of PEGylation to control ocular biodistribution of antibodies.

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Blood retinal barrier and ocular pharmacokinetics: Considerations for the development of oncology drugs

Cited by 6 publications

References 57 publications

ABCB1 and ABCG2 Together Limit the Distribution of ABCB1/ABCG2 Substrates to the Human Retina and the ABCG2 Single Nucleotide Polymorphism Q141K (c.421C> A) May Lead to Increased Drug Exposure

ABCB1 and ABCG2 Together Limit the Distribution of ABCB1/ABCG2 Substrates to the Human Retina and the ABCG2 Single Nucleotide Polymorphism Q141K (c.421C> A) May Lead to Increased Drug Exposure

Pharmacological inhibition of MERTK induces in vivo retinal degeneration: a multimodal imaging ocular safety assessment

PEGylation of anti-MerTK Antibody Modulates Ocular Biodistribution

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