A multiple ascending dose study of CSL112, an infused formulation of ApoA‐I

Easton, Rachael; Gille, Andreas; D’Andrea, Denise; Davis, Roslyn; Wright, Samuel D.; Shear, Charles L.

doi:10.1002/jcph.194

Cited by 80 publications

(102 citation statements)

References 23 publications

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“…15 Here, we report for the first time the effects of CSL112 on key biomarkers of RCT after single and multiple intravenous infusions in healthy adult subjects.…”

Section: Gille Et Al Csl112 Enhances Biomarkers Of Rct 2107mentioning

confidence: 85%

“…Here, we show that infusion of CSL112 causes an immediate rise in apoA-I (C max 2 hours) to levels that depending on the dose double or even triple endogenous levels of apoA-I (Figure 1). Like endogenously produced apoA-I, the infused apoA-I seems to have some but limited access to the extravascular space (volume of distribution range, 5.6-9.7 L) 15 and to have clearance properties similar to endogenous apoA-I.Infusion of CSL112 caused movement of tissue cholesterol into the plasma as documented by the rise in total plasma cholesterol (Figure 2A), and the pathway of this movement seems consistent with the normal steps documented in the literature: unesterified cholesterol but not cholesterol ester is known to move to HDL before further transport or metabolism. 20 In keeping with this pattern, the elevated plasma cholesterol caused by CSL112 infusion appeared as unesterified cholesterol (Figure 3) and appeared in the HDL fraction ( Figure 2B-2D).…”

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confidence: 99%

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CSL112 Enhances Biomarkers of Reverse Cholesterol Transport After Single and Multiple Infusions in Healthy Subjects

Gille

Easton

D’Andrea

et al. 2014

ATVB

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112

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Objective-The ability of apolipoprotein A-I (apoA-I) to transport cholesterol from atherosclerotic plaque is thought to underlie its inverse correlation with cardiovascular risk. To gauge the potential of infused apoA-I to transport cholesterol, we quantified cholesterol transport markers in human subjects infused with a novel formulation of apoA-I (CSL112). Approach and Results-CSL112 was infused into human subjects in single (57 subjects) and multiple (36 subjects) ascending dose trials. Pharmacokinetic and biomarker assessments were conducted before and after infusions. CSL112 caused an immediate, up to 3-fold elevation of apoA-I and subsequent movement of tissue cholesterol into plasma. Cholesterol appeared first as unesterified cholesterol in the high-density lipoprotein (HDL) fraction and was promptly esterified by lecithin cholesterol acyltransferase. HDL cholesterol increased up to 81±16.5%. Underlying this movement of cholesterol was an immediate and strong rise in the ability of plasma to promote cholesterol efflux from cells ex vivo. CSL112 had its greatest impact on the fraction of efflux mediated by ATP-binding cassette transporter A1 (ABCA1), a cholesterol transporter induced in cholesterol-loaded tissues such as plaque. ABCA1-dependent efflux capacity increased ≤630±421% and total efflux capacity by ≤192±40%. In keeping with this finding, we observed a profound rise in very small HDL, also known as preβ1-HDL, the preferred substrate for ABCA1. Very small HDL increased ≤3596±941%.Elevations in apoA-I, cholesterol efflux, and very small HDL were dose-proportional over a wide range. No significant changes in atherogenic lipids were observed at any dose. Conclusions-Infusion Gille et al CSL112 Enhances Biomarkers of RCT 2107CSL112 is a novel formulation of apoA-I, the chief protein component of HDL, purified from human plasma and reconstituted with phosphatidylcholine to form HDL particles suitable for infusion. The production, physical characteristics of CSL112, and the pharmacokinetic and biomarker profile in rabbits have recently been described.14 CSL112 is a discoid particle containing 2 copies of apoA-I and ≈110 molecules of phosphatidylcholine. CSL112 was designed to provide improved particle uniformity and an improved safety profile compared with a previous formulation termed CSL111. The safety characteristics of CSL111 12 and improved safety characteristics of CSL112 15 have been previously described. CSL112 is also designed to optimize cholesterol efflux by ATP-binding cassette transporter A1 (ABCA1), a transporter induced by excess cellular cholesterol and present in atherosclerotic plaque.16 A detailed description of CSL112 pharmacokinetic in a multiple ascending dose (MAD) phase 1 study has been described. 15 Here, we report for the first time the effects of CSL112 on key biomarkers of RCT after single and multiple intravenous infusions in healthy adult subjects. Materials and MethodsMaterials and Methods are available in the online-only Supplement. Results Demographics and Baseline Chara...

