Discovery of Cytotoxic Dolastatin 10 Analogues with N-Terminal Modifications

Maderna, Andreas; Doroski, Matthew; Subramanyam, Chakrapani; Porte, Alexander M.; Leverett, Carolyn A.; Vetelino, Beth C.; Chen, Zecheng; Risley, Hud; Parris, Kevin; Pandit, J.; Varghese, Alison H.; Shanker, Suman; Song, Cynthia; Sukuru, Sai Chetan K.; Farley, Kathleen A.; Wagenaar, M.; Shapiro, Michael J.; Musto, Sylvia; Lam, My-Hanh; Loganzo, Frank; O’Donnell, Christopher J

doi:10.1021/jm501649k

Cited by 120 publications

(167 citation statements)

References 37 publications

Supporting

Mentioning

160

Contrasting

Unclassified

Order By: Relevance

“…This is quite intriguing and clearly demonstrates a divergence of SAR between auristatins and tubulysins, as such substituents have yielded very potent auristatins. 14 Overall, tertiary amine 8g, containing an α-methyl tertiary amine designed based on our auristatin SAR, 14 provided the best balance of potency against a variety of cell lines, including the MDR1 expressing KB 8.5 line. It should be noted that 8g was predicted to overlay better with compound 2, especially the position of the terminal N atom, than compound 8f (Figure 2C vs D), thus giving support for our design approach.…”

Section: Acs Medicinal Chemistry Lettersmentioning

confidence: 98%

“…We selected ester 4 rather than the corresponding natural acid-containing Tup C-terminus for exploring N-termini SAR, primarily to minimize possible diminished activity in a cellbased assay, known to be reliant on permeability. 14 The Ntermini modified library (analogues 8a−g) was generated by coupling of the amine 4, prepared from known intermediate 7, 17 with selected Boc-or Fmoc-protected amino acids and removal of the protecting group (Scheme 1). N87 cells (liver metastasis from gastric carcinoma) and MDA-MB-361-DYT2 cells (breast carcinoma) were employed for cytotoxic evaluation of tubulysin analogues.…”

Section: Acs Medicinal Chemistry Lettersmentioning

confidence: 99%

“…There were two consistent observations during the library design using shape-based molecular overlay. First, the amide bond between Ile and Tuv residues in tubulysins appeared to be trans as compared to the cis configuration 14 between corresponding Val and Dil residues in the tubulin-bound auristatin ( Figure 2B). Second, the N-terminal backbone stereochemical differences between the compound classes ( Figure 2A,B) seem to have a direct impact on the position of the terminal N atom, especially in compounds with cyclic monomers 17f ( Figure 2C) and 17g ( Figure 2D).…”

mentioning

confidence: 99%

See 2 more Smart Citations

Design, Synthesis, and Cytotoxic Evaluation of Novel Tubulysin Analogues as ADC Payloads

Leverett

Sukuru

Vetelino

et al. 2016

ACS Med. Chem. Lett.

Self Cite

View full text Add to dashboard Cite

ABSTRACT:The tubulysin class of natural products has attracted much attention from the medicinal chemistry community due to its potent cytotoxicity against a wide range of human cancer cell lines, including significant activity in multidrug-resistant carcinoma models. As a result of their potency, the tubulysins have become an important tool for use in targeted therapy, being widely pursued as payloads in the development of novel small molecule drug conjugates (SMDCs) and antibody−drug conjugates (ADCs). A structure-based and parallel medicinal chemistry approach was applied to the synthesis of novel tubulysin analogues. These efforts led to the discovery of a number of novel and potent cytotoxic tubulysin analogues, providing a framework for our simultaneous report, which highlights the discovery of tubulysin-based ADCs, including use of site-specific conjugation to address in vivo stability of the C-11 acetate functionality.

show abstract

Section: Acs Medicinal Chemistry Lettersmentioning

confidence: 98%

Section: Acs Medicinal Chemistry Lettersmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Design, Synthesis, and Cytotoxic Evaluation of Novel Tubulysin Analogues as ADC Payloads

Leverett

Sukuru

Vetelino

et al. 2016

ACS Med. Chem. Lett.

