Analysis of microtubule sliding patterns in<i>Chlamydomonas</i>flagellar axonemes reveals dynein activity on specific doublet microtubules

Wargo, Matthew J.; McPeek, Mark A.; Smith, Elizabeth F.

doi:10.1242/jcs.01082

Cited by 48 publications

(59 citation statements)

References 56 publications

(90 reference statements)

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“…The output signal, presumably mediated by a radial spoke on one doublet microtubule, would be the activation of axonemal kinases located near I1-dynein Gaillard et al, 2006]. Consistent with these ideas, the central pair apparatus is asymmetric in structure and composition [Mitchell and Sale, 1999;Mitchell and Yokoyama, 2003;Mitchell, 2003a;Wargo and Smith, 2003;Smith and Yang, 2004;Lechtreck and Witman, 2007] and the position of the central pair correlates with sites of active sliding [Wargo and Smith, 2003;Wargo et al, 2004] and the position of doublets relative to the bend [Mitchell, 2003a;Smith and Yang, 2004]. The results have also revealed a functional role for kinases (PKA, CK1) and phosphatases (PP1, PP2A) that are physically localized in the axoneme Sale, 1996, 1997;King and Dutcher, 1997;Porter and Sale, 2000;Gaillard et al, 2001Gaillard et al, , 2006Gokhale et al, 2006].…”

Section: Functional Role Of I1 In Regulation Of Flagellar Bending: a mentioning

confidence: 87%

Keeping an eye on I1: I1 dynein as a model for flagellar dynein assembly and regulation

Wirschell

Hendrickson

Sale

2007

Cell Motil. Cytoskeleton

109

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Among the major challenges in understanding ciliary and flagellar motility is to determine how the dynein motors are assembled and localized and how dyneindriven outer doublet microtubule sliding is controlled. Diverse studies, particularly in Chlamydomonas, have determined that the inner arm dynein I1 is targeted to a unique structural position and is critical for regulating the microtubule sliding required for normal ciliary/flagellar bending. As described in this review, I1 dynein offers additional opportunities to determine the principles of assembly and targeting of dyneins to cellular locations and for studying the mechanisms that regulate dynein activity and control of motility by phosphorylation. Cell Motil.

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Section: Functional Role Of I1 In Regulation Of Flagellar Bending: a mentioning

confidence: 87%

Keeping an eye on I1: I1 dynein as a model for flagellar dynein assembly and regulation

Wirschell

Hendrickson

Sale

2007

Cell Motil. Cytoskeleton

109

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“…We have observed that lf1, lf2, and lf4 flagellar waveforms show serious deviations from the WT waveform. This points the way to further work involving an in vitro microtubule-sliding assay with isolated axonemes so as to examine the possible role of the central pair in modulating dynein activity on specific doublet microtubules [38][39][40]. A closer look at mutant cell shapes is, therefore, warranted.…”

Section: Discussionmentioning

confidence: 99%

Anomalies in the motion dynamics of long-flagella mutants of Chlamydomonas reinhardtii

Khona¹,

Rao²,

Motiwalla³

et al. 2012

J Biol Phys

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Chlamydomonas reinhardtii has long been used as a model organism in studies of cell motility and flagellar dynamics. The motility of the well-conserved '9+2' axoneme in its flagella remains a subject of immense curiosity. Using high-speed videography and morphological analyses, we have characterized long-flagella mutants (lf1, lf2-1, lf2-5, lf3-2, and lf4) of C. reinhardtii for biophysical parameters such as swimming velocities, waveforms, beat frequencies, and swimming trajectories. These mutants are aberrant in proteins involved in the regulation of flagellar length and bring about a phenotypic increase in this length. Our results reveal that the flagellar beat frequency and swimming velocity are negatively correlated with the length of the flagella. When compared to the wild-type, any increase in the flagellar length reduces both the swimming velocities (by 26-57%) and beat frequencies (by 8-16%). We demonstrate that with no apparent aberrations/ultrastructural Electronic supplementary material The online version of this article

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“…Phenotypic analyses of C1-defective mutants (e.g., Dutcher et al, 1984;Mitchell and Sale, 1999) as well as recent structural and functional studies (Smith, 2002a;Smith, 2002b;Wargo and Smith, 2003;Wargo et al, 2004) have provided ample evidence to indicate that the C1 microtubule plays a role in regulation of motility. In addition, each C1 projection appears to make a unique contribution to modulation of flagellar motility.…”

Section: Discussionmentioning

confidence: 99%

“…This control mechanism is disrupted in certain mutants including the C1-defective mutant, pf6 (Wargo et al, 2004). Our functional studies of dynein-driven microtubule sliding in isolated axonemes indicate that calmodulin and a calmodulin-dependent kinase may mediate the calcium signal and that the central apparatus and radial spokes are key components of the calcium signaling pathway (Smith, 2002b).…”

Section: Introductionmentioning

confidence: 86%

“…Our previous structural and functional studies of dyneindriven microtubule sliding provided evidence to indicate that calcium control of waveform includes modulation of the pattern of microtubule sliding between specific doublets (Wargo et al, 2004). This control mechanism is disrupted in certain mutants including the C1-defective mutant, pf6 (Wargo et al, 2004).…”

Section: Introductionmentioning

confidence: 97%

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Calmodulin and PF6 are components of a complex that localizes to the C1 microtubule of the flagellar central apparatus

Wargo

Dymek

Smith

2005

Journal of Cell Science

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Analysis of microtubule sliding patterns inChlamydomonasflagellar axonemes reveals dynein activity on specific doublet microtubules

Cited by 48 publications

References 56 publications

Keeping an eye on I1: I1 dynein as a model for flagellar dynein assembly and regulation

Keeping an eye on I1: I1 dynein as a model for flagellar dynein assembly and regulation

Anomalies in the motion dynamics of long-flagella mutants of Chlamydomonas reinhardtii

Calmodulin and PF6 are components of a complex that localizes to the C1 microtubule of the flagellar central apparatus

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