Structural evidence for elastic tethers connecting separating chromosomes in crane-fly spermatocytes

Forer, Arthur; Otsuka, Shotaro

doi:10.26508/lsa.202302303

Cited by 4 publications

(4 citation statements)

References 31 publications

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“…That tethers are separate structural components connecting telomeres of separating anaphase chromosomes can be seen directly in electron microscope tomograms of crane-fly spermatocytes (Forer and Otsuka, 2023), tethers appearing as two component structures extending between separating partner telomeres.…”

Section: Introductionmentioning

confidence: 99%

Elastic tethers remain functional during anaphase arrest in partially-lysed crane-fly spermatocytes: a possible approach for studying mitotic tethers

Aidil,

Malick,

Forer

2024

Preprint

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Mitotic tethers connect partner telomeres of all segregating anaphase chromosomes in all animal cells that have been tested, as detected by laser-cutting chromosome arms during anaphase and seeing that the arm fragments move rapidly across the equator to their partner chromosome moving to the opposite pole, telomere moving towards telomere. Tethers exert anti-poleward forces on the poleward separating telomeres, but tether elasticity (that produces the backwards forces) diminishes during anaphase: as determined by the behavior of arm fragments; short tethers (early anaphase) are elastic, long tethers (late anaphase) are not elastic, and medium-length tethers transition between the two states. We developed a procedure in which the tethers still functioned after we partially-lysed anaphase crane-fly spermatocytes. The partial lysis consistently arrested chromosome movements, after which the tethers moved the chromosomes backwards, potentially allowing the elastic tethers to be studied biochemically. To ensure that tether function was not altered by the partial cell-lysis procedure, we compared backward chromosome movements in partially-lysed cells with arm fragment movements in control cells. In the partially-lysed cells the backward chromosomal movements had characteristics identical to those of arm fragments in non-lysed (control) cells. In particular, in both control and partially-lysed cells shorter tethers caused backward movements more often than did longer tethers; shorter tethers caused backward movements over greater fractional distances (of the tether) than did longer tethers; and velocities of the backwards movements were the same for tethers of different lengths. We also compared the effects of Calyculin A (an inhibitor of Protein Phosphatase1) in control versus in partially-lysed cells. Calyculin A (CalA) added to control cells in early anaphase blocks dephosphorylation, thereby maintaining tether elasticity throughout anaphase: after the chromosomes reach the poles they move backwards when the usual poleward forces are reduced. Partial lysis preserves this tether functionality: after partial lysis of CalA-treated cells the chromosomes move backward and reach the partner telomeres at even very long tether lengths. We conclude that partial cell-lysis arrests anaphase chromosome poleward movement but does not affect tether function.

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Section: Introductionmentioning

confidence: 99%

Elastic tethers remain functional during anaphase arrest in partially-lysed crane-fly spermatocytes: a possible approach for studying mitotic tethers

Aidil,

Malick,

Forer

2024

Preprint

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“…This study investigates whether inhibiting microtubules during anaphase in crane-fly spermatocytes affects the backward forces on chromosomes produced by elastic mitotic tethers. Mitotic tethers, present in a broad range of animal cells (Forer et al, 2017), physically connect telomeres of each segregating pair of half-bivalents during anaphase in crane-fly primary spermatocytes (Forer and Otsuka, 2023). Each pair is connected in two of the four arms (LaFountain et al ., 2002; Sheykhani et al, 2017).…”

Section: Introductionmentioning

confidence: 99%

“…Such backward movement is due to elastic tethers and not microtubules because it occurs only when both partner telomeres are intact (LaFountain et al, 2002; Forer et al, 2021); occurs for only the arm fragment piece that has the kinetochore when the arm fragment itself is cut in half (LaFountain et al, 2002); and occurs when taxol stabilizes microtubule activity (Forer et al, 2018). The elastic tethers connecting separating telomeres have been identified electron microscopically (Forer and Otsuka, 2023) and are quite different from microtubules. The backward movement is not caused by ultra-fine DNA bridges because DNA-bridges are not elastic, are found only in a small number of anaphase chromosomes, mostly at the centromeric regions rather than at telomeres, and when present retard or stop anaphase segregation (Chan et al, 2007; Barefield and Karlseder, 2012; Gemble et al ., 2015; Su et al ., 2016).…”

