Niemann-Pick C1 Like 1 Protein Is Critical for Intestinal Cholesterol Absorption

S. Altmann; Harry R. Davis; Li-Ji Zhu; Xiaorui Yao; Lizbeth Hoos; Glen Tetzloff; Sai Prasad N. Iyer; Maureen Maguire; Andrei Golovko; Ming Zeng; Luquan Wang; Nicholas Murgolo; Michael P. Graziano

doi:10.1126/science.1093131

Niemann-Pick C1 Like 1 Protein Is Critical for Intestinal Cholesterol Absorption

S. Altmann(AIL Research (United States)), Harry R. Davis(AIL Research (United States)), Li-Ji Zhu(AIL Research (United States)), Xiaorui Yao(AIL Research (United States)), Lizbeth Hoos(AIL Research (United States)), Glen Tetzloff(AIL Research (United States)), Sai Prasad N. Iyer(AIL Research (United States)), Maureen Maguire(AIL Research (United States)), Andrei Golovko(AIL Research (United States)), Ming Zeng(AIL Research (United States)), Luquan Wang(AIL Research (United States)), Nicholas Murgolo(AIL Research (United States)), Michael P. Graziano(AIL Research (United States))

Science

February 19, 2004

10.1126/science.1093131

Cited by 1,764

Abstract

Dietary cholesterol consumption and intestinal cholesterol absorption contribute to plasma cholesterol levels, a risk factor for coronary heart disease. The molecular mechanism of sterol uptake from the lumen of the small intestine is poorly defined. We show that Niemann-Pick C1 Like 1(NPC1L1) protein plays a critical role in the absorption of intestinal cholesterol. NPC1L1 expression is enriched in the small intestine and is in the brush border membrane of enterocytes. Although otherwise phenotypically normal, NPC1L1-deficient mice exhibit a substantial reduction in absorbed cholesterol, which is unaffected by dietary supplementation of bile acids. Ezetimibe, a drug that inhibits cholesterol absorption, had no effect in NPC1L1 knockout mice, suggesting that NPC1L1 resides in an ezetimibe-sensitive pathway responsible for intestinal cholesterol absorption.

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