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“…15 Here, we report for the first time the effects of CSL112 on key biomarkers of RCT after single and multiple intravenous infusions in healthy adult subjects.…”

Section: Gille Et Al Csl112 Enhances Biomarkers Of Rct 2107mentioning

confidence: 85%

mentioning

confidence: 99%

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confidence: 99%

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CSL112 Enhances Biomarkers of Reverse Cholesterol Transport After Single and Multiple Infusions in Healthy Subjects

Gille

Easton

D’Andrea

et al. 2014

ATVB

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112

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“…Plaque volume, however, was reduced in the CSL-111 group compared with baseline ( 39 ). Recent studies show that CSL-112 administration in normal humans signifi cantly increases plasma apoA-I and HDL-C, suggesting an increase in cholesterol effl ux into the plasma compartment ( 40,41 ). apoA-I levels in CSL-112-treated patients remained elevated above baseline for 3 days after treatment ( 41 ).…”

Section: A Peptide-based Approach To Hdl Therapymentioning

confidence: 95%

“…Recent studies show that CSL-112 administration in normal humans signifi cantly increases plasma apoA-I and HDL-C, suggesting an increase in cholesterol effl ux into the plasma compartment ( 40,41 ). apoA-I levels in CSL-112-treated patients remained elevated above baseline for 3 days after treatment ( 41 ). At this time, effects of CSL-112 on atheroma regression have not been reported.…”

Section: A Peptide-based Approach To Hdl Therapymentioning

confidence: 99%

Anti-inflammatory and cholesterol-reducing properties of apolipoprotein mimetics: a review

White

Garber

Anantharamaiah

2014

Journal of Lipid Research

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Nanomedicine for Diagnosis and Treatment of Atherosclerosis

Cheng,

Huang,

Chen

et al. 2023

Advanced Science

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With the changing disease spectrum, atherosclerosis has become increasingly prevalent worldwide and the associated diseases have emerged as the leading cause of death. Due to their fascinating physical, chemical, and biological characteristics, nanomaterials are regarded as a promising tool to tackle enormous challenges in medicine. The emerging discipline of nanomedicine has filled a huge application gap in the atherosclerotic field, ushering a new generation of diagnosis and treatment strategies. Herein, based on the essential pathogenic contributors of atherogenesis, as well as the distinct composition/structural characteristics, synthesis strategies, and surface design of nanoplatforms, the three major application branches (nanodiagnosis, nanotherapy, and nanotheranostic) of nanomedicine in atherosclerosis are elaborated. Then, state‐of‐art studies containing a sequence of representative and significant achievements are summarized in detail with an emphasis on the intrinsic interaction/relationship between nanomedicines and atherosclerosis. Particularly, attention is paid to the biosafety of nanomedicines, which aims to pave the way for future clinical translation of this burgeoning field. Finally, this comprehensive review is concluded by proposing unresolved key scientific issues and sharing the vision and expectation for the future, fully elucidating the closed loop from atherogenesis to the application paradigm of nanomedicines for advancing the early achievement of clinical applications.

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A multiple ascending dose study of CSL112, an infused formulation of ApoA‐I

Cited by 80 publications

References 23 publications

CSL112 Enhances Biomarkers of Reverse Cholesterol Transport After Single and Multiple Infusions in Healthy Subjects

CSL112 Enhances Biomarkers of Reverse Cholesterol Transport After Single and Multiple Infusions in Healthy Subjects

Anti-inflammatory and cholesterol-reducing properties of apolipoprotein mimetics: a review

Nanomedicine for Diagnosis and Treatment of Atherosclerosis

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