A subset of HOX genes negatively correlates with HOX/PBX inhibitor target gene expression and is associated with apoptosis, DNA repair, and metabolism in prostate cancer

Lists

Morgan, Richard ORCID: https://orcid.org/0000-0002-8721-4479, Smith, Christopher and Pandha, Hardev (2025) A subset of HOX genes negatively correlates with HOX/PBX inhibitor target gene expression and is associated with apoptosis, DNA repair, and metabolism in prostate cancer. Genes, 16 (7). pp. 1-12.

Preview

PDF (PDF/A)
A subset of HOX genes negatively correlates_MorganR_accessible.pdf - Draft Version
Available under License Creative Commons Attribution.
Download (5MB) | Preview

Official URL: https://www.mdpi.com/2073-4425/16/7/824

Abstract

Background/Objectives: The HOX genes encode a family of homeodomain-containing transcription factors that have important roles in defining cell and tissue identity in embryonic development, but which also show deregulated expression in many cancers and have been shown to have pro-oncogenic roles. Due to their functionally redundant nature, strategies to target HOX protein function in cancer have focused on their interaction with their PBX cofactor using competitive peptides such as HXR9. HOX/PBX inhibition triggers apoptosis through a sudden increase in target gene expression, including Fos, DUSP1, and ATF3, which are otherwise repressed by HOX/PBX binding.

Methods: We analyzed publicly available transcriptomic data in the R2 platform.

Results: We show that a specific subgroup of HOX genes is negatively correlated with Fos, DUSP1, and ATF3 expression
in prostate cancer, and that this subgroup also shows a strong positive corelation with pathways that support tumour growth, most notably DNA repair and aminoacyl tRNA biosynthesis, and a negative correlation with genes that promote cell adhesion and prevent motility. In addition, this set of HOX genes strongly correlates with patient age, reflecting a previously identified progressive loss of regulation of HOX expression in normal peripheral blood cells.

Conclusions: Our findings indicate these HOX genes may have pro-oncogenicfunctions in prostate cancer.

Item Type:	Article
Identifier:	10.3390/genes16070824
Keywords:	HOX; PBX; DUSP1; ATF3; HXR9; ageing
Depositing User:	Richard Morgan
Date Deposited:	22 Jul 2025 07:49
Last Modified:	22 Jul 2025 08:00
URI:	https://repository.uwl.ac.uk/id/eprint/13889

Downloads

Downloads per month over past year

Actions (login required)

View Item

References

1. Mallo, M.; Wellik, D.M.; Deschamps, J. Hox Genes and Regional Patterning of the Vertebrate Body Plan. Dev. Biol. 2010, 344, 7–15.

2. Alharbi, R.A.; Pettengell, R.; Pandha, H.S.; Morgan, R. The Role of HOX Genes in Normal Hematopoiesis and Acute Leukemia.
Leukemia 2013, 27, 1000–1008.

3. Morgan, R.; Hunter, K.; Pandha, H.S. Downstream of the HOX Genes: Explaining Conflicting Tumour Suppressor and Oncogenic
Functions in Cancer. Int. J. Cancer 2022, 150, 1919–1932.
4. Drake, K.A.; Adam, M.; Mahoney, R.; Potter, S.S. Disruption of Hox9,10,11 Function Results in Cellular Level Lineage Infidelity in
the Kidney. Sci. Rep. 2018, 8, 6306.
5. Morgan, R.; El-Tanani, M.; Hunter, K.D.; Harrington, K.J.; Pandha, H.S. Targeting HOX/PBX Dimers in Cancer. Oncotarget 2017, 8,
32322–32331.
6. Morgan, R.; Pirard, P.M.; Shears, L.; Sohal, J.; Pettengell, R.; Pandha, H.S. Antagonism of HOX/PBX Dimer Formation Blocks the
in Vivo Proliferation of Melanoma. Cancer Res. 2007, 67, 5806–5813.
7. Kelly, Z.L.; Michael, A.; Butler-Manuel, S.; Pandha, H.S.; Morgan, R.G. HOX Genes in Ovarian Cancer. J. Ovarian Res. 2011, 4, 16.

