CholesterylEsterTransferProtein

Cholesteryl Ester Transfer Protein

http://www.100md.com 《动脉硬化血栓血管生物学》2003年第2期

     Abstract4sh, http://www.100md.com

    Cholesteryl ester transfer protein (CETP) promotes the transferof cholesteryl esters from antiatherogenic HDLs to proatherogenicapolipoprotein B (apoB)–containing lipoproteins, includingVLDLs, VLDL remnants, IDLs, and LDLs. A deficiency of CETP isassociated with increased HDL levels and decreased LDL levels,a profile that is typically antiatherogenic. Studies in rabbits,a species with naturally high levels of CETP, support the therapeuticpotential of CETP inhibition as an approach to retarding atherogenesis.Studies in mice, a species that lacks CETP activity, have providedmixed results. Human subjects with heterozygous CETP deficiencyand an HDL cholesterol level >60 mg/dL have a reduced riskof coronary heart disease. Evidence that atherosclerosis maybe increased in CETP-deficient subjects whose HDL levels arenot increased is difficult to interpret and may reflect confoundingor bias. Small-molecule inhibitors of CETP have now been testedin human subjects and shown to increase the concentration ofHDL cholesterol while decreasing that of LDL cholesterol andapoB. Thus, it seems important and timely to test the hypothesisin randomized trials of humans that pharmacological inhibitionof CETP retards the development of atherosclerosis.

    Key Words: HDL LDL reverse cholesterol transport genetic CETP deficiencyuuf]v{, http://www.100md.com

    Introductionuuf]v{, http://www.100md.com

    The possibility that cholesteryl ester transfer protein (CETP)might be proatherogenic and that inhibition of its activitymight be antiatherogenic was first raised >10 years ago.¹The potential atherogenicity of CETP relates to its abilityto transfer cholesteryl esters from the antiatherogenic HDLsto the proatherogenic VLDL and LDL fractions. However, thereis also evidence that CETP may be involved in reverse cholesteroltransport (RCT). Thus, theoretically, CETP may be either proatherogenicor antiatherogenic. Most experimental evidence in animals favorsa proatherogenic role for CETP and supports a view that inhibitionof CETP is antiatherogenic.uuf]v{, http://www.100md.com

    It has also been suggested that CETP has the potential to inhibitatherogenesis by enhancing the rate of RCT, the pathway by whichcholesterol in peripheral tissues is transported to the liverfor elimination in the bile. This pathway involves an initialuptake of cell cholesterol by HDL, where it is esterified bylecithin:cholesterol acyltransferase (LCAT). A proportion ofthe HDL cholesteryl esters is delivered directly to the liver,whereas another proportion is transferred by CETP to LDL andVLDL. The cholesteryl esters in the VLDL/LDL pool are subsequentlydelivered to the liver via the LDL receptor pathway.

    The available clinical data in humans are incomplete and donot permit a definite conclusion about the relation of CETPdeficiency to the risk of coronary heart disease (CHD). In thisarticle, we review the totality of evidence on CETP and suggestfurther research.q, http://www.100md.com

    What Is CETP and What Does It Do?q, http://www.100md.com

    CETP is a hydrophobic glycoprotein that is secreted mainly fromthe liver and that circulates in plasma, bound mainly to HDL.²It promotes the redistribution of cholesteryl esters, triglycerides,and, to a lesser extent, phospholipids between plasma lipoproteins.CETP transfers lipids from 1 lipoprotein particle to anotherin a process that results in equilibration of lipids betweenlipoprotein fractions.³ Most of the cholesteryl esters in plasmaoriginate in HDL in the reaction catalyzed by LCAT, and themajority of the triglycerides enter the plasma as a componentof chylomicrons and VLDLs (triglyceride-rich lipoproteins [TRLs]).The overall effect of CETP is a net mass transfer of cholesterylesters from HDLs to TRLs and LDLs and of triglycerides fromTRLs to LDLs and HDLs Thus, CETP-mediated transfersfrom HDL to VLDL and LDL provide a potential indirect pathwayby which HDL cholesteryl esters can be delivered to the liver.In a high-CETP species such as the rabbit, this indirect pathwaymay account for as much as 70% of the cholesteryl esters thatoriginate in HDL.⁴

