Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration

David Croteau; Steven S. Rossi; Brookie M. Best; Edmund Capparelli; Ronald J. Ellis; David B. Clifford; Ann C. Collier; Benjamin B. Gelman; Christina M. Marra; Justin Mcarthur; J. Allen Mccutchan; Susan Morgello; David M. Simpson; Igor Grant; Scott Letendre

doi:10.1093/jac/dks441

Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration

David Croteau, Steven S. Rossi, Brookie M. Best, Edmund Capparelli, Ronald J. Ellis, David B. Clifford, Ann C. Collier, Benjamin B. Gelman, Christina M. Marra, Justin Mcarthur, J. Allen Mccutchan, Susan Morgello, David M. Simpson, Igor Grant, Scott Letendre

School of Medicine

Research output: Contribution to journal › Article › peer-review

28 Scopus citations

Abstract

Objectives: Higher CSF antiretroviral concentrations may be associated with better control of HIV replication and neurocognitive performance, but only the unbound fraction of antiretrovirals is available to inhibit HIV. Therefore, the objective of this study was to determine total and unbound darunavir concentrations in CSF and compare findings with plasma concentrations as well as the wild-type HIV-1 90% inhibitory concentration (IC. ₉₀). Methods: Subjects with HIV infection were selected based on the use of darunavir-containing regimens with a twice-daily dosing schedule and availability of stored CSF and matched plasma. Total darunavir was measured by HPLC for plasma or liquid chromatography-tandem mass spectroscopy (LC/MS/MS) for CSF. Plasma unbound darunavir was measured by ultrafiltration and LC/MS/MS. CSF protein binding was determined by competitive binding exchange with radiolabelled darunavir. Results: Twenty-nine matched CSF-plasma pairs were analysed and darunavir was detected in all CSF specimens (median total concentration 55.8 ng/mL), with a CSF unbound fraction of 93.5%. Median fractional penetrance was 1.4% of median total and 9.4% of median unbound plasma concentrations. Unbound darunavir concentrations in CSF exceeded the median IC. ₉₀ for wild-type HIV in all subjects by a median of 20.6-fold, despite the relatively low fractional penetrance. Total darunavir concentrations in CSF correlated with both total and unbound darunavir concentrations in plasma. Conclusions: Darunavir should contribute to the control of HIV replication in the CNS as a component of effective combination antiretroviral regimens.

Original language	English (US)
Pages (from-to)	684-689
Number of pages	6
Journal	Journal of Antimicrobial Chemotherapy
Volume	68
Issue number	3
DOIs	https://doi.org/10.1093/jac/dks441
State	Published - Mar 2013

Keywords

Antiretroviral therapy
Central nervous system
HIV
Protein binding

ASJC Scopus subject areas

Pharmacology
Microbiology (medical)
Pharmacology (medical)
Infectious Diseases

Access to Document

10.1093/jac/dks441

Cite this

Croteau, D., Rossi, S. S., Best, B. M., Capparelli, E., Ellis, R. J., Clifford, D. B., Collier, A. C., Gelman, B. B., Marra, C. M., Mcarthur, J., Mccutchan, J. A., Morgello, S., Simpson, D. M., Grant, I., & Letendre, S. (2013). Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration. Journal of Antimicrobial Chemotherapy, 68(3), 684-689. https://doi.org/10.1093/jac/dks441

Croteau, D, Rossi, SS, Best, BM, Capparelli, E, Ellis, RJ, Clifford, DB, Collier, AC, Gelman, BB, Marra, CM, Mcarthur, J, Mccutchan, JA, Morgello, S, Simpson, DM, Grant, I & Letendre, S 2013, 'Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration', Journal of Antimicrobial Chemotherapy, vol. 68, no. 3, pp. 684-689. https://doi.org/10.1093/jac/dks441

