spostrzeżenie - Biomineralization - # Actomyosin Regulation in Eukaryote Biomineralization

Actomyosin Role in Sea Urchin Skeletogenesis

Q: How does the role of actomyosin machinery in sea urchins compare to other organisms' biomineralization processes

In sea urchins, the actomyosin machinery plays a crucial role in biomineralization processes by regulating spicule formation, growth, and morphology. This is evident from the study where Rho-associated coiled-coil kinase (ROCK), a key protein involved in actomyosin remodeling, was found to control the formation and elongation of calcite spicules in sea urchin larvae. The actin filaments are enriched around the spicules, particularly at the tips of growing skeletal rods. Perturbations in actin polymerization or myosin contractility led to significant effects on skeletal growth and branching patterns. Comparatively, in other organisms such as vertebrates, the actomyosin network also plays essential roles in biomineralization processes related to bone and teeth formation. For instance, Rho GTPases and ROCK have been shown to regulate differentiation of chondrocytes, osteoblasts, and odontoblasts while influencing gene expression in these biomineralizing cells. In diatoms and foraminifera as well as coccolithophores and diatoms among unicellular organisms that undergo biomineralization using distinct minerals like silica or calcium carbonate shells respectively - there is evidence of association between actin filaments with mineral deposition compartments. Overall, while specific details may vary across different organisms due to their evolutionary history and structural differences in skeletons or shells produced (e.g., calcite vs hydroxyapatite), it is clear that the actomyosin machinery serves as a common regulatory mechanism for controlling mineral growth during biomineralization processes across diverse species.

Q: What potential implications could altering actomyosin activity have on human bone development or dental health

Altering activity within the actomyosin machinery could have significant implications for human bone development or dental health based on insights gained from studies on sea urchins' skeletogenesis process. Bone Development: Understanding how ROCK inhibition affects skeletal growth rate and branching patterns can provide valuable insights into potential therapeutic targets for conditions affecting human bones such as osteoporosis or fractures. By modulating ROCK activity pharmacologically or genetically similar to what was done with sea urchins' embryos - researchers could potentially influence bone regeneration rates or prevent abnormal bone formations. Dental Health: Since teeth are another form of biominerals created through complex cellular processes akin to those seen in skeletogenesis - altering actomyosin activity might impact tooth enamel formation which involves intricate interactions between ameloblasts (cells responsible for enamel production) along with proteins like amelogenins that guide mineral deposition pathways. Regenerative Medicine: Insights into how molecular mechanisms including F-actin organization around forming structures contribute to proper mineral deposition can inform regenerative medicine strategies aimed at enhancing tissue repair post-injury or disease-related damage involving hard tissues like bones or teeth.

Q: How might understanding the molecular mechanisms behind biomineralization contribute to advancements in regenerative medicine

Understanding molecular mechanisms behind biomineralization holds great promise for advancements in regenerative medicine by offering insights into controlled tissue engineering approaches: Biomimetic Materials: Knowledge about how natural systems utilize specific proteins like ROCK within an organized cytoskeletal framework during mineralized tissue development can inspire bioengineers towards creating biomimetic materials mimicking these biological processes more effectively. Targeted Therapies: Unraveling signaling pathways influenced by molecules such as VEGF alongside downstream effectors like ROCK provides potential targets for developing precise therapies targeting specific stages of tissue regeneration where controlled mineral deposition is critical. 3** Stem Cell Differentiation:** Understanding how genes associated with skeletogenic lineage progression respond under altered mechanical cues mediated by factors like F-actinand MyoII offers valuable information guiding stem cell differentiation protocols towards generating specialized cell types required for effective regenerative strategies focused on musculoskeletal disordersor dental reconstruction efforts

Główne pojęcia

Actomyosin network, specifically ROCK, plays a crucial role in controlling mineral growth and morphology during sea urchin skeletogenesis by regulating gene expression and spicule formation.

Streszczenie

Biomineralization across different phyla involves the actomyosin network, with ROCK playing a key role in sea urchin skeletogenesis. ROCK controls spicule initiation, elongation, and branching by influencing gene expression and F-actin organization. The study highlights the importance of actomyosin machinery in biomineral growth and morphogenesis.

The study reveals that ROCK regulates cell differentiation and gene expression in vertebrates' biomineralizing cells. In sea urchins, ROCK controls the formation, growth, and morphology of calcite spicules downstream of VEGF signaling. Inhibition of ROCK leads to skeletal loss, disrupted gene expression, reduced skeletal growth rate, and ectopic spicule branching.

