4.8 Article

The 3D architecture and molecular foundations of de novo centriole assembly via bicentrioles

期刊

CURRENT BIOLOGY
卷 31, 期 19, 页码 4340-+

出版社

CELL PRESS
DOI: 10.1016/j.cub.2021.07.063

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资金

  1. FCT (Fundacao para a Ciencia e a Tecnologia) [PD/BD/114350/2016]
  2. JSPS KAKENHI [17H06471]
  3. FCT ERA-CAPS project EVOREPRO [ERA-CAPS-0001-2014]
  4. Cristian Boulin fellowship (EMBL)
  5. [ERC-2015-CoG-683258-BirthDeath]
  6. Grants-in-Aid for Scientific Research [17H06471] Funding Source: KAKEN
  7. Fundação para a Ciência e a Tecnologia [PD/BD/114350/2016, ERA-CAPS/0001/2014] Funding Source: FCT

向作者/读者索取更多资源

Centrioles in the spermatogenesis of the bryophyte Physcomitrium patens are born through an uncharacterized de novo pathway, showing twisted and asymmetric morphology. This phenomenon reveals that centriole biogenesis is more diverse than previously thought.
Centrioles are structurally conserved organelles, composing both centrosomes and cilia. In animal cycling cells, centrioles often form through a highly characterized process termed canonical duplication. However, a large diversity of eukaryotes assemble centrioles de novo through uncharacterized pathways. This unexplored diversity is key to understanding centriole assembly mechanisms and how they evolved to assist specific cellular functions. Here, we show that, during spermatogenesis of the bryophyte Physcomitrium patens, centrioles are born as a co-axially oriented centriole pair united by a cartwheel. Interestingly, we observe that these centrioles are twisted in opposite orientations. Microtubules emanate from the bicentrioles, which localize to the spindle poles during cell division. After their separation, the two resulting sister centrioles mature asymmetrically, elongating specific microtubule triplets and a naked cartwheel. Subsequently, two motile cilia are assembled that appear to alternate between different motility patterns. We further show that centriolar components SAS6, Bld10, and POC1, which are conserved across eukaryotes, are expressed during spermatogenesis and required for this de novo biogenesis pathway. Our work supports a scenario where centriole biogenesis, while driven by conserved molecular modules, is more diverse than previously thought.

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