Cancer Research

, том 81 , издание 12 , страницы 3402-3414

Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors

Darren C. Phillips ¹

Fritz G. Buchanan ¹

Dong Cheng ¹

Larry R. Solomon ²

Yu Xiao ¹

John Xue ¹

Stephen K. Tahir ¹

Morey L Smith ¹

Haichao Zhang ¹

Deborah Widomski ¹

Vivek C Abraham ¹

Nan Xu ¹

Zhihong Liu ¹

Li Zhou ³

Enrico Digiammarino ³

Xin Lu ⁴

Nandini Rudra-Ganguly ⁵

Bruce Trela ⁶

Susan E Morgan Lappe ¹

Скрыть аффилиации авторов Показать аффилиации авторов: 6 аффилиаций

1Oncology Discovery, AbbVie Inc., North Chicago, Illinois. |

2Abbvie Inc., North Chicago, Illinois. |

3Protein Biochemistry, AbbVie Inc., North Chicago, Illinois. |

⁴

4Genomic Research Center, AbbVie Inc., North Chicago, Illinois. |

⁵

5Drug Metabolism and Pharmacokinetics, AbbVie Inc., North Chicago, Illinois. |

⁶

6Pre-clinical Safety, AbbVie Inc., North Chicago, Illinois. |

Тип публикации: Journal Article

Дата публикации: 2021-03-09

American Association for Cancer Research (AACR)

Cancer Research

scimago Q1

wos Q1

БС1

SJR: 3.879

CiteScore: 17.8

Impact factor: 16.6

ISSN: 00085472, 15387445

DOI: 10.1158/0008-5472.can-20-2178

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PubMed ID: 33687950

Cancer Research

Oncology

Краткое описание

TRAIL can activate cell surface death receptors, resulting in potent tumor cell death via induction of the extrinsic apoptosis pathway. Eftozanermin alfa (ABBV-621) is a second generation TRAIL receptor agonist engineered as an IgG1-Fc mutant backbone linked to two sets of trimeric native single-chain TRAIL receptor binding domain monomers. This hexavalent agonistic fusion protein binds to the death-inducing DR4 and DR5 receptors with nanomolar affinity to drive on-target biological activity with enhanced caspase-8 aggregation and death-inducing signaling complex formation independent of FcγR-mediated cross-linking, and without clinical signs or pathologic evidence of toxicity in nonrodent species. ABBV-621 induced cell death in approximately 36% (45/126) of solid cancer cell lines in vitro at subnanomolar concentrations. An in vivo patient-derived xenograft (PDX) screen of ABBV-621 activity across 15 different tumor indications resulted in an overall response (OR) of 29% (47/162). Although DR4 (TNFSFR10A) and/or DR5 (TNFSFR10B) expression levels did not predict the level of response to ABBV-621 activity in vivo, KRAS mutations were associated with elevated TNFSFR10A and TNFSFR10B and were enriched in ABBV-621–responsive colorectal carcinoma PDX models. To build upon the OR of ABBV-621 monotherapy in colorectal cancer (45%; 10/22) and pancreatic cancer (35%; 7/20), we subsequently demonstrated that inherent resistance to ABBV-621 treatment could be overcome in combination with chemotherapeutics or with selective inhibitors of BCL-XL. In summary, these data provide a preclinical rationale for the ongoing phase 1 clinical trial (NCT03082209) evaluating the activity of ABBV-621 in patients with cancer.

Significance:

This study describes the activity of a hexavalent TRAIL-receptor agonistic fusion protein in preclinical models of solid tumors that mechanistically distinguishes this molecular entity from other TRAIL-based therapeutics.

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31 публикация, 279 цитирований, 4 рецензии

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Московский государственный университет имени М.В. Ломоносова

Институт биоорганической химии им. академиков М.М. Шемякина и Ю.А. Овчинникова РАН

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Phillips D. C. et al. Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors // Cancer Research. 2021. Vol. 81. No. 12. pp. 3402-3414.

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Phillips D. C., Buchanan F. G., Cheng D., Solomon L. R., Xiao Yu., Xue J., Tahir S. K., Smith M. L., Zhang H., Widomski D., Abraham V. C., Xu N., Liu Z., Zhou L., Digiammarino E., Lu X., Rudra-Ganguly N., Trela B., Morgan Lappe S. E. Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors // Cancer Research. 2021. Vol. 81. No. 12. pp. 3402-3414.

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TY - JOUR

DO - 10.1158/0008-5472.can-20-2178

UR - https://doi.org/10.1158/0008-5472.can-20-2178

TI - Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors

T2 - Cancer Research

AU - Phillips, Darren C.

AU - Buchanan, Fritz G.

AU - Cheng, Dong

AU - Solomon, Larry R.

AU - Xiao, Yu

AU - Xue, John

AU - Tahir, Stephen K.

AU - Smith, Morey L

AU - Zhang, Haichao

AU - Widomski, Deborah

AU - Abraham, Vivek C

AU - Xu, Nan

AU - Liu, Zhihong

AU - Zhou, Li

AU - Digiammarino, Enrico

AU - Lu, Xin

AU - Rudra-Ganguly, Nandini

AU - Trela, Bruce

AU - Morgan Lappe, Susan E

PY - 2021

DA - 2021/03/09

PB - American Association for Cancer Research (AACR)

SP - 3402-3414

IS - 12

VL - 81

PMID - 33687950

SN - 0008-5472

SN - 1538-7445

ER -

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@article{2021_Phillips,

author = {Darren C. Phillips and Fritz G. Buchanan and Dong Cheng and Larry R. Solomon and Yu Xiao and John Xue and Stephen K. Tahir and Morey L Smith and Haichao Zhang and Deborah Widomski and Vivek C Abraham and Nan Xu and Zhihong Liu and Li Zhou and Enrico Digiammarino and Xin Lu and Nandini Rudra-Ganguly and Bruce Trela and Susan E Morgan Lappe},

title = {Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors},

journal = {Cancer Research},

year = {2021},

volume = {81},

publisher = {American Association for Cancer Research (AACR)},

month = {mar},

url = {https://doi.org/10.1158/0008-5472.can-20-2178},

number = {12},

pages = {3402--3414},

doi = {10.1158/0008-5472.can-20-2178}

}

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Phillips, Darren C., et al. “Hexavalent TRAIL Fusion Protein Eftozanermin Alfa Optimally Clusters Apoptosis-Inducing TRAIL Receptors to Induce On-Target Antitumor Activity in Solid Tumors.” Cancer Research, vol. 81, no. 12, Mar. 2021, pp. 3402-3414. https://doi.org/10.1158/0008-5472.can-20-2178.

Издатель

American Association for Cancer Research (AACR)

Журнал

Cancer Research

scimago Q1

wos Q1

БС1

SJR

3.879

CiteScore

17.8

Impact factor

16.6

ISSN

00085472 (Print)

15387445 (Electronic)