KANAZAWA, Japan, Oct. 3, 2024
/PRNewswire/ -- Researchers at Nano Life Science Institute
(WPI-NanoLSI), Kanazawa University, demonstrate
how morphogens combined with cell adhesion can
generate tissue domains with a
sharp boundary in an in
vitro model system.
Figure 1
https://nanolsi.kanazawa-u.ac.jp/wp/wp-content/uploads/Toda_Fig.-1.jpg
Caption Figure 1: How does the morphogen gradient
regulate multicellular patterning?
Recent advances that have enabled the growth of tissue cultures
into organoids and embryoids have heightened interest as
to how tissue growth is controlled during the natural processes of
embryo development. It is known that the diffusion of signaling
molecules called morphogens directs patterned tissue growth but
what has been harder to understand is how the gradient of
morphogens from this diffusion can lead to sharply defined domains
in the resulting tissue (Fig. 1). Now Satoshi Toda at Kanazawa University NanoLSI
(currently Osaka University,
Institute for Protein Research), alongside Kosuke Mizuno at NanoLSI and Tsuyoshi Hirashima at the National University of Singapore, demonstrate a
simple model system – SYnthetic
Morphogen system for Pattern Logic Exploration using 3D spheroids
(SYMPLE3D) – that sheds light on the process.
Various previous studies have looked at the role of morphogens
and cell adhesion during tissue growth separately. However, the
researchers noted a couple of recent studies indicating how a
morphogen involved in neural tube patterning controls expression of
a family of adhesion proteins called cadherins to form sharply
defined structures. Prompted by these insights, they devised
their model system to investigate the interplay between morphogens
and cadherins. They highlight how in vivo morphogens induce
numerous changes in cellular properties simultaneously, making it
hard to disentangle what is going on. For this reason, as they
highlight in the discussion of their report, "SYMPLE3D provides a
new synthetic biology approach for mechanistically studying tissue
patterning and engineering organoid structures."
SYMPLE3D uses two types of cells – one, the GFP secretors, which
secrete GFP and express P-cadherin forming what they describe as
"GFP-secreting organizer spheroids". The other is a GFP receiver
cell, initially engineered to express a synthetic
receptor called "synNotch" that recognizes GFP and
induces mCherry reporter – "imC cells" (Fig. 2A).
The first stage looked at the result of co-culturing the GFP
secretors and receiver cells. They found that although the imC
cells did capture the secreted GFP resulting in a GFP gradient, the
resulting gradient contained ectopically active cells –
expression of the high-level mCherry reporter in an
inappropriate position of the gradient (Fig. 2B, upper panel). To deal with the issue of
ectopically active cells, Mizuno and Toda engineered GFP receiver
cells to induce mCherry-fused E-cadherin, a cell adhesion molecule.
To their surprise, a uniformly activated tissue domain with
sharp boundary emerged instead of a gradient between the
secretor and receiver cells (Fig. 2B, lower panel).
Figure 2:
https://nanolsi.kanazawa-u.ac.jp/wp/wp-content/uploads/Toda_Fig.-2.jpg
Caption Figure 2. Tissue domain formation through the
coupling of morphogen signals and cell adhesion. (A) SYnthetic
Morphogen system for Pattern Logic Exploration using 3D spheroids
(SYMPLE3D). (B) mCherry (upper panel) or Ecad-mCherry (lower panel)
was induced in response to the GFP gradient.
The sharp boundary was also robust to changes in
growth conditions. Since the addition of a single factor,
E-cadherin, caused a significant change in the pattern, they then
focused on the mechanism of the pattern formation process with
a combination of molecular gradient and E-cadherin in their model
system.
By monitoring the real time process of tissue
growth, they were able to identify activated GFP receiver
cells engineered to induce mCherry-fused E-cadherin were initially
scattered but aggregated over the course of time. Ectopically
active cells were then gradually absorbed into this active domain
resulting in a sharp cut off between the mCherry positive and
negative domains. They also note "an intriguing aspect" of their
synthetic tissue domain, in that across the active domain the
distribution of induced E-cadherin-mCherry was uniformly high,
whereas GFP was distributed with a gradient. Here, they revealed a
key feature of E-cadherin for the synthetic tissue domain
formation. They analyzed the behavior of cells that express various
levels of E-cadherin in response to different amounts of GFP and
found that the behavior was the same whether the cells induced low
or high levels of E-cadherin. Furthermore, they showed that cells
that induced more than a certain amount of E-cadherin were able to
mix with each other and form a single cell population, regardless
of the expression level. Therefore, the mixing of cells that
induced different levels of E-cadherin within the GFP gradient
allowed the cells to receive GFP uniformly and thus the expression
level of E-cadherin became evenly high in the synthetic tissue
domain (Fig. 3). A simple mathematical model, developed by
Hirashima, based on cell movement governed by differential
adhesion energy supported their experimental observations. "Our
findings suggest the possibility of programming a new tissue domain
with sharp boundaries in organoids by combining synthetic
morphogens with cell adhesion control," they conclude in their
report.
