Human Immunodeficiency Virus-associated Neurocognitive Impairment in Diverse Resource-limited Settings

AIDS Clinical Trials Group

doi:10.1093/cid/ciy767

Human Immunodeficiency Virus-associated Neurocognitive Impairment in Diverse Resource-limited Settings

AIDS Clinical Trials Group

School of Medicine

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

3 Scopus citations

Abstract

Background. Neurocognitive impairment remains a common complication of human immunodeficiency virus (HIV) despite effective antiretroviral therapy (ART). We previously reported improved neurocognitive functioning with ART initiation in 7 resource-limited countries for HIV+ participants from the AIDS Clinical Trials Group (ACTG) 5199 International Neurological Study (INS). Here, we apply normative data from the International Neurocognitive Normative Study (INNS) to INS to provide previously unknown rates of neurocognitive impairment. Methods. The A5199 INS assessed neurocognitive and neurological performance within a randomized clinical trial with 3 arms containing World Health Organization first-line recommended ART regimens (ACTG 5175; PEARLS). The ACTG 5271 INNS collected normative comparison data on 2400 high-risk HIV-negative participants from 10 voluntary counseling and testing sites aligned with INS. Normative comparison data were used to create impairment ratings for HIV+ participants in INS; associations were estimated using generalized estimating equations. Results. Among 860 HIV+ adults enrolled in ACTG 5199, 55% had no neurocognitive impairment at baseline. Mild neurocognitive impairment was found in 25%, moderate in 17%, and severe in 3% of participants. With the initiation of ART, the estimated odds of impairment were reduced 12% (95% confidence interval, 9%, 14%) for every 24 weeks (P < .0001) on ART. Mild impairment dropped slightly and then remained at about 18% out to week 168. Conclusions. Almost half of HIV+ participants had neurocognitive impairment at baseline before ART, based on local norms. With ART initiation, there were significant overall reductions in neurocognitive impairment over time, especially in those with moderate and severe impairments.

Original language	English (US)
Pages (from-to)	1733-1738
Number of pages	6
Journal	Clinical Infectious Diseases
Volume	68
Issue number	10
DOIs	https://doi.org/10.1093/cid/ciy767
State	Published - May 1 2019

Keywords

Antiretroviral
HIV-associated neurocognitive disorders
International settings
Neurocognitive
Neurology

ASJC Scopus subject areas

Microbiology (medical)
Infectious Diseases

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10.1093/cid/ciy767

Cite this

@article{bee8b7781df2434e9b61ffae737248ae,

title = "Human Immunodeficiency Virus-associated Neurocognitive Impairment in Diverse Resource-limited Settings",

abstract = "Background. Neurocognitive impairment remains a common complication of human immunodeficiency virus (HIV) despite effective antiretroviral therapy (ART). We previously reported improved neurocognitive functioning with ART initiation in 7 resource-limited countries for HIV+ participants from the AIDS Clinical Trials Group (ACTG) 5199 International Neurological Study (INS). Here, we apply normative data from the International Neurocognitive Normative Study (INNS) to INS to provide previously unknown rates of neurocognitive impairment. Methods. The A5199 INS assessed neurocognitive and neurological performance within a randomized clinical trial with 3 arms containing World Health Organization first-line recommended ART regimens (ACTG 5175; PEARLS). The ACTG 5271 INNS collected normative comparison data on 2400 high-risk HIV-negative participants from 10 voluntary counseling and testing sites aligned with INS. Normative comparison data were used to create impairment ratings for HIV+ participants in INS; associations were estimated using generalized estimating equations. Results. Among 860 HIV+ adults enrolled in ACTG 5199, 55% had no neurocognitive impairment at baseline. Mild neurocognitive impairment was found in 25%, moderate in 17%, and severe in 3% of participants. With the initiation of ART, the estimated odds of impairment were reduced 12% (95% confidence interval, 9%, 14%) for every 24 weeks (P < .0001) on ART. Mild impairment dropped slightly and then remained at about 18% out to week 168. Conclusions. Almost half of HIV+ participants had neurocognitive impairment at baseline before ART, based on local norms. With ART initiation, there were significant overall reductions in neurocognitive impairment over time, especially in those with moderate and severe impairments.",

keywords = "Antiretroviral, HIV-associated neurocognitive disorders, International settings, Neurocognitive, Neurology",

author = "{AIDS Clinical Trials Group} and Robertson, {Kevin R.} and Hongyu Jiang and Johnstone Kumwenda and Khuanchai Supparatpinyo and Marra, {Christina M.} and Baiba Berzins and James Hakim and Ned Sacktor and Campbell, {Thomas B.} and Jeffrey Schouten and Katie Mollan and Srikanth Tripathy and Nagalingeswaran Kumarasamy and Rosa, {Alberto La} and Breno Santos and Silva, {Marcus T.} and Cecilia Kanyama and Cindy Firhnhaber and Robert Murphy and Colin Hall and Cheryl Marcus and Linda Naini and Reena Masih and Hosseinipour, {Mina C.} and Rosie Mngqibisa and Sharlaa Badal-Faesen and Sarah Yosief and Alyssa Vecchio and Apsara Nair",