    fig.ommittedvsl, 百拇医药

     Role of CETP in plasma lipid transport. CETP promotes bidirectional transfers of cholesteryl esters (CE) and triglyceride (TG) between plasma lipoproteins. Because most of the CEs in plasma originate in HDL in the reaction catalyzed by LCAT and the majority of the TG enters plasma as a component of TRLs secreted either from the liver (VLDL) or intestine (chylomicrons), the overall effect of CETP is to promote a net mass transfer of CE from HDL to TRL and LDL and of TG from TRL to LDL and HDL. Pathways of RCT that deliver plasma CE to the liver include the hepatic uptake from HDL via the scavenger receptor B-1 (SRB-1) or the hepatic uptake of LDL via the LDL receptor (LDL-R).vsl, 百拇医药

    Under usual conditions, the rate of CETP-mediated cholesterylester transfer is rapid relative to the rate of HDL and LDLcatabolism.³ As a consequence, the pools of cholesteryl estersin HDLs and LDLs approach equilibrium in vivo. Thus, whereasan increase in the activity of CETP beyond physiological levelswould further increase the rate of bidirectional transfers betweenHDLs and LDLs, the effect on the distribution of cholesterylesters between the 2 lipoprotein fractions would be relativelysmall. In contrast, if CETP were inhibited, then there wouldbe a point beyond which its activity was rate limiting. Underthese circumstances, the level of CETP activity may have animportant role in determining the distribution of cholesterylesters between LDLs and HDLs. In the case of transfers betweenHDLs and the much more rapidly catabolized VLDLs, the amountof CETP in plasma is almost certainly rate limiting under mostconditions. Indeed, when the concentration of VLDLs is increased,the quantity of CETP is demonstrably the limiting factor inthe rate at which cholesteryl esters are transferred from HDLs.⁵

    When the level of VLDLs is normal, CETP-mediated transfers ofHDL cholesteryl esters are directed preferentially to LDLs⁶ In contrast, when the concentration of VLDLs isincreased, as in patients with type 2 diabetes, HDL cholesterylesters are preferentially transferred by CETP to larger VLDLparticles that become cholesterol rich and thus, potentiallymore atherogenic.⁶ Transfers of cholesteryl esters to TRLs areenhanced in the postprandial state.^7,8 The rate of cholesterylester transfer to TRLs and LDLs and the mass of CETP are increasedin patients with a range of atherogenic dyslipidemias.⁹0, http://www.100md.com

    fig.ommitted0, http://www.100md.com

     Effects of CETP in normotriglyceridemia (Normo TG) and hypertriglyceridemia (Hyper TG). The magnitude of the net flux of cholesteryl esters (CE) and TGs between lipoproteins is dependent, in large part, on the relative sizes of the TRL, LDL, and HDL pools. In Normo TG, net CE flux to LDLs from HDLs predominates, with minor transfer to TRLs. In contrast, in Hyper TG, increased particle numbers of large VLDLs exhibit elevated acceptor activity for CETP. Under these conditions, there are high net transfer rates of CEs from HDLs to TRLs and of TGs from TRLs to both HDLs and LDLs. TG-enriched LDLs and HDLs are substrates for hepatic lipase (HL) that hydrolyzes phospholipid (PL) and TGs to form small, dense LDL and small, dense HDL, respectively.