Furthermore, perturbations of the actomyosin network affect skeletal growth and branching patterns. F-actin polymerization inhibition results in severe deformation of shells, while MyoII activation inhibition leads to ectopic branching at the tips of rods. The spatial expression of key regulatory genes is altered under ROCK inhibition, affecting skeletogenic lineage progression.

Overall, the study demonstrates the critical role of ROCK and the actomyosin network in sea urchin skeletogenesis through regulation of gene expression and mineral deposition processes.

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biorxiv.org

Statystyki

"ROCK controls spicule initiation, elongation, and morphology."
"Inhibition of ROCK leads to skeletal loss and disrupted gene expression."
"F-actin polymerization perturbations result in severe deformation of shells."
"MyoII activation inhibition causes ectopic branching at rod tips."

Cytaty

"In sea urchins, ROCK controls the formation, growth, and morphology of calcite spicules downstream of VEGF signaling."
"Continuous ROCK inhibition results in downregulation of multiple skeletogenic genes essential for biomineralization."

Kluczowe wnioski z

ROCK and the actomyosin network control biomineral growth and morphology during sea urchin skeletogenesis

by Hijaze,E., G... o www.biorxiv.org 12-21-2022

https://www.biorxiv.org/content/10.1101/2022.12.21.521381v5

Głębsze pytania

How does the role of actomyosin machinery in sea urchins compare to other organisms' biomineralization processes

In sea urchins, the actomyosin machinery plays a crucial role in biomineralization processes by regulating spicule formation, growth, and morphology. This is evident from the study where Rho-associated coiled-coil kinase (ROCK), a key protein involved in actomyosin remodeling, was found to control the formation and elongation of calcite spicules in sea urchin larvae. The actin filaments are enriched around the spicules, particularly at the tips of growing skeletal rods. Perturbations in actin polymerization or myosin contractility led to significant effects on skeletal growth and branching patterns.
Comparatively, in other organisms such as vertebrates, the actomyosin network also plays essential roles in biomineralization processes related to bone and teeth formation. For instance, Rho GTPases and ROCK have been shown to regulate differentiation of chondrocytes, osteoblasts, and odontoblasts while influencing gene expression in these biomineralizing cells. In diatoms and foraminifera as well as coccolithophores and diatoms among unicellular organisms that undergo biomineralization using distinct minerals like silica or calcium carbonate shells respectively - there is evidence of association between actin filaments with mineral deposition compartments.
Overall, while specific details may vary across different organisms due to their evolutionary history and structural differences in skeletons or shells produced (e.g., calcite vs hydroxyapatite), it is clear that the actomyosin machinery serves as a common regulatory mechanism for controlling mineral growth during biomineralization processes across diverse species.

What potential implications could altering actomyosin activity have on human bone development or dental health

Altering activity within the actomyosin machinery could have significant implications for human bone development or dental health based on insights gained from studies on sea urchins' skeletogenesis process.

Bone Development: Understanding how ROCK inhibition affects skeletal growth rate and branching patterns can provide valuable insights into potential therapeutic targets for conditions affecting human bones such as osteoporosis or fractures. By modulating ROCK activity pharmacologically or genetically similar to what was done with sea urchins' embryos - researchers could potentially influence bone regeneration rates or prevent abnormal bone formations.

Dental Health: Since teeth are another form of biominerals created through complex cellular processes akin to those seen in skeletogenesis - altering actomyosin activity might impact tooth enamel formation which involves intricate interactions between ameloblasts (cells responsible for enamel production) along with proteins like amelogenins that guide mineral deposition pathways.

Regenerative Medicine: Insights into how molecular mechanisms including F-actin organization around forming structures contribute to proper mineral deposition can inform regenerative medicine strategies aimed at enhancing tissue repair post-injury or disease-related damage involving hard tissues like bones or teeth.

How might understanding the molecular mechanisms behind biomineralization contribute to advancements in regenerative medicine

Understanding molecular mechanisms behind biomineralization holds great promise for advancements in regenerative medicine by offering insights into controlled tissue engineering approaches:

Biomimetic Materials: Knowledge about how natural systems utilize specific proteins like ROCK within an organized cytoskeletal framework during mineralized tissue development can inspire bioengineers towards creating biomimetic materials mimicking these biological processes more effectively.

Targeted Therapies: Unraveling signaling pathways influenced by molecules such as VEGF alongside downstream effectors like ROCK provides potential targets for developing precise therapies targeting specific stages of tissue regeneration where controlled mineral deposition is critical.

3** Stem Cell Differentiation:** Understanding how genes associated with skeletogenic lineage progression respond under altered mechanical cues mediated by factors like F-actinand MyoII offers valuable information guiding stem cell differentiation protocols towards generating specialized cell types required for effective regenerative strategies focused on musculoskeletal disordersor dental reconstruction efforts