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  • 1
    ISSN: 1432-1351
    Keywords: Mechanosensation ; Gravitaxis ; Kinesis ; Paramecium
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology , Medicine
    Notes: Summary 1. We have investigated a physiological component of the gravitaxis of Paramecium using established mechanisms of ciliate mechanosensitivity. The horizontal, up and down swimming rates of cells, and the sedimentation of immobilized specimens were determined. Weak DC voltage gradients were applied to predetermine the Paramecium swimming direction. 2. An observed steady swimming rate is the vector sum of active propulsion (P), a possible gravity-dependent change in swimming rate (Δ), and rate of sedimentation (S). We approximated P from horizontal swimming. S was measured after cell immobilization. 3. Theory predicts that the difference between the down and up swimming rates, divided by two, equals the sum of S and Δ. Δ is supposed to be the arithmetic mean of two subcomponents, Δ a and Δ p, from gravistimulation of the anterior and posterior cell ends, respectively. 4. A negative value of Δ (0.038 mm/s) was isolated with Δ a(0.070 mm/s) subtracting from downward swimming, and Δ p(0.005 mm/s) adding to upward propulsion. The data agree with one out of three possible ways of gravisensory transduction: outward deformation of the mechanically sensitive ‘lower’ soma membrane. We call the response a negative gravikinesis because both Δ a and Δ p antagonize sedimentation.
    Type of Medium: Electronic Resource
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  • 2
    ISSN: 1435-232X
    Keywords: myotonic dystrophy ; unstable CTG repeat sequence ; anticipation ; dynamic mutation ; contraction
    Source: Springer Online Journal Archives 1860-2000
    Topics: Biology , Medicine
    Notes: Summary To study the characteristics, if any, of unstable CTG repeat sequence in Japanese myotonic dystrophy (DM), we analyzed DNA from 351 at risk individuals (including affected and non-affected carriers and their descendants) from 105 families in Japan. A total of 93 DM families (196 affected and 116 unaffected individuals), including 84 DM parentchild pairs (44 father-child and 40 mother-child pairs), were examined, many of which had been previously tested by linkage analysis. We detected unstable CTG repeat mutations between 0.15 kb and 8.7 kb in size. The size of the mutation correlated with the age of onset of symptoms. There was a significant difference in DM allele size among the four groups (congenital, juvenile onset, classical, and minimal). Congenital DM had on average the largest repeat sizes. Comparison of parent-child pairs showed that most offspring had a larger repeat size than their parents, with only 2 of 84 showing a definite decrease in repeat size. The correlation coefficients for maternal and paternal transmission were 0.41 and 0.15, respectively. The parental age (maternal and paternal) did not correlate with intergenerational change of repeat. These observations are similar to those reported in Caucasians.
    Type of Medium: Electronic Resource
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