    CETP contributes to an atherogenic lipid phenotype in severalways. It increases the cholesteryl ester content and thus, theatherogenicity of VLDLs. It also interacts with triglyceridelipases to generate small, dense LDLs¹⁰ and HDLs¹¹.The CETP-mediated reduction in HDL particle size is accompaniedby the dissociation of lipid-poor apolipoprotein A-I (apoA-I)from the particle.^12–14 When the number of circulatingacceptor VLDL and LDL particles is reduced in vivo by treatmentwith a 3-hydroxy-3-methylglutaryl coenzyme A reductase inhibitor,there is retention of cholesteryl esters in the HDL fractionand an increase in the proportion of larger HDL₂ particles.¹⁵]1doi, 百拇医药

    Natural Inhibitors of CETP in Human Plasma]1doi, 百拇医药

    The presence of natural inhibitors of CETP has been reportedin human plasma. One such protein, initially referred to aslipid transfer inhibitor protein, has recently been identifiedas apoF.¹⁶ This protein preferentially suppresses transfersinvolving LDLs but has less effect on transfers involving HDLs.CETP inhibitory activity within the HDL fraction has been identifiedas apoC-I.¹⁷

    Role of CETP in the Development of Atherosclerosis in Animals.ha[, 百拇医药

    Expression of CETP in Transgenic Mice.ha[, 百拇医药

    Several species, including mice and rats, are naturally deficientin CETP. Introduction of the human CETP gene into mice resultsin a dose-related reduction in HDL levels and a small increasein VLDL and LDL cholesterol and apoB levels.^18,19 Mice are relativelyresistant to the development of diet-induced atherosclerosisand must clearly accomplish RCT by pathways that do not involveCETP activity. In fact, in studies of bile salt and cholesterol-fed,C57-B16 mice, the introduction and expression of the simiancetp gene resulted in enhanced formation of fatty streak lesionscompared with nonexpressing controls.²⁰ It was concluded thatthe enhancement of lesion development by CETP was secondaryto a redistribution of cholesterol from HDLs to the VLDL/LDLfraction..ha[, 百拇医药

    In another study,²¹ the human CETP gene was introduced intochow-fed, apoE-knockout mice and also into Western diet–fed,LDL receptor–knockout mice, both of which develop spontaneousatherosclerosis. CETP expression in these animal models redistributedcholesterol from HDLs to the VLDL/LDL pool and also increasedthe development of atherosclerosis. These results again supporta view that CETP is proatherogenic, possibly by virtue of reducingthe concentration of HDLs and redistributing cholesteryl estersfrom HDLs to the VLDL/LDL pool. However, when the CETP genewas overexpressed in apoE-knockout mice that also overexpressedhuman apoA-I, the effect of CETP on the development of atherosclerosiswas nonsignificant, despite being associated with a major reductionin the concentration of HDL cholesterol.²¹

    There are some circumstances in which the expression of CETPin mice has been reported to be antiatherogenic rather thanproatherogenic. An antiatherogenic effect of CETP has been observedin mice that have been engineered to overexpress human apoC-III.²²These animals have high levels of triglyceride-rich remnantlipoproteins and develop small fatty-streak lesions. Introductionand expression of the CETP gene into these animals appearedto reduce the extent of the lesions.²² In this and a more recentstudy in a hypertriglyceridemic mouse model (produced by streptozotocin-induceddiabetes and lipoprotein lipase deficiency), CETP was antiatherogenic,probably by decreasing the concentration of cholesterol in smallVLDL remnants.²³ Whether a comparable situation ever prevailsin humans is uncertain. Another example of an antiatherogeniceffect of CETP is seen in transgenic mice expressing human LCAT.²⁴These LCAT-transgenic mice have an increased concentration ofHDL cholesterol but paradoxically, also an increased susceptibilityto atherosclerosis. Expression of simian cetp in these animalsreduces the atherosclerosis.²⁵ It has been speculated, thoughnot tested, that the cholesteryl ester–enriched HDLs thatcirculate in LCAT-transgenic mice may be less able to acceptcholesterol from cells. If this were proved to be so, then theintroduction of CETP would provide a means for transferringcholesteryl esters from the HDLs, possibly restoring their efficiencyas acceptors of cell cholesterol and thus, as inhibitors ofthe development of atherosclerosis. This speculation is consistentwith studies of rabbits, a species with a naturally high levelof CETP. Transgenic expression of the human LCAT gene in rabbitsincreases the level of HDL cholesterol, reduces the concentrationof LDL cholesterol, and, in contrast to mice, reduces diet-inducedatherosclerosis.²⁶

