Abstract
The potential for basic research to uncover the inner workings of regenerative processes and produce meaningful medical therapies has inspired scientists, clinicians, and patients for hundreds of years. Decades of studies using a handful of highly regenerative model organisms have significantly advanced our knowledge of key cell types and molecular pathways involved in regeneration. However, many questions remain about how regenerative processes unfold in regeneration-competent species, how they are curtailed in non-regenerative organisms, and how they might be induced (or restored) in humans. Recent technological advances in genomics, molecular biology, computer science, bioengineering, and stem cell research hold promise to collectively provide new experimental evidence for how different organisms accomplish the process of regeneration. In theory, this new evidence should inform the design of new clinical approaches for regenerative medicine. A deeper understanding of how tissues and organs regenerate will also undoubtedly impact many adjacent scientific fields. To best apply and adapt these new technologies in ways that break long-standing barriers and answer critical questions about regeneration, we must combine the deep knowledge of developmental and evolutionary biologists with the hard-earned expertise of scientists in mechanistic and technical fields. To this end, this perspective is based on conversations from a workshop we organized at the Banbury Center, during which a diverse cross-section of the regeneration research community and experts in various technologies discussed enduring questions in regenerative biology. Here, we share the questions this group identified as significant and unanswered, i.e., known unknowns. We also describe the obstacles limiting our progress in answering these questions and how expanding the number and diversity of organisms used in regeneration research is essential for deepening our understanding of regenerative capacity. Finally, we propose that investigating these problems collaboratively across a diverse network of researchers has the potential to advance our field and produce unexpected insights into important questions in related areas of biology and medicine.
| Original language | English |
|---|---|
| Article number | 1139 |
| Journal | Communications Biology |
| Volume | 6 |
| Issue number | 1 |
| DOIs |
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| State | Published - Dec 2023 |
Bibliographical note
Publisher Copyright:© 2023, The Author(s).
Funding
We thank the Banbury Center for providing an amazing atmosphere for our vintage workshop experiment and, specifically, Rebecca Leshan for her backing and encouragement. We acknowledge Genentech and The Cold Spring Harbor Laboratory Corporate Sponsor Program for supporting the workshop. In addition to input from all attendees of the Banbury Workshop that informed this perspective article, we thank Francesca Mariani for significant editorial input. In a better-designed version of itself, academia would encourage the type of collaborative effort that went into this paper to be formally recognized with co-authorship. While nothing precludes this arrangement, how current conflict of interest (COI) declarations impact review procedures for grant proposals and promotion panels created unavoidable conflicts among participants to be co-authors. Lastly, we would like to thank John (Jack) Allen and Kelly Ross for their perspectives on an early version of this paper. Research in A.W. Seifert’s lab is funded by NIH grants R01 AR070313, R21 DE028070, the ASAP Collaborative Research Network through the Michael J. Fox Foundation, and DOD CDMRP 6W81XWH2110503. Research in R.M. Zayas’s lab is funded by NIH grant R01 GM135657. Research in E.M. Duncan’s lab is funded through NIH grant R35 GM142679.
| Funders | Funder number |
|---|---|
| Cold Spring Harbor Laboratory Corporate Sponsor Program | |
| DOD CDMRP | R01 GM135657, R35 GM142679, 6W81XWH2110503 |
| National Institutes of Health (NIH) | R01 AR070313, R21 DE028070 |
| National Institutes of Health (NIH) | |
| The Michael J Fox Foundation for Parkinson's Research | |
| Genentech Incorporated |
ASJC Scopus subject areas
- Medicine (miscellaneous)
- General Biochemistry, Genetics and Molecular Biology
- General Agricultural and Biological Sciences