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New study decodes one of the living world's fastest cell movements

Researchers find the genes and proteins involved in heliozoan arms withdrawal in response to environmental changes, which is one of the fastest examples of cell motility

Date:
January 18, 2023
Source:
Okayama University
Summary:
Heliozoan axopodia are important for their motility. However, the underlying mechanism of their axopodial contraction has remained ambiguous. Recently, researchers have reported that microtubules are simultaneously cleaved at multiple sites, allowing the radiating axopodia in a heliozoan, Raphidocystis contractilis, to disappear almost instantly. They have now identified the gene set and proteins involved in this microtubule disruption. This research can help develop a method to detect water pollution and evaluate the efficacy of new anticancer drugs.
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FULL STORY

Raphidocystis contractilisbelongs to Heliozoa, a group of eukaryotes commonly found in fresh, brackish, and sea water. The organisms of this group have finger-like arms -- axopodia -- which radiate out from their body, giving them a sun-like appearance. Hence, they are also known as "solar worms." Each axopodium is composed of the proteins, alpha-beta tubulin heterodimers, which form filaments called microtubules.R. contractiliscan withdraw its axopodia extremely fast in response to external stimuli. However, the mechanism underlying this rapid arm shortening remains a mystery.

To this end, a team of researchers including Professor Motonori Ando, Dr. Risa Ikeda (both from the Laboratory of Cell Physiology) and Associate Professor Mayuko Hamada (from the Ushimado Marine Institute), of Okayama University, Japan, explored the mechanism involved in one of the fastest cell movements in the living world.

So, where did it all begin? Sharing the motivation behind their study, Professor Ando says, "Recently, a wide variety of heliozoans have been discovered in various hydrospheres in the Okayama Prefecture, making it clear that several species of sun worms inhabit the same environment. We are trying to unravel the mysteries around these protozoans and gradually expand the horizons of our knowledge."

The authors started their investigation by immunolabelling the tubulin protein and observing its movement before and after axopodial contraction. They found that before shortening, tubulins were arranged systematically all along the length of the axopodia, but after axopodial withdrawal, those swiftly accumulated at the cell surface. This led them to believe that during the rapid axopodial withdrawal, the microtubules broke down into tubulin instantly. However, microtubule degradation is generally not a rapid phenomenon; it progresses rather slowly.

How then, could R. contractilis achieve this change so quickly?

The researchers hypothesized that this was possible if the microtubules split at multiple sites simultaneously. To validate their hypothesis, the authors set out to find the proteins and genes involved in the instant cleavage of microtubules inR. contractilis.Their findings were published online inTheJournal of Eukaryotic Microbiologyon 21 November 2022.

The researchers performedde novotranscriptome sequencing (analysis of the genes expressed at a particular time in a cell) and identified close to 32,000 genes inR. contractilis. This gene set was most similar to that found in protozoans (which are single-celled organisms), followed by metazoans (multicellular organisms with well-differentiated cells; this includes humans, and other animals).

获得的同源性和系统发育分析gene set revealed several genes (and their corresponding proteins) involved in microtubule disruption. Among these, the most important ones were katanin p60, kinesin, and calcium signaling proteins. Katanin p60 was involved in controlling the axopodial arm length. Several duplicates of kinesin genes were found. Among the identified kinesins, kinesin-13, a major microtubule destabilizing protein, was found to play an important role in the rapid contraction of axopodia. Calcium signaling genes regulate the entry of calcium ions into the cell from its surroundings and the induction of axopodial withdrawal.

The researchers also noticed a lack of genes linked with flagellar formation and motility, indicating that the axopodia ofR. contractilishave not evolved from flagella. Although many genes remain unclassified, the newly established gene set will serve as a reference for future studies aiming to understand the axopodial motility ofR. contractilis.

Heliozoan axopodia can function as a sensitive sensor. They can detect minute changes in their environment, e.g., the presence of heavy metal ions and anticancer drugs. Discussing their vision for the future, Professor Ando shares, "We believe that the axopodial response of heliozoa can be used as an index to develop temporary detection and monitoring devices for environmental and tap water pollution. It can also be used as a novel bioassay system for the primary screening of novel anticancer drugs. In the future, we plan to continue to work together as a team to enhance basic and applied research on these organisms."

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Story Source:

Materialsprovided byOkayama University.注:内容可以编辑风格and length.


Journal Reference:

  1. Risa Ikeda, Tosuke Sakagami, Mayuko Hamada, Tatsuya Sakamoto, Toshimitsu Hatabu, Noboru Saito, Motonori Ando.De novo transcriptome analysis of the centrohelid Raphidocystis contractilis to identify genes involved in microtubule‐based motility.Journal of Eukaryotic Microbiology, 2022; DOI:10.1111/jeu.12955

Cite This Page:

Okayama University. "New study decodes one of the living world's fastest cell movements." ScienceDaily. ScienceDaily, 18 January 2023. /releases/2023/01/230118092028.htm>.
Okayama University. (2023, January 18). New study decodes one of the living world's fastest cell movements.ScienceDaily. Retrieved October 30, 2023 from www.koonmotors.com/releases/2023/01/230118092028.htm
Okayama University. "New study decodes one of the living world's fastest cell movements." ScienceDaily. www.koonmotors.com/releases/2023/01/230118092028.htm (accessed October 30, 2023).

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