    Inhibition of CETP in Rabbits(+#6o, http://www.100md.com

    Rabbits are highly susceptible to the development of diet-inducedatherosclerosis. Rabbits also have a naturally high level ofCETP. Furthermore, it has been demonstrated in several rabbitmodels of atherosclerosis that inhibiting CETP results in amarked reduction in atherosclerosis.(+#6o, http://www.100md.com

    In cholesterol-fed rabbits, the inhibition of CETP by injectionof antisense oligodeoxynucleotides (ODNs) against CETP resultedin a reduction in CETP mRNA and mass in the liver, a reductionin plasma total cholesterol, and an increased concentrationof HDL cholesterol.²⁷ There was also an increase in LDL receptormRNA associated with the antisense ODNs. These changes wereaccompanied by a marked reduction in aortic cholesterol contentas a marker of the extent of atherosclerosis.(+#6o, http://www.100md.com

    It is also possible to inhibit CETP in vivo by infusing anti-CETPantibodies into rabbits.²⁸ This study showed an effect of CETPon the distribution of cholesteryl esters between HDLs and VLDLs/LDLsbut did not investigate the effects of inhibition on the developmentof atherosclerosis. In a more recent report,²⁹ a vaccine approachhas been used to generate auto-antibodies against CETP in vivoin rabbits. In a study of cholesterol-fed rabbits, animals thatwere immunized against CETP had a reduced plasma activity ofCETP and a substantial increase in the concentration of HDLcholesterol. They also had a modest decrease in LDL cholesterolconcentration and a significant reduction in aortic atheroscleroticlesions. This study demonstrates that long-term inhibition ofCETP is not only possible but also, at least in rabbits, reducesthe susceptibility to atherosclerosis.

    A newly developed chemical inhibitor of CETP has been used inanother recent study of cholesterol-fed rabbits.³⁰ This inhibitorreduced CETP activity in rabbits by >90%, almost doubledthe level of HDL cholesterol, and decreased the non-HDL cholesterolby {approx} 50%. There was an accompanying 70% reduction in atheroscleroticlesions in the aortas of these animals. It was not possibleto determine the relative importance of the increased HDL versusthe decreased LDL in the reduction of atherosclerosis observedin these rabbit studies. It was speculated that short-term treatmentof humans with the same CETP inhibitor would result in a 40%to 45% increase in HDL cholesterol and a 15% to 20% decreasein LDL cholesterol.$2!^}, http://www.100md.com

    CETP, Lipoprotein Metabolism, and Atherosclerosis in Humans$2!^}, http://www.100md.com

    Genetic CETP Deficiency in Humans and Effects on Lipoprotein Metabolism$2!^}, http://www.100md.com

    Several mutations of the CETP gene have been identified as acause of CETP deficiency and elevated levels of HDL cholesterol.These include a G-to-A mutation at the +1 position of intron14,^1,31 a mutation that is present in up to 2% of the overallJapanese population^32,33 and in as many as 27% of people inthe Omagari area of Japan.³⁴ Individuals homozygous for thismutations have no measurable CETP mass or activity in theirplasma but do have elevated concentrations of both HDL lipids(cholesterol and phospholipid; 3- to 4-fold) and apoA-I (1.7-fold).³¹A second common functional mutation of the CETP gene, presentin up to 7% of the Japanese population, involves a D-to-G substitutionat the 442 position of exon 15³³ that also results in increasedHDL levels. However, subjects homozygous for this D442G mutationhave only a partial rather than a complete CETP deficiency,and HDL levels are elevated 1- to 2- fold.³³

