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Submitted URL: https://be6aprogram.com/
Effective URL: https://www.pfizerclinicaltrials.com/HCP/Be6A/C575
Submission: On May 18 via api from US — Scanned from DE

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SIGVOTATUG VEDOTIN (SV/SGN-B6A):


A NOVEL INTEGRIN
BETA-6-DIRECTED THERAPEUTIC APPROACH IN CANCER

The information provided on this page is intended for health care professionals
in the United States only.

Get Started



SIGVOTATUG VEDOTIN (SV/SGN-B6A):


A NOVEL INTEGRIN
BETA-6-DIRECTED THERAPEUTIC APPROACH IN CANCER

The information provided on this page is intended for health care professionals
in the United States only.

Get Started




The Be6A program is a series of clinical studies evaluating sigvotatug vedotin
in multiple solid tumors expression integrin beta-6 (IB6)

Sigvotatug vedotin is a first-in-class investigational antibody-drug conjugate
(ADC) designed to deliver the cytotoxic payload monomethyl auristatin E (MMAUE)
to cells expressing IB6. IB6 is a surface cell receptor overexpressed in many
solid tumors, such as non-small cell lung cancer (NSCLC), head and neck squamous
cell carcinoma (HNSCC), esophageal cancer, and cutaneous squamous cell
carcinoma.1

Data from the initial clinical study of sigvotatug vedotin demonstrates
preliminary and encouraging antitumor activity and durability with a tolerable
and manageable safety profile in heavily pretreated patients.2,3

Read on to learn more about sigvotatug vedotin and cancers that overexpress IB6
to see if your patients may qualify for enrolling studies.


PROPOSED MECHANISM OF ACTION

Sigvotatug Vedotin is thought to induce tumor cell death through:

 * Direct cytotoxicity via preferential release of MMAE within target cells and
   subsequent apoptosis
 * The bystander effect
 * Immunogenic cell death4,5




ABOUT IB6-OVEREXPRESSING CANCERS

IB6 is a member of the integrin family of proteins involved in cellular
adhesion, motility, and cytokinesis. IB6 is expressed at low levels in normal
adult epithelial tissues, but expression is induced by tissue injury due to its
role in wound repair.6 High levels of IB6 expression have been demonstrated in
different types of cancer1 and are associated with poor prognosis based on
multiple retrospective analyses.7,8 Additional investigations suggest tumors may
exploit the remodeling function associated with IB6 to promote invasiveness and
metastasis.9,10

Recruiting
Sigvotatug Vedotin for Non-Small Cell Lung Cancer (Be6A-LUNG-01)

This Phase 3 study will evaluate sigvotatug vedotin versus docetaxel for
patients with previously treated metastatic non-small cell lung cancer.

Connect with a clinical trial site
Recruiting
Sigvotatug Vedotin for Advanced Solid Tumors

This Phase 1 study will evaluate sigvotatug vedotin monotherapy and in
combination with pembrolizumab for patients with advanced solid tumors.

View clinical trial listing


TO CONNECT WITH PFIZER ABOUT THE BE6A PROGRAM CLICK HERE.

Is this page helpful?


References

1. Lyon, RP, Jonas M, Frantz C et al. SGN-B6A: A new vedotin antibody-drug
conjugate directed to integrin beta-6 for multiple carcinoma indications. Mol
Cancer Ther. 2023;MCT02200817. doi:10.1158/1535-7163
2. Hollebecque A, Lopez J, Piha-Paul S, et al. A first-in-human of an integrin
beta-6 targeted antibody-drug conjugate (ADC), SGN-B6A, in patients with
advanced solid tumors: interim results of a phase 1 study (SGN-B6A-001). J
Immunother Cancer. 2022;10(Suppl 2):A763
3. Hollebecque A, Lopez J, Piha-Paul, SA, et al. A first-in-human trial of an
integrin beta-6 targeted antibody-drug conjugate (ADC), SGN-B6A, in patients
with advanced solid tumors: Interim results of a Phase 1 study (SGNB6A-001).
Poster presented at Society for Immunotherapy of Cancer Annual Meeting; Nov
8-12. 2022; Boston, MA.
4. Lyon R, Trang V, Gosnik JJ, et al. Abstract 1522: SGN-B6A induces immunogenic
cell death as an additional mechanism of action. J ImmunoTher Cancer. 2022;
10(suppl 2). doi:10.1136/jitc-2022-SITC2022. 1186
5. Trang VH, Mazahreh R, Gosnik JJ, et al. Abstract 1522: SGN-B6A induces
immunogenic cell death as an additional mechanism of action. Cancer Res.
2023;83(suppl 7):1522-1522. doi:10.1158/1538-7445.am2023-1522
6. Van Aarsen LA, Leone DR, Ho S, et al. Antibody-mediated blockade of integrin
alpha v beta 6 inhibits tumor progression in vivo by transforming growth
factor-beta-regulated mechanism. CancerRes.
2008;68(2):561-570.doi:10.1158/008-5472.CAN07-0245
7. Elayadi AN, Samli KN, Prudkin L, et al. A peptide selected by biopanning
identifies the integrin alphabeta6 as a prognostic biomarker for nonsmall cell
lung cancer. Cancer Res. 2007:67(12):5889-5895.
8. Elez E, Kocakova I, Hokler T, et al. Abituzumab combined with cetuximab plus
irinotecan versus cetuximab plus irinotecan alone for patients with KRAS
wild-type metastatic colorectal cancer: the randomised phase I/II POSEIDON
trial. Ann Oncol. 2015;26(1):13-140. doi:10.1093/annonc/mdu474
9. Hamidi H, Ivaska J. Every step of the way: integrins in cancer progression
and metastasis. Nat Rev Cancer. 2018:18(9):533-548.
doi:10.1038/s41568-018-0038-z
10. Marsh D, Dickinson S, Neill GW, Marshall JF, Hart IR, Thomas GJ. Apha vbeta
6 integrin promotes the invasion of morphoeic basal cell carcinoma through
stromal modulation. Cancer Res.
2008:68(9):3295-3303.doi:10.1158/0008-5472.CAN-08-0174

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