note = "Funding Information: Potential conflicts of interest. J. S. (Clinical Trials Unit [CTU] grant UM1 AI069481-08). T. B. C., M.D. grant support from NIAID AIDS CTU # AI069450. reports grants from NIH, during the conduct of the study; personal fees from Gilead, personal fees from ViiV, personal fees from Theratechnologies, outside the submitted work. Deise Vieira M.D. and M. T. S., M.D. – PhD-IPEC-FIOCRUZ (Site 12101) Rio de Janeiro, Brazil, CTU Grant # AI69476 N. K., M.B.B.S., Ph.D. and Jabin Sharma-YRGCARE Medical Centre (Site 11701) CTU Grant # AI069432 Virginia M. Kayoyo, Franklin D. Kilembe, M.Ph. Mitch Matoga MBBS, M. C. H., M.D. University of North Carolina Project, Kamuzu Central Hospital, Lilongwe (Site 12001) CTU Grant # AI069518 Mauleen Waison and Rachel Mahachi-Parirenyatwa CRS (Site 30313) CTU Grant # BRS-ACURE-Q-08-00173-TOOI-OOO Cynthia Firnhaber, M.D. and Daphne S. Radebe, B.A. - Wits HIV Clinical Research Site (Helen Joseph Hosp) (Site 11101) CTU Grant# AI069463; BRS-ACURE-Q-07-00143 T006 Thira Sirisanthana, M.D. and Daralak Tavornprasit-Research Institute for Health Sciences-Chiang Mai University (Site 11501) CTU Grant # AI069399; AACTG.27.5199.06 Maria Siliprandi, M.D. and Renata Londero,M.D. -Hospital Nossa Senhora da Conceicao CRS (Site 12201) CTU Grant # 5 U01 AI069401 Anjali A. Joglekar, M.B.B.S. and S. T., M.D., M.B.B.S.-NARI Pune CRS (Site 11601) CTU Grant # 5U01AI069417-03 Jorge Sanchez, MD, MPH, and Juan Carlos Hurtado, M.D. - Asociaci{\'o}n Civil Impacta Salud y Educaci{\'o}n (Site 11301) CTU Grant # AI069438; BRS-ACURE-Q-08-00007-T-002 Manisha V. Ghate, M.B.B.S., D.C.H. and Madhura Nene, M.B.B.S. - NARI-NIV Clinic (Site 11603) CTU Grant # 5U01AI069417-03 Dr Raman Gnagakhedkar and Usha Katti, M.B.B.S.-Dr Kotnis Dispensary, NARI (Site 11602) CTU Grant # 5U01AI069417-03 Umesh Lalloo, M.D., F.R.C.P. and R. M., MB ChB –Durban, South Africa Adult HIV CRS (Site 11201) CTU Grant # 5U01AI069426-03 Ben Kalonga and Henry Chamba-Blantyre College of Medicine, Malawi-Johns Hopkins Project (Site 30301) CTU Grant # U01A1069518 Carlos Mosquera, M.D., and Rosa Infante, M.D.-INMENSA-Lince CRS Lima, Peru (Site 11302) CTU Grant # 5U01 AI069438-03; BRS-ACURE-Q-07-00141-T001-001 H. J. was funded in part by the Statistical and Data Management Center of the Adult AIDS Clinical Trials Group grant 1 U01 068634. K. M. reports grants from NIH, during the conduct of the study; grants from Merck, outside the submitted work. K. R. R. reports non-financial support from ViiV, personal fees from ViiV, outside the submitted work; K. S. reports grants from NIH, during the conduct of the study; A. L. R. reports grants from National Institute of Allergy and Infectious Diseases, during the conduct of the study; personal fees from MSD Peru, outside the submitted work; R. M. reports grants from NIH/NIAID, during the conduct of the study. N. K. reports a grant from the NIH. Funding Information: Financial support. The project described was supported by the NIAID (award U01AI068636) and by NIMH, National Institute of Dental and Craniofacial Research, and Statistical and Data Analysis Center (grant AI-068634). This work was also a part of ACTG DR005, which was partially supported by the University of North Carolina at Chapel Hill Center for AIDS Research (P30 AI50410) for work by K. M. Publisher Copyright: {\textcopyright} The Author(s) 2018. Published by Oxford University Press for the Infectious Diseases Society of America. All rights",

year = "2019",

month = may,

day = "1",

doi = "10.1093/cid/ciy767",

language = "English (US)",

volume = "68",

pages = "1733--1738",

journal = "Clinical Infectious Diseases",

issn = "1058-4838",

publisher = "Oxford University Press",

number = "10",

}

TY - JOUR

T1 - Human Immunodeficiency Virus-associated Neurocognitive Impairment in Diverse Resource-limited Settings

AU - AIDS Clinical Trials Group

AU - Robertson, Kevin R.