@article{2317fc62dd9a49a2bb8721eb35a02cad,

title = "Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration",

abstract = "Objectives: Higher CSF antiretroviral concentrations may be associated with better control of HIV replication and neurocognitive performance, but only the unbound fraction of antiretrovirals is available to inhibit HIV. Therefore, the objective of this study was to determine total and unbound darunavir concentrations in CSF and compare findings with plasma concentrations as well as the wild-type HIV-1 90% inhibitory concentration (IC. 90). Methods: Subjects with HIV infection were selected based on the use of darunavir-containing regimens with a twice-daily dosing schedule and availability of stored CSF and matched plasma. Total darunavir was measured by HPLC for plasma or liquid chromatography-tandem mass spectroscopy (LC/MS/MS) for CSF. Plasma unbound darunavir was measured by ultrafiltration and LC/MS/MS. CSF protein binding was determined by competitive binding exchange with radiolabelled darunavir. Results: Twenty-nine matched CSF-plasma pairs were analysed and darunavir was detected in all CSF specimens (median total concentration 55.8 ng/mL), with a CSF unbound fraction of 93.5%. Median fractional penetrance was 1.4% of median total and 9.4% of median unbound plasma concentrations. Unbound darunavir concentrations in CSF exceeded the median IC. 90 for wild-type HIV in all subjects by a median of 20.6-fold, despite the relatively low fractional penetrance. Total darunavir concentrations in CSF correlated with both total and unbound darunavir concentrations in plasma. Conclusions: Darunavir should contribute to the control of HIV replication in the CNS as a component of effective combination antiretroviral regimens.",

keywords = "Antiretroviral therapy, Central nervous system, HIV, Protein binding",

author = "David Croteau and Rossi, {Steven S.} and Best, {Brookie M.} and Edmund Capparelli and Ellis, {Ronald J.} and Clifford, {David B.} and Collier, {Ann C.} and Gelman, {Benjamin B.} and Marra, {Christina M.} and Justin Mcarthur and Mccutchan, {J. Allen} and Susan Morgello and Simpson, {David M.} and Igor Grant and Scott Letendre",

note = "Funding Information: This work was supported by an investigator-initiated research grant from Tibotec and by the National Institutes of Health via the following awards: N01 MH22005, HHSN271201000030C and HHSN271201000036C. Funding Information: R. J. E. received consultant fees from NeurogesX and is funded by NIH grants R01MH058076, U01MH83506, P30MH62512, R01MH83552, P50DA26306, R01MH095621 and 2U01NS32228. D. B. C. is supported by NIH grants NS32228, AI69495, MH22005, DA022137, MH058076 and 3857-53187. He has also received support from Pfizer, NeurogesX and Biogen. In addition, he has provided scientific advisory or consulting to Biogen Idec, Elan, Roche, Genentech, GlaxoSmithKline, Janssen, Millennium, Bristol-Myers Squibb, Genzyme, Wyeth and Pfizer. A. C. C. had the following disclosures: research support from Boehringer-Ingelheim (past), Gilead Sciences (past), Koronis (past), Merck & Company (current), Schering-Plough (past) and Tibotec-Virco (past); former member of a Data, Safety and Monitoring Board for a Merck-sponsored study; attendee at Advisory Board Meetings for GlaxoSmithKline (past) and Pfizer (past); and stock ownership (personal/immediate family member) with Abbott Laboratories, Bristol-Myers Squibb, Johnson and Johnson, and Pfizer. B. B. G. receives support from NIH grants NS072005 and MH79886. C. M. M. receives research support from the NIH (NINDS and NIMH). She receives royalties from Lippincott Williams and Wilkins and from UptoDate. J. M. receives support from N01 MH22005. J. A. M. authors chapters on HIV for the Merck Manual and receives related research funding from NIH P30 MH62512, NIH U01 MH83506, NIH/Centers for Disease Control and Prevention (CDC) U2G PS00623, NIH U01 AI69432, NIH N01 MH22005, NIH K30 RR22681, NIH R01 MH58076 and NIH U13 MH81676. D. M. S. receives research support from the NIH (NINDS and NIMH). He provided consultancy to GlaxoSmithKline and Gilead. I. G. receives ongoing research support from NIH P30 MH62512, NIH P50 DA26306, NIH P01 DA12065, NIH N01 MH22005, NIH U01 MH83506, NIH R01 MH78748, NIH R01 AG15301, NIH R01 MH83552 and NIH/University of Nebraska P01 DA026146. He has also received honoraria from Abbott Pharmaceuticals as part of their Educational Speaker Program. The salary of S. L. was funded by NIH research awards, including N01 MH22005, R01 MH58076, R01 MH92225, P50 DA26306 and P30 MH62512. He has received support for research projects from Abbott, Merck, Tibotec and GlaxoSmithKline. He has consulted for Gilead Sciences, GlaxoSmithKline, Merck and Tibotec, and has received lecture honoraria from Abbott and Boehringer-Ingelheim. The remaining authors have none to declare.",

