22 research outputs found
Cortical Contributions to Saccadic Suppression
The stability of visual perception is partly maintained by saccadic suppression: the selective reduction of visual sensitivity that accompanies rapid eye movements. The neural mechanisms responsible for this reduced perisaccadic visibility remain unknown, but the Lateral Geniculate Nucleus (LGN) has been proposed as a likely site. Our data show, however, that the saccadic suppression of a target flashed in the right visual hemifield increased with an increase in background luminance in the left visual hemifield. Because each LGN only receives retinal input from a single hemifield, this hemifield interaction cannot be explained solely on the basis of neural mechanisms operating in the LGN. Instead, this suggests that saccadic suppression must involve processing in higher level cortical areas that have access to a considerable part of the ipsilateral hemifield
A Motion Illusion Reveals Mechanisms of Perceptual Stabilization
Visual illusions are valuable tools for the scientific examination of the mechanisms underlying perception. In the peripheral drift illusion special drift patterns appear to move although they are static. During fixation small involuntary eye movements generate retinal image slips which need to be suppressed for stable perception. Here we show that the peripheral drift illusion reveals the mechanisms of perceptual stabilization associated with these micromovements. In a series of experiments we found that illusory motion was only observed in the peripheral visual field. The strength of illusory motion varied with the degree of micromovements. However, drift patterns presented in the central (but not the peripheral) visual field modulated the strength of illusory peripheral motion. Moreover, although central drift patterns were not perceived as moving, they elicited illusory motion of neutral peripheral patterns. Central drift patterns modulated illusory peripheral motion even when micromovements remained constant. Interestingly, perceptual stabilization was only affected by static drift patterns, but not by real motion signals. Our findings suggest that perceptual instabilities caused by fixational eye movements are corrected by a mechanism that relies on visual rather than extraretinal (proprioceptive or motor) signals, and that drift patterns systematically bias this compensatory mechanism. These mechanisms may be revealed by utilizing static visual patterns that give rise to the peripheral drift illusion, but remain undetected with other patterns. Accordingly, the peripheral drift illusion is of unique value for examining processes of perceptual stabilization
HIGH-MOLECULAR-WEIGHT HYDROXYPROPYLMETHYLCELLULOSE - A CHOLESTEROL-LOWERING AGENT
Background: We assessed the efficacy of a high-molecular-weight
hydroxypropylmethylcellulose (K8515) as a cholesterol-lowering agent,
the dose-response profile of its action, and the ability of adult
subjects to tolerate its ingestion at effective doses.
Methods: These studies were conducted at the Clinical Research Center of
The University of Michigan Hospitals, Ann Arbor. Efficacy was assessed
in 10 normal and 12 mildly hyperlipidemic subjects in double-blind,
randomized crossover trials of 1 and 2 weeks’ duration, respectively.
The dose-response profile was studied in 12 mildly hypercholesterolemic
subjects in a nonrandomized control trial with doses given in escalating
order. Tolerance was assessed by a questionnaire of adverse effects and
bowel movement habits in all subjects.
Results: We found that 10 g of K8515 ingested in a prehydrated form
three times a day with meals lowered total cholesterol levels by an
average of 1.45 mmol/L (56 mg/dL) (32%) in normal subjects within 1
week. In two studies in subjects with mildly elevated cholesterol levels
(with entry levels ranging from 5.35 mmol/L [207 mg/dL] to 6.70
nunol/L [260 mg/dL]), average reductions of 1.00 mmol/L (39 mg/dL)
(18%) and 1.15 mmol/L (45 mg/dL) (20%) were observed within the same
period. The effect was primarily due to a reduction in low-density
lipoprotein cholesterol levels. Low-density lipoprotein levels in normal
subjects were an average of 1.10 mmol/L (42 mg/dL) (38%) lower after a
week of 10 g of K8515 three times a day with meals, and in the two
studies in subjects with mild hyperlipidemia, the reductions in
low-density lipoprotein levels after 1 week were 0.95 mmol/L (37 mg/dL)
(23%) and 1.05 mmol/L (40 mg/dL) (25%). Although there was a tendency
for high-density lipoprotein cholesterol levels to decrease, this was
significant only in normal subjects. Decreases in cholesterol levels
were not accompanied by any rise in triglyceride levels. Dose-response
studies in those with mildly elevated cholesterol levels indicated that
it is possible to achieve a 15% decrease in low-density lipoprotein
cholesterol levels within 1 week at a dose of 6.7 g three times a day,
with minimal adverse effects.
Conclusions: These results suggest a role for high-molecular-weight
hydroxypropylmethylcellulose in the clinical treatment of mild
hypercholesterolemia