AU - Jiang, Hongyu

AU - Kumwenda, Johnstone

AU - Supparatpinyo, Khuanchai

AU - Marra, Christina M.

AU - Berzins, Baiba

AU - Hakim, James

AU - Sacktor, Ned

AU - Campbell, Thomas B.

AU - Schouten, Jeffrey

AU - Mollan, Katie

AU - Tripathy, Srikanth

AU - Kumarasamy, Nagalingeswaran

AU - Rosa, Alberto La

AU - Santos, Breno

AU - Silva, Marcus T.

AU - Kanyama, Cecilia

AU - Firhnhaber, Cindy

AU - Murphy, Robert

AU - Hall, Colin

AU - Marcus, Cheryl

AU - Naini, Linda

AU - Masih, Reena

AU - Hosseinipour, Mina C.

AU - Mngqibisa, Rosie

AU - Badal-Faesen, Sharlaa

AU - Yosief, Sarah

AU - Vecchio, Alyssa

AU - Nair, Apsara

N1 - Funding Information: Potential conflicts of interest. J. S. (Clinical Trials Unit [CTU] grant UM1 AI069481-08). T. B. C., M.D. grant support from NIAID AIDS CTU # AI069450. reports grants from NIH, during the conduct of the study; personal fees from Gilead, personal fees from ViiV, personal fees from Theratechnologies, outside the submitted work. Deise Vieira M.D. and M. T. S., M.D. – PhD-IPEC-FIOCRUZ (Site 12101) Rio de Janeiro, Brazil, CTU Grant # AI69476 N. K., M.B.B.S., Ph.D. and Jabin Sharma-YRGCARE Medical Centre (Site 11701) CTU Grant # AI069432 Virginia M. Kayoyo, Franklin D. Kilembe, M.Ph. Mitch Matoga MBBS, M. C. H., M.D. University of North Carolina Project, Kamuzu Central Hospital, Lilongwe (Site 12001) CTU Grant # AI069518 Mauleen Waison and Rachel Mahachi-Parirenyatwa CRS (Site 30313) CTU Grant # BRS-ACURE-Q-08-00173-TOOI-OOO Cynthia Firnhaber, M.D. and Daphne S. Radebe, B.A. - Wits HIV Clinical Research Site (Helen Joseph Hosp) (Site 11101) CTU Grant# AI069463; BRS-ACURE-Q-07-00143 T006 Thira Sirisanthana, M.D. and Daralak Tavornprasit-Research Institute for Health Sciences-Chiang Mai University (Site 11501) CTU Grant # AI069399; AACTG.27.5199.06 Maria Siliprandi, M.D. and Renata Londero,M.D. -Hospital Nossa Senhora da Conceicao CRS (Site 12201) CTU Grant # 5 U01 AI069401 Anjali A. Joglekar, M.B.B.S. and S. T., M.D., M.B.B.S.-NARI Pune CRS (Site 11601) CTU Grant # 5U01AI069417-03 Jorge Sanchez, MD, MPH, and Juan Carlos Hurtado, M.D. - Asociación Civil Impacta Salud y Educación (Site 11301) CTU Grant # AI069438; BRS-ACURE-Q-08-00007-T-002 Manisha V. Ghate, M.B.B.S., D.C.H. and Madhura Nene, M.B.B.S. - NARI-NIV Clinic (Site 11603) CTU Grant # 5U01AI069417-03 Dr Raman Gnagakhedkar and Usha Katti, M.B.B.S.-Dr Kotnis Dispensary, NARI (Site 11602) CTU Grant # 5U01AI069417-03 Umesh Lalloo, M.D., F.R.C.P. and R. M., MB ChB –Durban, South Africa Adult HIV CRS (Site 11201) CTU Grant # 5U01AI069426-03 Ben Kalonga and Henry Chamba-Blantyre College of Medicine, Malawi-Johns Hopkins Project (Site 30301) CTU Grant # U01A1069518 Carlos Mosquera, M.D., and Rosa Infante, M.D.-INMENSA-Lince CRS Lima, Peru (Site 11302) CTU Grant # 5U01 AI069438-03; BRS-ACURE-Q-07-00141-T001-001 H. J. was funded in part by the Statistical and Data Management Center of the Adult AIDS Clinical Trials Group grant 1 U01 068634. K. M. reports grants from NIH, during the conduct of the study; grants from Merck, outside the submitted work. K. R. R. reports non-financial support from ViiV, personal fees from ViiV, outside the submitted work; K. S. reports grants from NIH, during the conduct of the study; A. L. R. reports grants from National Institute of Allergy and Infectious Diseases, during the conduct of the study; personal fees from MSD Peru, outside the submitted work; R. M. reports grants from NIH/NIAID, during the conduct of the study. N. K. reports a grant from the NIH. Funding Information: Financial support. The project described was supported by the NIAID (award U01AI068636) and by NIMH, National Institute of Dental and Craniofacial Research, and Statistical and Data Analysis Center (grant AI-068634). This work was also a part of ACTG DR005, which was partially supported by the University of North Carolina at Chapel Hill Center for AIDS Research (P30 AI50410) for work by K. M. Publisher Copyright: © The Author(s) 2018. Published by Oxford University Press for the Infectious Diseases Society of America. All rights

