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A Clinical Trial of CCR5 Inhibition
     in Treated HIV Infection:
 Highlighting Multidisciplinary T1 Research
            from the SFGH CRS

               Peter W. Hunt, M.D.
         Assistant Professor in Residence
         UCSF, SFGH HIV/AIDS Division
SFGH CRC:
Aā€œHubā€ for Multidisciplinary T1 Research
                      Clinical Trials
                      Hunt, Hatano,
                      Hsue, Deeks       Cardiovascular
     SCOPE Cohort                        (FMD, IMT, etc)
      Deeks/Martin                           Hsue

                                                     Lymph Node
Gut Mucosal
                                                       Biopsy
Biospy Core                                             Hatano
Somsouk/Hunt

                        SFGH                            Neurology
                                                     (CSF Biomarkers)
  Specimen
    Bank
                        CRC                                Price

     ASB                                                Basic
                                                     Laboratories
                                                     McCune/Nixon
        Virology
        Core Lab                        Immunology
           Liegler                        Core Lab
                                          Sinclair
                      Clinical Lab
HIV+ Patients Still Have a 10y Shorter Life
         Expectancy than HIV- Controls
                                                    Survival from Age 25 Years
                                                              N= 3,990
                                1
    Probability of Survival




                              0.75                                                                 Population
                                                                                                   controls


                               0.5

                                                                                                      Late HAART
                                                                                                      (2000ā€“2005)
                              0.25
                                                                                                      Early HAART
                                                                                                      (1997ā€“1999)
                                                                                                      Pre-HAART
                                0                                                                     (1995ā€“1996)
                                     25   30   35     40    45    50    55       60     65       70
                                                                   Age, years
Adapted from Lohse N, et al. Ann Intern Med 2007;146:87ā€“95             (See Also: ART-CC, Lancet, 2008; Lewden, JAIDS, 2007)
Many morbidities associated with
       aging also appear to be increased in
               treated HIV disease
   ā€¢ Cardiovascular disease [1-3]
   ā€¢ Cancer (non-AIDS) [4]
   ā€¢ Bone fractures / osteoporosis [5,6]
   ā€¢ Liver disease [7]
   ā€¢ Kidney disease [8]
   ā€¢ Cognitive decline [9]
   ā€¢ Frailty [10]
1. Klein D, et al. J Acquir Immune Defic Syndr. 2002;30:471-477. 2; Hsue P, et al. Circulation. 2004;109:316-319. 3. Grinspoon SK,
et al. Circulation. 2008;118:198-210. 4. Patel P, et al. Ann Int Med, 2008;148:728-736. 5. Triant V, et al. J Clin Endocrinol Metab.
2008;93:3499-3504. 6. Arnsten JH, et al. AIDS. 2007 ;21:617-623. 7. Odden MC, et al. Arch Intern Med. 2007;167:2213-2219. 8.
Choi A, et al. AIDS, 2009;23(16):2143-49. 9. McCutchan JA, et a. AIDS. 2007 ;21:1109-1117. 10. Desquilbet L, et al. J Gerontol A
Biol Sci Med Sci. 2007;62:1279-1286
Many Chronic Diseases of Aging May Be
Driven By Lifestyle Factors and ART Toxicity




                ART
               Toxicity
                                       Premature
                                         Aging
 Lifestyle
 (smoking, etc.)




                          Deeks and Phillips, BMJ, 2009
Persistent Immune Activation and
Inflammation May Also Play Important Role




        ART
       Toxicity
                                       Premature
                                         Aging

 Lifestyle
             Persistent
           Inflammation


                          Deeks and Phillips, BMJ, 2009
An Important Clue from Nature




Sooty Mangabey                      Rhesus Macaque
ā€¢Infect with SIV                    ā€¢Infect with SIV
ā€¢High Levels of Viral Replication   ā€¢High Levels of Viral Replication
ā€¢No AIDS, normal lifespan           ā€¢AIDS and death
ā€¢Minimal Immune Activation             ā€¢Massive Immune Activation
                        Silvestri, Immunity, 2003
T Cell Activation Declines with ART




            Hunt et al, JID, 2003 and 2008
But Remains Abnormally High During
  ART-mediated Viral Suppresion




