Humanized Affinity-matured Monoclonal Antibody 8H9 Has Potent Antitumor Activity and Binds to FG Loop of Tumor Antigen B7-H3

Ahmed, Mahiuddin; Cheng, Ming Huei; Zhao, Qi; Goldgur, Yehuda; Cheal, Sarah M.; Guo, Hong-Fen; Larson, Steven M.; Cheung, Nai‐Kong V.

doi:10.1074/jbc.m115.679852

Cited by 87 publications

(75 citation statements)

References 64 publications

(68 reference statements)

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“…IgG1 is the human isotype most effective at stimulating ADCC or CDC in humans and mice, and other anti-CD276 IgG1s have been shown to elicit ADCC in preclinical studies (Ahmed et al, 2015; Loo et al, 2012) suggesting that m276 could also have therapeutic activity on its own. However, preliminary studies in mice indicated that m276 had little, if any, anti-tumor activity.…”

Section: Resultsmentioning

confidence: 99%

“…Another humanized antibody, 8H9, originally identified based on its selective reactivity with human tumors cells, was later found to recognize CD276 and is also in Phase I clinical trials (Ahmed et al, 2015; Modak et al, 2001). However, these mAbs recognize human but not rodent CD276 precluding an assessment of the contribution of CD276 positive tumor-associated stromal cells in therapeutic targeting, and potential toxicities caused by inappropriate targeting of CD276 positive normal cells in preclinical rodent models.…”

Section: Introductionmentioning

confidence: 99%

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Eradication of Tumors through Simultaneous Ablation of CD276/B7-H3-Positive Tumor Cells and Tumor Vasculature

Seaman

Zhu²,

Saha³

et al. 2017

Cancer Cell

293

313

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SUMMARY Targeting the tumor vasculature with antibody-drug conjugates (ADCs) is a promising anti-cancer strategy that, in order to be realized, must overcome several obstacles, including identification of suitable targets and optimal warheads. Here, we demonstrate that the cell surface protein CD276/B7-H3 is broadly overexpressed by multiple tumor types on both cancer cells and tumor-infiltrating blood vessels, making it a potentially ideal dual-compartment therapeutic target. In preclinical studies CD276-ADCs armed with a conventional MMAE warhead destroyed CD276-positive cancer cells, but were ineffective against tumor vasculature. In contrast, pyrrolobenzodiazepine-conjugated CD276-ADCs killed both cancer cells and tumor vasculature, eradicating large established tumors and metastases, and improving long-term overall survival. CD276 targeted dual-compartment ablation could aid in development of highly selective broad-acting anti-cancer therapies.

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Eradication of Tumors through Simultaneous Ablation of CD276/B7-H3-Positive Tumor Cells and Tumor Vasculature

Seaman

Zhu²,

Saha³

et al. 2017

Cancer Cell

293

313

View full text Add to dashboard Cite

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“…8H9 is a mAb specific to B7-H3 that demonstrated clinical success as an ADC following it being radiolabeled to iodine-131 ( 131 I) and administrated to patients with metastatic central nervous system neuroblastoma (49). 8H9 also distinguishes itself from other B7-H3 specific antibodies in that it binds to the FG loop of B7-H3, a region critical to its immunological function (50). Recently, 8H9 was humanized and affinity matured and maintained its ability to kill B7-H3 positive neuroblastoma cells in vitro .…”

Section: Clinical-translational Advancesmentioning

confidence: 99%

“…Two-fold and five-fold enhancements in killing were observed by the affinity matured and humanized 8H9 compared to the non-matured and chimeric generations, respectively. Furthermore, the mAb was labeled with 131 I and injected into athymic nude mice xenografted with human neuroblastoma and showed successful biodistribution to the tumor (50). Currently, clinical trials with radiolabeled 8H9 are ongoing in patients with peritoneal cancers, gliomas, and advanced central nervous system cancers (NCT01099644, NCT01502917, and NCT00089245).…”

