Ulf Lundstam scite author profile

Background-Using new, very high-resolution ultrasound biomicroscopy, we examined the thickness of artificial layers of silicone and intima thickness (IT) of radial and anterior tibial arteries in healthy subjects and in patients with vascular disease. Methods and Results-Silicone layers of varying thicknesses and mesenteric artery specimens obtained from 18 patients undergoing colectomy were measured by both ultrasound biomicroscopy (55 MHz) and morphometry. There was high correlation (rϾ0.9; PϽ0.0001) between IT and intima area versus ultrasound biomicroscopy. In 90 healthy subjects (aged between 10 and 90 years), radial and anterior tibial arterial IT and intima-media thickness were measured, as was carotid intima-media thickness in 56 of these subjects. Age was strongly related with both media thickness and IT of both peripheral arteries. Correlations were found between carotid intima-media thickness and both radial and anterior tibial IT/intima-media thickness (rϭ0.44 to 0.53; PϽ0.0001). The IT-to-lumen diameter ratio increased with age and was larger at all ages in the anterior tibial artery (0.067Ϯ0.034) versus the radial artery (0.036Ϯ0.012; PϽ0.0001). A thicker radial intimal layer was found in patients with peripheral artery disease. Conclusion-This

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N-acetylcysteine treatment lowers plasma homocysteine but not serum lipoprotein(a) levels

Wiklund

Fager²,

Andersson

et al. 1996

Atherosclerosis

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A mutation in POLE predisposing to a multi-tumour phenotype

Rohlin

Zagoras

Nilsson

et al. 2014

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Somatic mutations in the POLE gene encoding the catalytic subunit of DNA polymerase ɛ have been found in sporadic colorectal cancers (CRCs) and are most likely of importance in tumour development and/or progression. Recently, families with dominantly inherited colorectal adenomas and colorectal cancer were shown to have a causative heterozygous germline mutation in the proofreading exonuclease domain of POLE. The highly penetrant mutation was associated with predisposition to CRC only and no extra-colonic tumours were observed. We have identified a mutation in a large family in which the carriers not only developed CRC, they also demonstrate a highly penetrant predisposition to extra-intestinal tumours such as ovarian, endometrial and brain tumours. The mutation, NM_006231.2:c.1089C>A, p.Asn363Lys, also located in the proofreading exonuclease domain is directly involved in DNA binding. Theoretical prediction of the amino acid substitution suggests a profound effect of the substrate binding capability and a more severe impairment of the catalytic activity compared to the previously reported germline mutation. A possible genotype to phenotype correlation for deleterious mutations in POLE might exist that needs to be considered in the follow-up of mutation carriers.

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Ulf Lundstam

Increasing Peripheral Artery Intima Thickness From Childhood to Seniority

N-acetylcysteine treatment lowers plasma homocysteine but not serum lipoprotein(a) levels

A mutation in POLE predisposing to a multi-tumour phenotype

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