8. Morgan, R.; Boxall, A.; Harrington, K.J.; Simpson, G.R.; Michael, A.; Pandha, H.S. Targeting HOX Transcription Factors in Prostate
Cancer. BMC Urol. 2014, 14, 17.
9. Morgan, R.; Simpson, G.; Gray, S.; Gillett, C.; Tabi, Z.; Spicer, J.; Harrington, K.J.; Pandha, H.S. HOX Transcription Factors are
Potential Targets and Markers in Malignant Mesothelioma. BMC Cancer 2016, 16, 85–87.
10. Errico, M.C.; Felicetti, F.; Bottero, L.; Mattia, G.; Boe, A.; Felli, N.; Petrini, M.; Bellenghi, M.; Pandha, H.S.; Calvaruso, M.; et al.
The Abrogation of the HOXB7/PBX2 Complex Induces Apoptosis in Melanoma through the miR-221&222-C-FOS Pathway. Int. J.
Cancer 2013, 133, 879–892.
11. Kasibhatla, S.; Brunner, T.; Genestier, L.; Echeverri, F.; Mahboubi, A.; Green, D.R. DNA Damaging Agents Induce Expression of
Fas Ligand and Subsequent Apoptosis in T Lymphocytes Via the Activation of NF-Kappa B and AP-1. Mol. Cell 1998, 1, 543–551.

12. Yan, C.; Lu, D.; Hai, T.; Boyd, D.D. Activating Transcription Factor 3, a Stress Sensor, Activates p53 by Blocking its Ubiquitination.
EMBO J. 2005, 24, 2425–2435.
13. Shen, J.; Zhang, Y.; Yu, H.; Shen, B.; Liang, Y.; Jin, R.; Liu, X.; Shi, L.; Cai, X. Role of DUSP1/MKP1 in Tumorigenesis, Tumor
Progression and Therapy. Cancer Med. 2016, 5, 2061–2068.
14. Ben, S.; Ding, Z.; Xin, J.; Li, F.; Cheng, Y.; Chen, S.; Fan, L.; Zhang, Q.; Li, S.; Du, M.; et al. piRNA PROPER Suppresses DUSP1
Translation by Targeting N(6)-Methyladenosine-Mediated RNA Circularization to Promote Oncogenesis of Prostate Cancer. Adv.
Sci. (Weinh) 2024, 11, e2402954.
15. Hu, B.; Wang, C.; Wu, Y.; Han, C.; Liu, J.; Chen, R.; Wang, T. Revealing the Mechanism of Ethyl Acetate Extracts of Semen
Impatientis Against Prostate Cancer Based on Network Pharmacology and Transcriptomics. J. Ethnopharmacol. 2024, 330, 118228.

16. Ross-Adams, H.; Lamb, A.D.; Dunning, M.J.; Halim, S.; Lindberg, J.; Massie, C.M.; Egevad, L.A.; Russell, R.; Ramos-Montoya, A.;
Vowler, S.L.; et al. Integration of Copy Number and Transcriptomics Provides Risk Stratification in Prostate Cancer: A Discovery
and Validation Cohort Study. EBioMedicine 2015, 2, 1133–1144.
17. Taylor, B.S.; Schultz, N.; Hieronymus, H.; Gopalan, A.; Xiao, Y.; Carver, B.S.; Arora, V.K.; Kaushik, P.; Cerami, E.; Reva, B.; et al.
Integrative Genomic Profiling of Human Prostate Cancer. Cancer Cell 2010, 18, 11–22.
18. McFarland, J.M.; Ho, Z.V.; Kugener, G.; Dempster, J.M.; Montgomery, P.G.; Bryan, J.G.; Krill-Burger, J.M.; Green, T.M.; Vazquez,
F.; Boehm, J.S.; et al. Improved Estimation of Cancer Dependencies from Large-Scale RNAi Screens using Model-Based
Normalization and Data Integration. Nat. Commun. 2018, 9, 4610–4615.
19. Wu, X.; Chen, H.; Parker, B.; Rubin, E.; Zhu, T.; Lee, J.S.; Argani, P.; Sukumar, S. HOXB7, a Homeodomain Protein, is Overexpressed
in Breast Cancer and Confers Epithelial-Mesenchymal Transition. Cancer Res. 2006, 66, 9527–9534.
20. Wang, T.; Lin, F.; Sun, X.; Jiang, L.; Mao, R.; Zhou, S.; Shang, W.; Bi, R.; Lu, F.; Li, S. HOXB8 Enhances the Proliferation and
Metastasis of Colorectal Cancer Cells by Promoting EMT Via STAT3 Activation. Cancer Cell Int. 2019, 19, 3–6, eCollection 2019.