PY - 2019/5/1

Y1 - 2019/5/1

N2 - Background. Neurocognitive impairment remains a common complication of human immunodeficiency virus (HIV) despite effective antiretroviral therapy (ART). We previously reported improved neurocognitive functioning with ART initiation in 7 resource-limited countries for HIV+ participants from the AIDS Clinical Trials Group (ACTG) 5199 International Neurological Study (INS). Here, we apply normative data from the International Neurocognitive Normative Study (INNS) to INS to provide previously unknown rates of neurocognitive impairment. Methods. The A5199 INS assessed neurocognitive and neurological performance within a randomized clinical trial with 3 arms containing World Health Organization first-line recommended ART regimens (ACTG 5175; PEARLS). The ACTG 5271 INNS collected normative comparison data on 2400 high-risk HIV-negative participants from 10 voluntary counseling and testing sites aligned with INS. Normative comparison data were used to create impairment ratings for HIV+ participants in INS; associations were estimated using generalized estimating equations. Results. Among 860 HIV+ adults enrolled in ACTG 5199, 55% had no neurocognitive impairment at baseline. Mild neurocognitive impairment was found in 25%, moderate in 17%, and severe in 3% of participants. With the initiation of ART, the estimated odds of impairment were reduced 12% (95% confidence interval, 9%, 14%) for every 24 weeks (P < .0001) on ART. Mild impairment dropped slightly and then remained at about 18% out to week 168. Conclusions. Almost half of HIV+ participants had neurocognitive impairment at baseline before ART, based on local norms. With ART initiation, there were significant overall reductions in neurocognitive impairment over time, especially in those with moderate and severe impairments.

AB - Background. Neurocognitive impairment remains a common complication of human immunodeficiency virus (HIV) despite effective antiretroviral therapy (ART). We previously reported improved neurocognitive functioning with ART initiation in 7 resource-limited countries for HIV+ participants from the AIDS Clinical Trials Group (ACTG) 5199 International Neurological Study (INS). Here, we apply normative data from the International Neurocognitive Normative Study (INNS) to INS to provide previously unknown rates of neurocognitive impairment. Methods. The A5199 INS assessed neurocognitive and neurological performance within a randomized clinical trial with 3 arms containing World Health Organization first-line recommended ART regimens (ACTG 5175; PEARLS). The ACTG 5271 INNS collected normative comparison data on 2400 high-risk HIV-negative participants from 10 voluntary counseling and testing sites aligned with INS. Normative comparison data were used to create impairment ratings for HIV+ participants in INS; associations were estimated using generalized estimating equations. Results. Among 860 HIV+ adults enrolled in ACTG 5199, 55% had no neurocognitive impairment at baseline. Mild neurocognitive impairment was found in 25%, moderate in 17%, and severe in 3% of participants. With the initiation of ART, the estimated odds of impairment were reduced 12% (95% confidence interval, 9%, 14%) for every 24 weeks (P < .0001) on ART. Mild impairment dropped slightly and then remained at about 18% out to week 168. Conclusions. Almost half of HIV+ participants had neurocognitive impairment at baseline before ART, based on local norms. With ART initiation, there were significant overall reductions in neurocognitive impairment over time, especially in those with moderate and severe impairments.

KW - Antiretroviral

KW - HIV-associated neurocognitive disorders

KW - International settings

KW - Neurocognitive

KW - Neurology

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UR - http://www.scopus.com/inward/citedby.url?scp=85064392473&partnerID=8YFLogxK

U2 - 10.1093/cid/ciy767

DO - 10.1093/cid/ciy767

M3 - Article

C2 - 30219843

AN - SCOPUS:85064392473

SN - 1058-4838

VL - 68

SP - 1733

EP - 1738

JO - Clinical Infectious Diseases

JF - Clinical Infectious Diseases

IS - 10

ER -

Human Immunodeficiency Virus-associated Neurocognitive Impairment in Diverse Resource-limited Settings

Abstract

Keywords

ASJC Scopus subject areas

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