Self Cite

View full text Add to dashboard Cite

show abstract

“…S1A; ref. 27). However, a key difference of MMAF is the presence of a N-methylated a,a-dimethyl amino acid (Aib) that replaces the N-methyl valine on the N-terminus of MMAF.…”

Section: Linker/payload Lp2mentioning

confidence: 99%

“…To test this hypothesis, we humanized L6, generating antibody v1.10; L6 and v1.10, unlike 8G4, cross-react with cynomolgus monkey TM4SF1 (10). We then armed v1.10 with LP2 (chemical name mc-3377), a synthetic analog of dolastatin-10 (26); dolastatin-10 and synthetic analogs, termed auristatins, inhibit tubulin polymerization, and ultimately induce G 2 -M cell-cycle arrest and cell death at low picomolar intracellular concentrations (27). Tubulin inhibitors have been extensively investigated as vascular targeting agents and seem to be preferentially toxic against tumor and tumor vascular endothelial cells with high proliferation rates, while sparing the nondividing endothelial cells of normal tissues (28)(29)(30).…”

Section: Introductionmentioning

confidence: 99%

Novel Anti-TM4SF1 Antibody–Drug Conjugates with Activity against Tumor Cells and Tumor Vasculature

Visintin

Knowlton

Tyminski

et al. 2015

Molecular Cancer Therapeutics

Self Cite

View full text Add to dashboard Cite

Antibody-drug conjugates (ADC) represent a promising therapeutic modality for managing cancer. Here, we report a novel humanized ADC that targets the tetraspanin-like protein TM4SF1. TM4SF1 is highly expressed on the plasma membranes of many human cancer cells and also on the endothelial cells lining tumor blood vessels. TM4SF1 is internalized upon interaction with antibodies. We hypothesized that an ADC against TM4SF1 would inhibit cancer growth directly by killing cancer cells and indirectly by attacking the tumor vasculature. We generated a humanized anti-human TM4SF1 monoclonal antibody, v1.10, and armed it with an auristatin cytotoxic agent LP2 (chemical name mc-3377). v1.10-LP2 selectively killed cultured human tumor cell lines and human endothelial cells that express TM4SF1. Acting as a single agent, v1.10-LP2 induced complete regression of several TM4SF1-expressing tumor xenografts in nude mice, including non-small cell lung cancer and pancreas, prostate, and colon cancers. As v1.10 did not react with mouse TM4SF1, it could not target the mouse tumor vasculature. Therefore, we generated a surrogate antimouse TM4SF1 antibody, 2A7A, and conjugated it to LP2. At 3 mpk, 2A7A-LP2 regressed several tumor xenografts without noticeable toxicity. Combination therapy with v1.10-LP2 and 2A7A-LP2 together was more effective than either ADC alone. These data provide proof-of-concept that TM4SF1-targeting ADCs have potential as anticancer agents with dual action against tumor cells and the tumor vasculature. Such agents could offer exceptional therapeutic value and warrant further investigation.

show abstract

The Design and Development of Antibody–Drug Conjugates (ADCs) for the Treatment of Cancer

Tumey

2021

Burger's Medicinal Chemistry and Drug Discovery

View full text Add to dashboard Cite

Over the past 10 years, antibody–drug conjugates (ADCs) have rapidly become an important player in the oncology therapeutic space. ADCs consist of three components: (i) A potently cytotoxic drug; (ii) An antibody that is designed to deliver the drug to specific antigen‐expressing cells; and (iii) A linker that holds these two components together but is rapidly cleaved by cancer cells. Tremendous technical advances have been made in the ADC field over the past 15 years that have culminated in the FDA approval of six ADCs and the clinical evaluation (currently) of nearly 100 ADCs. This article provides an overview of the history of ADCs and highlighted important developments in the selection of antigens, design of the linker, selection of conjugation chemistry, and the design of the payload itself. We will focus on promising preclinical strategies that are working their way toward clinical evaluation.

show abstract

Discovery of Cytotoxic Dolastatin 10 Analogues with N-Terminal Modifications

Cited by 120 publications

References 37 publications

Design, Synthesis, and Cytotoxic Evaluation of Novel Tubulysin Analogues as ADC Payloads

Design, Synthesis, and Cytotoxic Evaluation of Novel Tubulysin Analogues as ADC Payloads

Novel Anti-TM4SF1 Antibody–Drug Conjugates with Activity against Tumor Cells and Tumor Vasculature

The Design and Development of Antibody–Drug Conjugates (ADCs) for the Treatment of Cancer

Contact Info

Product

Resources

About