           Hunt et al, JID, 2003 and 2008
CCR5 Inhibition:
     A Potential Intervention to Reduce T Cell Activation

ā€¢ Maraviroc is a CCR5 inhibitor and the only currently approved
  ARV drug that targets a host element.
ā€¢ In addition to blocking HIV entry, maraviroc blocks binding of
  natural CCR5 ligands.
   ā€“ Contribute to T cell and monocyte trafficking and activation

ā€¢ Potential immunologic benefit to blocking CCR5 supported by:
   ā€“ CCR5 āˆ†32 causes delayed HIV disease progression.
   ā€“ Natural hosts of non-pathogenic SIV have low CCR5 on central
     memory T cells and low T cell activation.
ā€¢ Hypothesis: Adding maraviroc to a suppressive regimen will
  decrease T cell activation in treated HIV infection
Maraviroc Intensification Trial
               Schematic

   Randomize                                                      ART alone
     (N=42)              Add Maraviroc BID x 24 weeks           x 12 weeks
     ART>1y
     VL<75                                                      ART alone
    CD4<350
                           Add Placebo BID x 24 weeks           x 12 weeks


Study Visits at Weeks: -2 0 1 2 4 6 8      12    16    20 22 24      28   36

        T Cell Activation, biomarkers, Low-level Viremia (SCA), FMD (Cardiovascular)
        Clinical monitoring, CD4 count
        Flexible Sigmoidoscopy, Rectosigmoid Biopsy (UCSF only)
CCR5 Expression is Much More Common
     on T Cells in Rectal Mucosa
Baseline Characteristics
                                                 Placebo           Maraviroc
Characteristic                                   Median (IQR)       Median (IQR)
                                                    N=22               N=23

Age, years                                      50 (43 to 57)      50 (46 to 56)

Male Gender, No. (%)                               20 (91)           23 (100)

CD4 count, cells/mm3                           202 (161 to 256)   206 (131 to 260)

Plasma HIV RNA level, copies/ml                      <48                <48

Duration of current ART regimen, months         31 (15 to 43)      30 (21 to 42)

Hepatitis C Virus Antibody Positive, No. (%)        2 (14)             3 (20)
Early Decline in Plasma HIV RNA Levels
  by Single Copy Assay in Both Arms
Similar CD4 Count Increase in Both Arms




     No evidence for difference in the rate of
    CD4+ T cell recovery between arms, P=0.97
CD8+ T Cell Activation Declined
Significantly in the Placebo Arm
While CD8+ T Cell Activation Tended
 to Increase in the Maraviroc Arm
Maraviroc Increases CD8 Activation
      Compared to Placebo




      P values represent difference between groups
      in the change from baseline at each timepoint.
Maraviroc Prevents the Decline in CD4
  Activation Compared to Placebo




          P values represent difference between groups in
            the change from baseline at each timepoint.
No Change in Rectal T Cell Activation on Placebo




CD4+




CD8+
But Maraviroc Causes a Nearly 2-fold increase in
             Rectal T Cell Activation




CD4+




CD8+
MVC intensification increases sCD14 levels
                                                            Ī” Wk 24-36
                             Ī” Wk 0-4           Ī” Wk 0-24   P=0.31
                             P=0.053            P=0.017




         MVC arm had a mean 0.33 Āµg/mL greater increase in sCD14
           from baseline to week 24 (95%CI: 0.06, 0.61, p=0.017)

Interestingly, sCD14 levels tended to increase further after discontinuation of MVC.
Why does CCR5 inhibition
increase T cell and monocyte
      activation in vivo?
Ligand approaches CCR5         Binding and Signaling       Ligand-Receptor Internalization




Lederman, JAMA, 2006

ā€¢ Maraviroc blocks internalization of receptor-ligand complexes leading to:
    ā€¢ Increased CCR5 expression on cell surface
    ā€¢ Increase in soluble ligands in plasma and tissues
      (Lin/Corbeau, AIDS, 2007; Nakata/Mitsuya, Antiviral Threrapy, 2010)

ā€¢ CCR5 ligands (MIP-1Ī±, MIP-1Ī² and RANTES) also bind other chemokine
  receptors (CCR1 on monocytes/neutrophils, CCR4/CCR4 on T cells)
  (Wolpe, J Exp Med, 1988; Fahey, JI, 1992)