    Subjects with a homozygous CETP deficiency have elevated concentrationsof HDL cholesterol, apoA-I, apoA-II, and apoE. The HDL fractionis especially enriched in larger, less dense, cholesteryl esterand apoE-enriched HDL₂ particles.³⁵ The increased HDL concentrationis due to a reduction in the rate of catabolism, with a markedlydelayed catabolism of both apoA-I and apoA-II.³⁶ In contrast,the synthesis of both apoA-I and apoA-II is similar to thatin control subjects.³⁶ Despite the delayed catabolism of apoA-Iand apoA-II, it has not been established whether the net fluxof cholesterol to the liver is decreased in patients with CETPdeficiency. In fact, there are no data to suggest that the rateof HDL apolipoprotein turnover is directly correlated with thenet flux of cholesterol to the liver.yi/ge-, 百拇医药

    The ability of HDLs from homozygous CETP-deficient individualsto promote the efflux of cholesterol from macrophages has beeninvestigated.³⁷ The large, apoE-rich HDLs were poor acceptorsof macrophage cholesterol, but the apoE-free HDL₂ and the HDL₃from these subjects functioned normally as acceptors of macrophagecholesterol.

    In addition to the elevation of HDL that accompanies CETP deficiency,in homozygotes there is a substantial reduction ({approx} 40%) in theconcentration of LDL cholesterol and apoB.³¹ These individualshave a polydisperse LDL fraction extending across the wholeLDL density range.^38,39 Human CETP deficiency is associatedwith both a decreased rate of production of apoB and an increasein its rate of catabolism, consistent with an upregulation ofthe LDL receptor in these subjects.⁴⁰ When preparations of LDLisolated from CETP-deficient patients and from control subjectswere injected into control subjects, the CETP-deficient LDLhad a delayed catabolism.⁴⁰ This result is consistent with theobservation of decreased affinity of the CETP-deficient LDLsfor the LDL receptor.⁴¹ One plausible explanation consistentwith both the LDL kinetic studies and the LDL receptor–bindingstudies is that the LDLs from CETP deficient patients are altered.However, these results are difficult to interpret in terms ofatherogenic potential, because any rapidly cleared particleswould be underrepresented. Furthermore, it is not known whetherthe net mass of cholesteryl esters cleared is altered when theparticle number is reduced.

    Atherosclerosis in CETP-Deficient Human Subjectso/i83h@, 百拇医药

    The relation between mutations of the CETP gene and susceptibilityto premature atherosclerosis is complex. In the Honolulu HeartStudy, many of the participants of Japanese origin were heterozygousfor the D442G mutation in the CETP gene and had reduced levelsof CETP.⁴² Those in whom the CETP deficiency coincided withHDL cholesterol concentrations of 41 to 60 mg/dL (1.0 to 1.5mmol/L) had an apparent 50% increase in CHD, although the totalnumber of events in this group was too low to enable firm conclusionsto be drawn. When the CETP deficiency was associated with higherHDL cholesterol levels (>60 mg/dL; >1.5 mmol/L), therewas no evidence of an increase in CHD. Rather, in this subgroup,there was a low rate of CHD, comparable to that observed inthe subjects in whom an elevated HDL cholesterol level was notassociated with a deficiency of CETP.o/i83h@, 百拇医药

    A recent analysis of the 7-year prospective data from the HonoluluHeart Study revealed no statistically significant relation betweenheterozygous mutations of CETP and CHD or stroke, a findingat variance with the previous suggestion from prevalence dataof increased risks (A.R Tall et al, in preparation). In fact,prospective analysis of the data has revealed a nonsignificanttrend toward a lower incidence of cardiovascular events in subjectswith CETP mutations.

