Miss Sophie Wiszniak

Senior Research Fellow

Centre for Cancer Biology

College of Health

Eligible to supervise Masters and PhD - email supervisor to discuss availability.

Dr. Sophie Wiszniak leads the Neural Crest and Cardiac Development Group at the Centre for Cancer Biology.
Her team studies how tissue-tissue interactions orchestrate many processes throughout embryonic development, with a particular focus on neural crest cell interactions with the cardiovascular system. Her team studies the role of neural crest cells in directing correct development of the heart and other associated structures, which has important implications for understanding the cellular mechanisms underpinning congenital heart disease and other birth defects. Her team also studies the role of blood vessels, and in particular blood vessel-derived 'angiocrine' factors in controlling tissue development and function in embryogenesis and disease.

Neural crest cells as modulators of Wnt signalling in congenital heart disease:

Using genetic mouse models and RNA sequencing approaches, we have discovered that neural crest cells signal to cardiac progenitor cells during heart development to influence their differentiation potential. Current work is focussed on identifying the molecular signalling pathways responsible, with a major candidate being the Wnt signalling pathway. We are using embryo analysis, histology, advanced imaging, and stem-cell culture approaches to address how neural crest cells are influencing heart development, and how this can go wrong to cause congenital heart defects.

Mechanistic roles for neural crest cells in development of pulmonary stenosis:

Pulmonary stenosis is the narrowing of the pulmonary artery and valve, which normally provides the pathway for blood to leave the heart and flow to the lungs. Pulmonary stenosis is one of the most common congenital heart defects. We have discovered that Notch signalling ligands on cardiac neural crest cells signal to other cell types in the developing heart to influence the size and shape of the pulmonary valve and branching arteries. We are currently using state-of-the-art single cell RNA sequencing approaches to interrogate which cells are responding to Notch signalling, and the downstream pathways that can lead to abnormal pulmonary valve development.

Date	Position	Institution name
2025 - ongoing	Senior Research Fellow	University of South Australia
2017 - 2024	Research Fellow	University of South Australia
2011 - 2016	Research Associate	SA Pathology

Date	Institution name	Country	Title
2007 - 2011	University of Adelaide	Australia	Doctor of Philosophy

Year	Citation
2023	Voges, H. K., Foster, S. R., Reynolds, L., Parker, B. L., Devilée, L., Quaife-Ryan, G. A., . . . Hudson, J. E. (2023). Vascular cells improve functionality of human cardiac organoids. Cell Reports, 42(5), 22 pages. DOI Scopus77 WoS79 Europe PMC78
2023	Bishop, D., Schwarz, Q., & Wiszniak, S. (2023). Endothelial-derived angiocrine factors as instructors of embryonic development. Frontiers in Cell and Developmental Biology, 11(1172114), 19 pages. DOI Scopus12 WoS11 Europe PMC12
2022	Lohraseb, I., McCarthy, P., Secker, G., Marchant, C., Wu, J., Ali, N., . . . Schwarz, Q. (2022). Global ubiquitinome profiling identifies NEDD4 as a regulator of Profilin 1 and actin remodelling in neural crest cells. Nature Communications, 13(1), 1-18. DOI Scopus5 WoS6 Europe PMC7
2021	Ofek, S., Wiszniak, S., Kagan, S., Tondl, M., Schwarz, Q., & Kalcheim, C. (2021). Notch signaling is a critical initiator of roof plate formation as revealed by the use of RNA profiling of the dorsal neural tube. BMC Biology, 19(1, article no. 84), 1-23. DOI Scopus10 WoS8 Europe PMC11
2021	Wiszniak, S., & Schwarz, Q. (2021). Exploring the intracrine functions of vegf-a. Biomolecules, 11(1), 1-13. DOI Scopus83 WoS76 Europe PMC66
2020	Marchant, C., Anderson, P., Schwarz, Q., & Wiszniak, S. (2020). Vessel-derived angiocrine IGF1 promotes Meckel's cartilage proliferation to drive jaw growth during embryogenesis. Development, 147(11), 1-8. DOI Scopus16 WoS14 Europe PMC13
2020	Marchant, C., Anderson, P., Schwarz, Q., & Wiszniak, S. (2020). Vessel-derived angiocrine IGF-1 promotes Meckel's cartilage proliferation to drive jaw growth during embryogenesis. Development. DOI
2019	Wiszniak, S., & Schwarz, Q. (2019). Notch signalling defines dorsal root ganglia neuroglial fate choice during early neural crest cell migration. BMC neuroscience, 20(1, article no. 21), 1-13. DOI Scopus16 WoS13 Europe PMC13
2019	Wiszniak, S. (2019). Ex vivo culture and manipulation of mouse neural crest cells from primary embryonic tissue explants. Methods in molecular biology, 1976, 83-95. DOI Scopus1 Europe PMC1
2016	Wiszniak, S., Harvey, N., & Schwarz, Q. (2016). Cell autonomous roles of Nedd4 in craniofacial bone formation. Developmental Biology, 410(1), 98-107. DOI Scopus22 WoS22 Europe PMC19
2015	Wiszniak, S., Mackenzie, F. E., Anderson, P., Kabbara, S., Ruhrberg, C., & Schwarz, Q. (2015). Neural crest cell-derived VEGF promotes embryonic jaw extension. Proceedings of the National Academy of Sciences of the United States of America, 112(19), 6086-6091. DOI Scopus53 WoS50 Europe PMC49
2015	Wiszniak, S., Scherer, M., Ramshaw, H., & Schwarz, Q. (2015). Neuropilin-2 genomic elements drive cre recombinase expression in primitive blood, vascular and neuronal lineages. Genesis, 53(11), 709-717. DOI Scopus4 WoS4 Europe PMC3
2015	Hare, L. M., Schwarz, Q., Wiszniak, S., Gurung, R., Montgomery, K. G., Mitchell, C. A., & Phillips, W. A. (2015). Heterozygous expression of the oncogenic Pik3caH1047R mutation during murine development results in fatal embryonic and extraembryonic defects. Developmental biology, 404(1), 14-26. DOI Scopus35 WoS35 Europe PMC34
2014	Lumb, R., Wiszniak, S., Kabbara, S., Scherer, M., Harvey, N., & Schwarz, Q. (2014). Neuropilins define distinct populations of neural crest cells. Neural Development, 9(1), 24-1-24-14. DOI Scopus21 WoS20 Europe PMC21
2013	Ramshaw, H., Xu, X., Jaehne, E., McCarthy, P., Greenberg, Z., Saleh, E., . . . Schwarz, Q. (2013). Locomotor hyperactivity in 14-3-3ζ KO mice is associated with dopamine transporter dysfunction. Translational Psychiatry, 3(e327), 1-10. DOI Scopus27 WoS26 Europe PMC24
2013	Wiszniak, S., Kabbara, S., Lumb, R., Scherer, M., Secker, G., Harvey, N., . . . Schwarz, Q. (2013). The ubiquitin ligase Nedd4 regulates craniofacial development by promoting cranial neural crest cell survival and stem-cell like properties. Developmental Biology, 383(2), 186-200. DOI Scopus25 WoS28 Europe PMC29
2013	Wiszniak, S., Lumb, R., Kabbara, S., Scherer, M., & Schwarz, Q. (2013). Li-gazing at the crest: Modulation of the neural crest by the ubiquitin pathway. The international journal of biochemistry and cell biology, 45(6), 1087-1091. DOI Scopus5 WoS4 Europe PMC4
2011	Wiszniak, S., Dredge, B., & Jensen, K. (2011). HuB (elavl2) mRNA is restricted to the germ cells by post-transcriptional mechanisms including stabilisation of the message by DAZL. PLoS One, 6(6), e20773-1-e20773-9. DOI Scopus23 WoS21 Europe PMC20

