FKBPL and its peptide derivatives inhibit endocrine therapy resistant cancer stem cells and breast cancer metastasis by downregulating DLL4 and Notch4

Lana McClements; Stephanie Annett; Anita Yakkundi; Martin O'Rourke; Andrea Valentine; Nermeen Moustafa; Abdelrahim Alqudah; Bruno M Simões; Fiona Furlong; Amy Short; Stuart A McIntosh; Helen O McCarthy; Robert B Clarke; Tracy Robson

doi:10.1186/s12885-019-5500-0

FKBPL and its peptide derivatives inhibit endocrine therapy resistant cancer stem cells and breast cancer metastasis by downregulating DLL4 and Notch4

BMC Cancer. 2019 Apr 11;19(1):351. doi: 10.1186/s12885-019-5500-0.

Authors

Lana McClements^{1

2

3}, Stephanie Annett^{2

4}, Anita Yakkundi², Martin O'Rourke^{2

5}, Andrea Valentine^{2

5}, Nermeen Moustafa², Abdelrahim Alqudah^{1

6}, Bruno M Simões⁷, Fiona Furlong², Amy Short², Stuart A McIntosh⁸, Helen O McCarthy², Robert B Clarke⁷, Tracy Robson^{9

10}

Affiliations

¹ Centre for Experimental Medicine, School of Medicine, Dentistry and Biomedical Sciences, Queen's University Belfast, Belfast, UK.
² School of Pharmacy, Queen's University Belfast, Belfast, UK.
³ The School of Life Sciences, University of Technology Sydney, Sydney, Australia.
⁴ Department of Molecular and Cellular Therapeutics, Irish Centre for Vascular Biology, Royal College of Surgeons in Ireland, RCSI, Dublin, Ireland.
⁵ Charles River Labs, 8-9 Spire Green Centre, Essex, Harlow, CM19 5TR, UK.
⁶ School of Pharmacy, Hashemite University, Amman, Jordan.
⁷ Manchester Breast Centre, Division of Cancer Sciences, University of Manchester, Oglesby Cancer Research Building, Manchester, UK.
⁸ Centre for Cancer Research and Cell Biology, Queen's University Belfast and Breast Surgery Department, Belfast City Hospital, Belfast, UK.
⁹ School of Pharmacy, Queen's University Belfast, Belfast, UK. tracyrobson@rcsi.ie.
¹⁰ Department of Molecular and Cellular Therapeutics, Irish Centre for Vascular Biology, Royal College of Surgeons in Ireland, RCSI, Dublin, Ireland. tracyrobson@rcsi.ie.

Abstract

Background: Optimising breast cancer treatment remains a challenge. Resistance to therapy is a major problem in both ER- and ER+ breast cancer. Tumour recurrence after chemotherapy and/or targeted therapy leads to more aggressive tumours with enhanced metastatic ability. Self-renewing cancer stem cells (CSCs) have been implicated in treatment resistance, recurrence and the development of metastatic disease.

Methods: In this study, we utilised in vitro, in vivo and ex vivo breast cancer models using ER+ MCF-7 and ER- MDA-MB-231 cells, as well as solid and metastatic breast cancer patient samples, to interrogate the effects of FKBPL and its peptide therapeutics on metastasis, endocrine therapy resistant CSCs and DLL4 and Notch4 expression. The effects of FKBPL overexpression or peptide treatment were assessed using a t-test or one-way ANOVA with Dunnett's multiple comparison test.

Results: We demonstrated that FKBPL overexpression or treatment with FKBPL-based therapeutics (AD-01, pre-clinical peptide /ALM201, clinical peptide) inhibit i) CSCs in both ER+ and ER- breast cancer, ii) cancer metastasis in a triple negative breast cancer metastasis model and iii) endocrine therapy resistant CSCs in ER+ breast cancer, via modulation of the DLL4 and Notch4 protein and/or mRNA expression. AD-01 was effective at reducing triple negative MDA-MB-231 breast cancer cell migration (n ≥ 3, p < 0.05) and invasion (n ≥ 3, p < 0.001) and this was translated in vivo where AD-01 inhibited breast cancer metastasis in MDA-MB-231-lucD3H1 in vivo model (p < 0.05). In ER+ MCF-7 cells and primary breast tumour samples, we demonstrated that ALM201 inhibits endocrine therapy resistant mammospheres, representative of CSC content (n ≥ 3, p < 0.05). Whilst an in vivo limiting dilution assay, using SCID mice, demonstrated that ALM201 alone or in combination with tamoxifen was very effective at delaying tumour recurrence by 12 (p < 0.05) or 21 days (p < 0.001), respectively, by reducing the number of CSCs. The potential mechanism of action, in addition to CD44, involves downregulation of DLL4 and Notch4.

Conclusion: This study demonstrates, for the first time, the pre-clinical activity of novel systemic anti-cancer therapeutic peptides, ALM201 and AD-01, in the metastatic setting, and highlights their impact on endocrine therapy resistant CSCs; both areas of unmet clinical need.

Keywords: AD-01; ALM201; Breast cancer stem cells; DLL4; Endocrine therapy; Estrogen receptor; FKBPL; Letrozole; Metastasis; Notch4; Tamoxifen; Triple negative breast cancer.

MeSH terms

Adaptor Proteins, Signal Transducing
Animals
Antineoplastic Agents, Hormonal / pharmacology
Antineoplastic Agents, Hormonal / therapeutic use
Antineoplastic Combined Chemotherapy Protocols / pharmacology*
Antineoplastic Combined Chemotherapy Protocols / therapeutic use
Breast / pathology
Breast Neoplasms / drug therapy*
Breast Neoplasms / pathology
Calcium-Binding Proteins
Cell Line, Tumor
Down-Regulation / drug effects
Drug Resistance, Neoplasm
Female
Gene Expression Regulation, Neoplastic / drug effects
Humans
Immunophilins / pharmacology*
Immunophilins / therapeutic use
Intercellular Signaling Peptides and Proteins / metabolism
Mice
Mice, SCID
Neoplasm Recurrence, Local / prevention & control
Neoplastic Stem Cells / drug effects*
Neoplastic Stem Cells / pathology
Peptides / pharmacology*
Peptides / therapeutic use
Receptor, Notch4 / metabolism
Signal Transduction / drug effects
Tacrolimus Binding Proteins
Tamoxifen / pharmacology
Tamoxifen / therapeutic use
Treatment Outcome
Xenograft Model Antitumor Assays

Substances

Adaptor Proteins, Signal Transducing
Antineoplastic Agents, Hormonal
Calcium-Binding Proteins
DLL4 protein, human
FKBPL protein, human
Intercellular Signaling Peptides and Proteins
NOTCH4 protein, human
Peptides
Receptor, Notch4
Tamoxifen
Tacrolimus Binding Proteins
Immunophilins

Abstract

MeSH terms

Substances

Grants and funding