year = "2013",

month = mar,

doi = "10.1093/jac/dks441",

language = "English (US)",

volume = "68",

pages = "684--689",

journal = "Journal of Antimicrobial Chemotherapy",

issn = "0305-7453",

publisher = "Oxford University Press",

number = "3",

}

TY - JOUR

T1 - Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration

AU - Croteau, David

AU - Rossi, Steven S.

AU - Best, Brookie M.

AU - Capparelli, Edmund

AU - Ellis, Ronald J.

AU - Clifford, David B.

AU - Collier, Ann C.

AU - Gelman, Benjamin B.

AU - Marra, Christina M.

AU - Mcarthur, Justin

AU - Mccutchan, J. Allen

AU - Morgello, Susan

AU - Simpson, David M.

AU - Grant, Igor

AU - Letendre, Scott

N1 - Funding Information: This work was supported by an investigator-initiated research grant from Tibotec and by the National Institutes of Health via the following awards: N01 MH22005, HHSN271201000030C and HHSN271201000036C. Funding Information: R. J. E. received consultant fees from NeurogesX and is funded by NIH grants R01MH058076, U01MH83506, P30MH62512, R01MH83552, P50DA26306, R01MH095621 and 2U01NS32228. D. B. C. is supported by NIH grants NS32228, AI69495, MH22005, DA022137, MH058076 and 3857-53187. He has also received support from Pfizer, NeurogesX and Biogen. In addition, he has provided scientific advisory or consulting to Biogen Idec, Elan, Roche, Genentech, GlaxoSmithKline, Janssen, Millennium, Bristol-Myers Squibb, Genzyme, Wyeth and Pfizer. A. C. C. had the following disclosures: research support from Boehringer-Ingelheim (past), Gilead Sciences (past), Koronis (past), Merck & Company (current), Schering-Plough (past) and Tibotec-Virco (past); former member of a Data, Safety and Monitoring Board for a Merck-sponsored study; attendee at Advisory Board Meetings for GlaxoSmithKline (past) and Pfizer (past); and stock ownership (personal/immediate family member) with Abbott Laboratories, Bristol-Myers Squibb, Johnson and Johnson, and Pfizer. B. B. G. receives support from NIH grants NS072005 and MH79886. C. M. M. receives research support from the NIH (NINDS and NIMH). She receives royalties from Lippincott Williams and Wilkins and from UptoDate. J. M. receives support from N01 MH22005. J. A. M. authors chapters on HIV for the Merck Manual and receives related research funding from NIH P30 MH62512, NIH U01 MH83506, NIH/Centers for Disease Control and Prevention (CDC) U2G PS00623, NIH U01 AI69432, NIH N01 MH22005, NIH K30 RR22681, NIH R01 MH58076 and NIH U13 MH81676. D. M. S. receives research support from the NIH (NINDS and NIMH). He provided consultancy to GlaxoSmithKline and Gilead. I. G. receives ongoing research support from NIH P30 MH62512, NIH P50 DA26306, NIH P01 DA12065, NIH N01 MH22005, NIH U01 MH83506, NIH R01 MH78748, NIH R01 AG15301, NIH R01 MH83552 and NIH/University of Nebraska P01 DA026146. He has also received honoraria from Abbott Pharmaceuticals as part of their Educational Speaker Program. The salary of S. L. was funded by NIH research awards, including N01 MH22005, R01 MH58076, R01 MH92225, P50 DA26306 and P30 MH62512. He has received support for research projects from Abbott, Merck, Tibotec and GlaxoSmithKline. He has consulted for Gilead Sciences, GlaxoSmithKline, Merck and Tibotec, and has received lecture honoraria from Abbott and Boehringer-Ingelheim. The remaining authors have none to declare.