Year	Citation
2022	Wiszniak, S., & Schwarz, Q. (2022). Mandible explant assay for the analysis of Meckel's cartilage development. In S. Dworkin (Ed.), Source details - Title: Craniofacial Development: Methods and Protocols (Vol. 2403, pp. 235-247). US: Humana Press. DOI Scopus1 Europe PMC1
2014	Wiszniak, S., & Schwarz, Q. (2014). Neural Crest Cells in Vascular Development. In P. Trainor (Ed.), Neural Crest Cells: Evolution, Development and Disease (pp. 313-333). US: Elsevier. DOI Scopus6

Year	Citation
2017	Wiszniak, S., & Schwarz, Q. (2017). Neural crest cell and second heart field interactions orchestrate cardiac outflow tract development. In MECHANISMS OF DEVELOPMENT Vol. 145 (pp. S154-S155). SINGAPORE, Natil Univ Singapore, Singapore: ELSEVIER SCIENCE BV. DOI WoS1

Year	Citation
2009	Wiszniak, S., & Jensen, K. (2009). Post-transcriptional regulation of the HuB 3UTR restricts expression of the HuB RNA-binding protein to the germ cells of zebrafish. Poster session presented at the meeting of Poster Abstracts from the 16th Annual Conference of the International Society of Development Biologists, as published in Mechanisms of Development. Edinburgh, Scotland: Elsevier. DOI

Year	Citation
2025	Wiszniak, S., Alankarage, D., Lohraseb, I., Marchant, C., Secker, G., Parker, W., . . . Schwarz, Q. (2025). Neural crest cell derived DKK1 modulates Wnt signalling in the second heart field to orchestrate cardiac outflow tract development. DOI

Tom Simpson Trust - Amira Software, National Heart Foundation of Australia (South Australian Division), 15/12/2023 - 14/12/2024
Defining the role of IGF-1 as a novel angiocrine factor in the development and treament of common craniofacial disorders, NHMRC - Project Grant, 01/01/2018 - 31/12/2021
Novel roles for neural crest cells in cardiac morphogenesis, NHMRC - Project Grant, 01/01/2019 - 31/12/2021
Tom Simpson Trust Equipment Grant - rotating bottle culture unit', National Heart Foundation of Australia (South Australian Division), 02/01/2017 - 30/11/2017

Date	Role	Research Topic	Program	Degree Type	Student Load	Student Name
2025	Principal Supervisor	-	-	Master	Full Time	Ms Briarn Elizabeth Dixon
2025	Co-Supervisor	-	Doctor of Philosophy	Doctorate	Full Time	Mr Rafaqat Hussain Haidari
2024	Principal Supervisor	-	-	Master	Full Time	Miss Jasmine Ella Hartmann

Date	Role	Committee	Institution	Country
2025 - ongoing	Member	SA Cardiovascular Research Network	National Heart Foundation of Australia	Australia

Position: Senior Research Fellow
Email: sophie.wiszniak@adelaide.edu.au

Miss Sophie Wiszniak

Miss Sophie Wiszniak

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Miss Sophie Wiszniak

Miss Sophie Wiszniak

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