Figure 3:
https://nanolsi.kanazawa-u.ac.jp/wp/wp-content/uploads/Toda_Fig.-3.jpg
Caption Figure 3. The pattern formation mechanism where
morphogen signals and cadherin expression cooperate to generate
tissue domains with a sharp boundary.
Note about the contributions of Kosuke Mizuno to research at the NanoLSI
Kosuke Mizuno, a second-year
doctoral student in the Nano Life Science Program, has made notable
contributions to NanoLSI research. He was awarded the NanoLSI
Transdisciplinary Research Grant for FY2023 and FY2024.
Glossary
Morphogen
A signaling molecule that controls cell fate decision
dependently on its local concentration to regulate morphogenesis.
Morphogens are secreted from source cells, diffuse within tissues
and form a concentration gradient that works as positional
information for cell differentiation. Representative morphogens
include Wnt, BMP, Shh, and retinoic acid.
Cadherins
Cadherins are a family of transmembrane proteins that
facilitate cell to cell adhesion. Mizuno, Hirashima and Toda use
E-cadherin and P-cadherin in the current study, which belong to the
classical cadherin family. Cadherins primarily bind to each other
via their homophilic extracellular domains. However, cadherins
also have an intracellular domain, which binds to adaptor proteins
connected to actin cytoskeletons and contributes to tissue
compaction and cell sorting.
Synthetic Notch receptor (synNotch)
Notch is a signal transduction receptor. When the extracellular
domain of Notch receptor binds to its ligand Delta, Notch
transmembrane region is cleaved, leading to the translocation of
Notch intracellular domain into the nucleus to regulate the
expression of target genes. The synNotch receptor is a modified
version of Notch receptor, in which the extracellular domain of
Notch is replaced by an antibody or nanobody and the intracellular
domain by an artificial transcription factor. Using synNotch
receptors, researchers can design what ligand molecule cells
recognize and what target genes cells express in response, which
enables manipulation of cell-cell communications.
Reference
Kosuke Mizuno, Tsuyoshi Hirashima, Satoshi Toda. Robust tissue pattern
formation by coupling morphogen signal and cell adhesion
EMBO Reports. 2024.
DOI:10.1038/s44319-024-00261-z
URL:
https://www.embopress.org/doi/full/10.1038/s44319-024-00261-z
Funding
This research was supported by the World Premier International
Research Center Initiative (WPI), MEXT, Japan, Japan Science and Technology Agency
(JST) PRESTO (JPMJPR2147), Grant-in-Aid for Scientific Research
(20K15828, 21H05291, 21H05290), Japan Agency for Medical Research
and Development (AMED) (22bm0704048h0003), Senri Life Science
Foundation, Kato Memorial Bioscience Foundation, Kao Foundation,
Yoshida Scholarship Foundation, and the Mechanobiology Institute,
National University of Singapore.
Contact
Fujiko Imanaga (Ms)
Project Planning and Outreach
NanoLSI Administration Office, Nano Life Science Institute
(WPI-NanoLSI)
Kanazawa University
Kakuma-machi, Kanazawa 920-1192, Japan
Email: nanolsi-office@adm.kanazawa-u.ac.jp
Tel: +81 (76) 234-4555
About Nano Life Science Institute (WPI-NanoLSI), Kanazawa
University
Understanding nanoscale mechanisms of life phenomena by
exploring "uncharted nano-realms".
Cells are the basic units of almost all life forms. We are
developing nanoprobe technologies that allow direct imaging,
analysis, and manipulation of the behavior and dynamics of
important macromolecules in living organisms, such as proteins and
nucleic acids, at the surface and interior of cells. We aim at
acquiring a fundamental understanding of the various life phenomena
at the nanoscale.
https://nanolsi.kanazawa-u.ac.jp/en/
About the World Premier International Research Center Initiative
(WPI)
The WPI program was launched in 2007 by Japan's Ministry of Education, Culture,
Sports, Science and Technology (MEXT) to foster globally visible
research centers boasting the highest standards and outstanding
research environments. Numbering more than a dozen and operating at
institutions throughout the country, these centers are given a high
degree of autonomy, allowing them to engage in innovative modes of
management and research. The program is administered by the Japan
Society for the Promotion of Science (JSPS).
See the latest research news from the centers at the WPI News
Portal: https://www.eurekalert.org/newsportal/WPI
Main WPI program site: www.jsps.go.jp/english/e-toplevel
About Kanazawa University
As the leading comprehensive university on the Sea of
Japan coast, Kanazawa University
has contributed greatly to higher education and academic research
in Japan since it was founded in
1949. The University has three colleges and 17 schools offering
courses in subjects that include medicine, computer engineering,
and humanities.
The University is located on the coast of the Sea of
Japan in Kanazawa – a city rich in
history and culture. The city of Kanazawa has a highly respected
intellectual profile since the time of the fiefdom (1598-1867).
Kanazawa University is divided into two main campuses: Kakuma and
Takaramachi for its approximately 10,200 students including 600
from overseas.
http://www.kanazawa-u.ac.jp/en/
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