Section: Clinical-translational Advancesmentioning

confidence: 99%

Molecular Pathways: Targeting B7-H3 (CD276) for Human Cancer Immunotherapy

Picarda

Ohaegbulam

Zang

2016

Clinical Cancer Research

399

340

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B7-H3 (CD276) is an important immune checkpoint member of the B7 and CD28 families. Induced on antigen presenting cells, B7-H3 plays an important role in the inhibition of T cell function. Importantly, B7-H3 is highly overexpressed on a wide range of human solid cancers and often correlates with both negative prognosis and poor clinical outcome in patients. Challenges remain to identify the receptor(s) of B7-H3 and thus better elucidate the role of the B7-H3 pathway in immune responses and tumor evasion. With a preferential expression on tumor cells, B7-H3 is an attractive target for cancer immunotherapy. Based on the clinical success of inhibitory immune checkpoint blockade (CTLA-4, PD-1 and PD-L1), developing monoclonal antibodies (mAbs) against B7-H3 appears promising therapeutic strategies. An unconventional mAb against B7-H3 with antibody-dependent cell-mediated cytotoxicity is currently being evaluated in a Phase I clinical trial and has shown encouraging preliminary results. Additional therapeutic approaches in targeting B7-H3, such as blocking mAbs, bispecific mAbs, chimeric antigen receptor T cells, small molecules inhibitors, and combination therapies should be evaluated as these technologies have already shown positive results in various cancer settings. A better understanding of the B7-H3 pathway in humans will surely help to further optimize associated cancer immunotherapies.

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“…It is also being evaluated in combination with ipilimumab (anti-CTLA-4 mAb) or pembrolizumab (anti-PD-1 mAb) in safety studies of refractory cancers (trial NCT02381314 and NCI201501495). The murine mAb 8H9 was found to target an unknown antigen on many solid tumors, and only recently has this antigen been discovered to be B7-H3 [59]. Radioimmunoconjugated 8H9 with cytotoxic I131 is currently in phase I trials for central nervous system and peritoneal tumors (NCT01099644 and NCT01502917), and other groups are testing 8H9 with other toxic conjugates [60] in murine models.…”

Section: New Immune Checkpoints B7-h3 B7x and Hhla2mentioning

confidence: 99%

The expanding repertoire of targets for immune checkpoint inhibition in bladder cancer: What lies beneath the tip of the iceberg, PD-L1

Sankin

Narasimhulu

John

et al. 2018

Urologic Oncology: Seminars and Original Investigations

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Over the last decade, a new understanding of tumor-immune system interplay has been ushered in, lead in large part by the discovery of immune checkpoints mediated through B7-CD28 family interactions. Therapeutic blockade of the PD-L1 immune checkpoint pathway has already shown great success as a cancer immunotherapy for advanced urothelial carcinoma, leading to durable clinical remissions in an otherwise incurable disease. There are newly described members of the B7-CD28 family including B7-H3, B7x, and HHLA2. These ligands are thought to play an essential role in suppressing T-cell response, leading to immune tolerance of tumors. This feature makes them attractive targets for novel immunotherapy treatment paradigms. Here, we review the literature of current strategies and future directions of immune checkpoint blockade therapy for bladder cancer.

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Humanized Affinity-matured Monoclonal Antibody 8H9 Has Potent Antitumor Activity and Binds to FG Loop of Tumor Antigen B7-H3

Cited by 87 publications

References 64 publications

Eradication of Tumors through Simultaneous Ablation of CD276/B7-H3-Positive Tumor Cells and Tumor Vasculature

Eradication of Tumors through Simultaneous Ablation of CD276/B7-H3-Positive Tumor Cells and Tumor Vasculature

Molecular Pathways: Targeting B7-H3 (CD276) for Human Cancer Immunotherapy

The expanding repertoire of targets for immune checkpoint inhibition in bladder cancer: What lies beneath the tip of the iceberg, PD-L1

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