    Results similar to those from the Honolulu Heart Study werefound in another study of Japanese subjects.⁴³ Individuals withHDL cholesterol levels >80 mg/dL were genotyped for intron14 and D442G mutations. Subjects with and without CETP genemutations (homozygous or heterozygous) who had HDL cholesterollevels >80 mg/dL had a very low risk of CHD. Given that theplasma level of CETP is, if anything, lower in deficient subjectswith the highest HDL cholesterol levels,⁴² it is difficult toimplicate CETP deficiency per se as a cause of increased CHD.It is possible that a deficiency of CETP is protective, so longas it induces a substantial increase in HDL cholesterol.g, 百拇医药

    HDLs may inhibit the development of atherosclerosis by mechanismsindependent of their involvement in RCT. These include antioxidant⁴⁴and anti-inflammatory^45,46 properties of HDL, both of whichhave an antiatherogenic potential that may be enhanced whenthe concentration of HDL is increased in CETP-deficient states.

    CETP Polymorphisms and Susceptibility to Atherosclerosis in Humansd\, http://www.100md.com

    There are several reported restriction fragment length polymorphisms(RFLPs) in the human CETP gene. Although many of thesestudies have demonstrated associations between CETP single-nucleotidepolymorphisms and small changes in plasma CETP and HDL levels,the relation between these polymorphisms and susceptibilityto atherosclerosis is variable Indeed, no consistentpicture has emerged from numerous studies examining the relationbetween polymorphisms and atherosclerotic cardiovascular disease.d\, http://www.100md.com

    fig.ommittedd\, http://www.100md.com

    Table 1. Mutations or Polymorphisms of the Human CETP Gened\, http://www.100md.com

    fig.ommittedd\, http://www.100md.com

    Relationship of Human CETP Polymorphisms to Atherosclerosis and CHDd\, http://www.100md.com

    The best-studied RFLP is Taq1B in intron 1. In 1 study, theTaq1B polymorphism accounted for 5.8% of the variance in HDLcholesterol.⁴⁷ Subjects homozygous for the B1 allele in theFramingham Offspring Study⁴⁸ had higher levels of CETP and lowerlevels of HDL cholesterol when compared with either B1B2 orB2B2 subjects. Men with the B2 allele appeared to have a reducedrisk of CHD, although there was no significant association inwomen. A similar result was obtained in the VA-HIT study inmen with CHD and low HDL.⁴⁹ The Taq1B genotype is associatedwith some of the variation in response to statin therapy, asmeasured by the progression of coronary atherosclerosis by angiography.⁵⁰Several other studies investigating the effects of the Taq1Bpolymorphism are summarized in Table 1. Overall, studies ofthe Taq1B polymorphism have been consistent and supportive ofa view that a lower level of CETP is associated with increasedHDL cholesterol and possibly a decreased risk of CHD in men.

    Results from studies of other polymorphisms have not demonstratedconsistent associations between CETP genotype and either atherosclerosisor CHD. In an investigation of the common I405V polymorphismamong 576 men of Japanese ancestry, plasma CETP concentrationswere 1.95 µg/mL for those with the II genotype, 1.91 µg/mLfor the IV genotype, and 1.77 µg/mL for the VV genotype.HDL levels were highest among those with the VV genotype andlowest among those with the II genotype,⁵¹ although the increasewas significant only in VV homozygotes with plasma triglyceridelevels >165 mg/dL (1.9 mmol/L). There were no differencesin CHD risk among the 3 genotypes in the total population, althoughin a subset of individuals with high plasma triglyceride levels,the CHD risk was higher in those with the VV genotype than inthose with the IV or II genotype (38% vs 27% vs 18%, respectively;P<0.05 for an interaction of genotype and plasma triglyceridelevels). Though not significant, the apparent trend was oppositein those with triglyceride levels <165 mg/dL (1.9 mmol/L).