PY - 2013/3

Y1 - 2013/3

N2 - Objectives: Higher CSF antiretroviral concentrations may be associated with better control of HIV replication and neurocognitive performance, but only the unbound fraction of antiretrovirals is available to inhibit HIV. Therefore, the objective of this study was to determine total and unbound darunavir concentrations in CSF and compare findings with plasma concentrations as well as the wild-type HIV-1 90% inhibitory concentration (IC. 90). Methods: Subjects with HIV infection were selected based on the use of darunavir-containing regimens with a twice-daily dosing schedule and availability of stored CSF and matched plasma. Total darunavir was measured by HPLC for plasma or liquid chromatography-tandem mass spectroscopy (LC/MS/MS) for CSF. Plasma unbound darunavir was measured by ultrafiltration and LC/MS/MS. CSF protein binding was determined by competitive binding exchange with radiolabelled darunavir. Results: Twenty-nine matched CSF-plasma pairs were analysed and darunavir was detected in all CSF specimens (median total concentration 55.8 ng/mL), with a CSF unbound fraction of 93.5%. Median fractional penetrance was 1.4% of median total and 9.4% of median unbound plasma concentrations. Unbound darunavir concentrations in CSF exceeded the median IC. 90 for wild-type HIV in all subjects by a median of 20.6-fold, despite the relatively low fractional penetrance. Total darunavir concentrations in CSF correlated with both total and unbound darunavir concentrations in plasma. Conclusions: Darunavir should contribute to the control of HIV replication in the CNS as a component of effective combination antiretroviral regimens.

AB - Objectives: Higher CSF antiretroviral concentrations may be associated with better control of HIV replication and neurocognitive performance, but only the unbound fraction of antiretrovirals is available to inhibit HIV. Therefore, the objective of this study was to determine total and unbound darunavir concentrations in CSF and compare findings with plasma concentrations as well as the wild-type HIV-1 90% inhibitory concentration (IC. 90). Methods: Subjects with HIV infection were selected based on the use of darunavir-containing regimens with a twice-daily dosing schedule and availability of stored CSF and matched plasma. Total darunavir was measured by HPLC for plasma or liquid chromatography-tandem mass spectroscopy (LC/MS/MS) for CSF. Plasma unbound darunavir was measured by ultrafiltration and LC/MS/MS. CSF protein binding was determined by competitive binding exchange with radiolabelled darunavir. Results: Twenty-nine matched CSF-plasma pairs were analysed and darunavir was detected in all CSF specimens (median total concentration 55.8 ng/mL), with a CSF unbound fraction of 93.5%. Median fractional penetrance was 1.4% of median total and 9.4% of median unbound plasma concentrations. Unbound darunavir concentrations in CSF exceeded the median IC. 90 for wild-type HIV in all subjects by a median of 20.6-fold, despite the relatively low fractional penetrance. Total darunavir concentrations in CSF correlated with both total and unbound darunavir concentrations in plasma. Conclusions: Darunavir should contribute to the control of HIV replication in the CNS as a component of effective combination antiretroviral regimens.

KW - Antiretroviral therapy

KW - Central nervous system

KW - HIV

KW - Protein binding

UR - http://www.scopus.com/inward/record.url?scp=84873600385&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=84873600385&partnerID=8YFLogxK

U2 - 10.1093/jac/dks441

DO - 10.1093/jac/dks441

M3 - Article

C2 - 23143899

AN - SCOPUS:84873600385

SN - 0305-7453

VL - 68

SP - 684

EP - 689

JO - Journal of Antimicrobial Chemotherapy

JF - Journal of Antimicrobial Chemotherapy

IS - 3

ER -

Darunavir is predominantly unbound to protein in cerebrospinal fluid and concentrations exceed the wild-type HIV-1 median 90% inhibitory concentration

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this