Section: Introductionmentioning

confidence: 99%

Elastic mitotic tethers remain functional after microtubules are inhibited

Adil,

Janan,

Forer

2024

Preprint

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During normal anaphase in animal cells, elastic tethers connect partner telomeres of segregating chromosomes and exert backward (anti-poleward) forces on those chromosomes. The experiments reported herein test whether microtubules need to be present in order for tethers to produce backwards forces. We disassembled spindle microtubules by treating anaphase crane-fly primary spermatocytes separately with nocodazole, colcemid, or podophyllotoxin. The drug treatments caused anaphase chromosomes to stop moving poleward; almost immediately thereafter they moved backward. The characteristics of the backward movements of the half-bivalents match those of the backwards movements of arm fragments formed by cutting chromosome arms during anaphase, for example the occurrence and lengths of backward movements were a function of tether length. The only difference from movement of arm fragments is that the chromosomes in the treated cells moved backwards slower than arm fragments did. Immunofluorescence of spindle tubulin after the drug treatments indicated that acetylated kinetochore microtubules were not depolymerized by the drugs, though the non-kinetochore spindle microtubules were depolymerized. Our data indicate that tethers move anaphase chromosomes backwards in the absence of functioning spindle microtubules. We suggest that the backward movements that take place when poleward forces are absent are due to tethers, and that the backward movements are slowed by the presence of acetylated kinetochore microtubules.

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“…Genes 2023, 14, 2193 2 of 17 Tethering can be transient and soft, as observed between promoters/enhancers at transcriptional hubs and during temporary relocation and association with transcriptional loci at nuclear periphery [12][13][14][15][16]. Tethering of a chromatin fiber at two ends can put DNA under enough tension to impact loop extrusion by resisting loop-extrusion forces [17,18].…”

Section: Introductionmentioning

confidence: 99%

Polymer Modeling Reveals Interplay between Physical Properties of Chromosomal DNA and the Size and Distribution of Condensin-Based Chromatin Loops

Kolbin,

Walker,

Hult

et al. 2023

Genes

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Transient DNA loops occur throughout the genome due to thermal fluctuations of DNA and the function of SMC complex proteins such as condensin and cohesin. Transient crosslinking within and between chromosomes and loop extrusion by SMCs have profound effects on high-order chromatin organization and exhibit specificity in cell type, cell cycle stage, and cellular environment. SMC complexes anchor one end to DNA with the other extending some distance and retracting to form a loop. How cells regulate loop sizes and how loops distribute along chromatin are emerging questions. To understand loop size regulation, we employed bead–spring polymer chain models of chromatin and the activity of an SMC complex on chromatin. Our study shows that (1) the stiffness of the chromatin polymer chain, (2) the tensile stiffness of chromatin crosslinking complexes such as condensin, and (3) the strength of the internal or external tethering of chromatin chains cooperatively dictate the loop size distribution and compaction volume of induced chromatin domains. When strong DNA tethers are invoked, loop size distributions are tuned by condensin stiffness. When DNA tethers are released, loop size distributions are tuned by chromatin stiffness. In this three-way interaction, the presence and strength of tethering unexpectedly dictates chromatin conformation within a topological domain.

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Structural evidence for elastic tethers connecting separating chromosomes in crane-fly spermatocytes

Cited by 4 publications

References 31 publications

Elastic tethers remain functional during anaphase arrest in partially-lysed crane-fly spermatocytes: a possible approach for studying mitotic tethers

Elastic tethers remain functional during anaphase arrest in partially-lysed crane-fly spermatocytes: a possible approach for studying mitotic tethers

Elastic mitotic tethers remain functional after microtubules are inhibited

Polymer Modeling Reveals Interplay between Physical Properties of Chromosomal DNA and the Size and Distribution of Condensin-Based Chromatin Loops

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