    In an analysis of the I405V polymorphism in participants ofthe Copenhagen City Heart Study, women heterozygous or homozygousfor the presence of valine at position 405 had increased levelsof HDL cholesterol but also a paradoxical increased risk ofCHD.⁵² There was no association between the I405V polymorphismand either HDL cholesterol levels or CHD risk in the men inthis study. In another investigation of the I405V polymorphismin the Stanislas cohort study, the I405V polymorphism was notrelated to any lipid parameter.⁵³*:q^%, 百拇医药

    A further report from Copenhagen focused on the A373P and R451Qpolymorphisms.⁵⁴ All carriers of 451Q also carried the 373Pallele. Carriers of the 451Q/373P alleles had reduced levelsof HDL cholesterol and a paradoxically lower CHD risk when comparedwith the overall study population. The reasons for these apparentlyconflicting observations remain unclear but may be related,at least in part, to uncontrolled confounding by other genesor environmental factors.

    Another possibly functional polymorphism has recently been reportedin the promoter region of the CETP gene (-629A/C).⁵⁵ The massof CETP was higher and the concentration of HDL cholesterollower in individuals with the A allele than in those with theC allele, although the HDL cholesterol concentration was notcorrelated significantly with CETP mass. In studies of possiblemechanisms whereby the polymorphism influenced CETP mass, itwas found that repressor transcription factors that bound tothe A allele did not bind to the C allele. An interaction betweenCETP polymorphisms and lifestyle factors is suggested by 2 recentreports that alcohol consumption greatly influences the apparenteffects of several of the CETP polymorphisms.^56,57{, 百拇医药

    Inhibition of CETP in Humans: Effects on Plasma Lipoproteins{, 百拇医药

    A newly developed chemical inhibitor of CETP, JTT-705, has beentested in humans.⁵⁸ In a 4-week, phase II, dose-response study,198 healthy individuals with mild hyperlipidemia were randomlyassigned to 300, 600, or 900 mg/d of JTT-705 or to placebo.⁵⁸Treatment with the highest dose was associated with a highlysignificant 37% decrease in CETP activity, a 34% increase inHDLs, and a 7% decrease in LDLs. Levels of triglycerides, phospholipidtransfer protein, and LCAT were unchanged. Doses up to 900 mg/dwere safe and well tolerated but were significantly more likelythan placebo to cause mild gastrointestinal side effects.

    Conclusionsh'[m., http://www.100md.com

    Expression of CETP in transgenic mice, a species that is naturallydeficient in this protein, has yielded inconsistent results,with reports of both an increased susceptibility and protectionagainst atherosclerosis in different models. In contrast, theeffects in rabbits have been remarkably consistent and stronglysupport the therapeutic potential of CETP inhibition for bluntingor even halting the development and progression of atherosclerosis.h'[m., http://www.100md.com

    The available human data, though sparse, generally support thehypothesis that CETP deficiency, especially when associatedwith a high HDL level, is antiatherogenic. Those studies suggestingthat atherosclerosis is increased in some individuals with aheterozygous CETP deficiency may reflect chance owing to smallsample sizes, confounding by other risk factors, or biases inherentin the study design. There are no reliable data indicating thatCETP inhibition in humans would be unsafe. Indeed, CETP inhibitorsmay provide a powerful therapeutic approach to raising HDL levels,lowering LDL levels, and reducing the development of atherosclerosisin humans. However, such a proposition is based on circumstantialevidence and will remain hypothetical until subjected to directtesting. The recent negative trials with postmenopausal estrogens(that also increase HDL and lower LDL levels) highlight thepitfalls of drawing therapeutic conclusions from circumstantialevidence.

    Thus, the hypothesis that pharmacological inhibition of CETPreduces the risk of atherosclerosis should be directly testedin randomized trials with either surrogate or clinical end points.Such trials should be of sufficient size, dose, and durationto reliably test the hypothesis. Further multidisciplinary researchefforts into the metabolism of HDL, the precise roles playedby CETP, and its interactions with other components of lipidtransport and metabolism are also necessary to complete thetotality of evidence.;7, 百拇医药

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