21. Dai, B.; Yang, Z.; Deng, P.; Chen, Y.; He, Z.; Yang, X.; Zhang, S.; Wu, H.; Ren, Z. HOXC10 Promotes Migration and Invasion Via
the WNT-EMT Signaling Pathway in Oral Squamous Cell Carcinoma. J. Cancer 2019, 10, 4540–4551.
22. Xiong, W.; Zhou, Q.; Liu, G.; Liu, X.; Li, X. Homeodomain-Containing Gene 10 Inhibits Cell Apoptosis and Promotes Cell Invasion
and Migration in Osteosarcoma Cell Lines. Tumour Biol. 2017, 39, 1010428317697566.
23. Ohta, H.; Hamada, J.; Tada, M.; Aoyama, T.; Furuuchi, K.; Takahashi, Y.; Totsuka, Y.; Moriuchi, T. HOXD3-Overexpression
Increases Integrin Alpha V Beta 3 Expression and Deprives E-Cadherin while it Enhances Cell Motility in A549 Cells. Clin. Exp.
Metastasis 2006, 23, 381–390.
24. Zhan, J.; Niu, M.; Wang, P.; Zhu, X.; Li, S.; Song, J.; He, H.; Wang, Y.; Xue, L.; Fang, W.; et al. Elevated HOXB9 Expression
Promotes Differentiation and Predicts a Favourable Outcome in Colon Adenocarcinoma Patients. Br. J. Cancer 2014, 111, 883–893.

25. Zhang, J.; Yang, M.; Li, D.; Zhu, S.; Zou, J.; Xu, S.; Wang, Y.; Shi, J.; Li, Y. Homeobox C8 is a Transcriptional Repressor of
E-Cadherin Gene Expression in Non-Small Cell Lung Cancer. Int. J. Biochem. Cell Biol. 2019, 114, 105557.

Taniguchi, Y.; Tanaka, O.; Sekiguchi, M.; Takekoshi, S.; Tsukamoto, H.; Kimura, M.; Imai, K.; Inoko, H. Enforced Expression of the
Transcription Factor HOXD3 Under the Control of the Wnt1 Regulatory Element Modulates Cell Adhesion Properties in the
Developing Mouse Neural Tube. J. Anat. 2011, 219, 589–600.
27. Lin, Z.; Hu, Y.; Lin, R.; Ye, H. The Effect of Overexpression of the HOXD10 Gene on the Malignant Proliferation, Invasion, and
Tumor Formation of Pancreatic Cancer Cell PANC-1. Gland. Surg. 2020, 9, 385–391.
28. Rubin, E.; Wu, X.; Zhu, T.; Cheung, J.C.Y.; Chen, H.; Lorincz, A.; Pandita, R.K.; Sharma, G.G.; Ha, H.C.; Gasson, J.; et al. A Role for
the HOXB7 Homeodomain Protein in DNA Repair. Cancer Res. 2007, 67, 1527–1535.
29. Chiba, N.; Comaills, V.; Shiotani, B.; Takahashi, F.; Shimada, T.; Tajima, K.; Winokur, D.; Hayashida, T.; Willers, H.; Brachtel, E.;
et al. Homeobox B9 Induces Epithelial-to-Mesenchymal Transition-Associated Radioresistance by Accelerating DNA Damage
Responses. Proc. Natl. Acad. Sci. USA 2012, 109, 2760–2765.
30. Kim, J.W.; Kim, J.Y.; Kim, J.E.; Kim, S.; Chung, H.; Park, C. HOXA10 is Associated with Temozolomide Resistance through
Regulation of the Homologous Recombinant DNA Repair Pathway in Glioblastoma Cell Lines. Genes Cancer 2014, 5, 165–174.

31. Morgan, R.; Begum, R.; Theti, D.; Chansa, M.; Pettengell, R.; Sohal, J. HOXA9 Expression Increases with Age in Human
Haemopoietic Cells. Leuk. Res. 2005, 29, 1221–1222.
32. Feiner, L.; Tierling, S.; Hollander, S.; Glanemann, M.; Rubie, C. An Aging and p53 Related Marker: HOXA5 Promoter Methylation
Negatively Correlates with mRNA and Protein Expression in Old Age. Aging 2021, 13, 4831–4849.
33. Turner, D.C.; Gorski, P.P.; Maasar, M.F.; Seaborne, R.A.; Baumert, P.; Brown, A.D.; Kitchen, M.O.; Erskine, R.M.; Dos-Remedios, I.;
Voisin, S.; et al. DNA Methylation Across the Genome in Aged Human Skeletal Muscle Tissue and Muscle-Derived Cells: The
Role of HOX Genes and Physical Activity. Sci. Rep. 2020, 10, 15360. [PubMed

Tools

CORE (COnnecting REpositories)

The University of West London

A subset of HOX genes negatively correlates with HOX/PBX inhibitor target gene expression and is associated with apoptosis, DNA repair, and metabolism in prostate cancer

Abstract

Downloads

Actions (login required)

Menu