ā€¢ Current Hypothesis: Activation of monocytes via CCR1 and T cells via
  CCR3/CCD4 might explain increased T cell and monocyte activation.
>2-fold Increase in Plasma MIP-1Ī² (CCR5 Ligand)
     Levels During Maraviroc Intensification
MVC-mediated Increases in CCR5 ligands
 are associated with increases in sCD14




                    Spearmanā€™s rho:
                    0.34, P=0.017
Brachial Artery Flow-Mediated Dilation

                        Endothelial Stimulus:
                        Reactive hyperemia after
                        five minute cuff occlusion.
                        Stimulates functioning
                        endothelial cells to release
                        NO. NO diffuses into vascular
                        smooth muscle. Muscle
                        relaxes.

                        Control stimulus:
                        Nitroglycerin, an
                        endothelium-independent
                        vasodilator

                        Quantity measured:
                        Diameter of artery, using B-
                        mode ultrasound
Normal Brachial Artery
Endothelium-Dependent Vasomotion
                      Vasodilation




Brachial Artery




  Baseline        Reactive Hyperemia
Despite MVC-mediated Increases in T cell and
 Monocyte Activation, No difference in FMD
                                                               Ī” Wk 24-36
                                            Ī” Wk 0-24
                  Ī” Wk 0-4                                     P=0.89
                                            P=0.61
                  P=0.40




                         ART + Study Drug           ART only




  Mean +0.46% greater week 24 change from baseline in MVC arm
               (95% CI: -0.36% to +1.28%, P=0.61)
Conclusions
   Maraviroc intensification in HIV+ subjects with
      incomplete ART-mediated CD4 recovery:
ā€¢ Causes a nearly 2-fold increase in T cell activation in GALT,
  and more modest increases in peripheral blood.
ā€¢ Also increases monocyte activation.
   ā€“ CCR5 ligand signaling through other chemokine receptors should be
     explored as a possible causal mechanism.
ā€¢ No clear effect on vascular function (by FMD)
   ā€“ Could decreased chemotaxis abrogate a negative effect of monocte
     and T cell activation?
ā€¢ The clinical implications of these findings are unclear.
   ā€“ CADIRIS, ANRS studies with clinical endpoints ongoing
SFGH CRC:
Aā€œHubā€ for Multidisciplinary T1 Research
                      Clinical Trials
                      Hunt, Hatano,
                      Hsue, Deeks       Cardiovascular
     SCOPE Cohort                        (FMD, IMT, etc)
      Deeks/Martin                           Hsue

                                                     Lymph Node
Gut Mucosal
                                                       Biopsy
Biospy Core                                             Hatano
Somsouk/Hunt

                        SFGH                            Neurology
                                                     (CSF Biomarkers)
  Specimen
    Bank
                        CRC                                Price

     ASB                                                Basic
                                                     Laboratories
                                                     McCune/Nixon
        Virology
        Core Lab                        Immunology
           Liegler                        Core Lab
                                          Sinclair
                      Clinical Lab
Acknowledgements
            Clinical Trial Sites                     Lederman Laboratory (CWRU)
   UCSF                  Rush/CORE Center            Brian Clagett
                                                     Nicholas Funderburg
   Lee Gilman            Oluwatoyin Adeyemi          Kathy Medvik
   Joy Madamba           Julia Lee
   Melissa Krone         Mieoak Bahk                 Karolinska Instituet
                                                     Victor Dahl
   Jeffrey Martin        Hamid Bouiri                Sarah Palmer
   Steven Deeks          Alan Landay
                                                     UCSF/SFGH GI Division
                                                     Ma Somsouk
   CWRU                  Stanford
                                                     UCSF/SFGH Cardiology Division
   Benigno Rodriguez     Debbie Slamowitz
                                                     Priscilla Hsue
   Jane Baum             Robert Shafer               Amanda Schnell
   Michelle Gallagher    Cindy Padilla
                                                     UC Davis Mucosal Immunology
   Michael Banchy        Martha Hamilton             Timothy Hayes
   Michael Lederman      Nancy Shulman               Barbara Shacklett

This trial was supported by investigator-initiated
grants from: Pfizer labs, Inc., and AMFAR
Acknowledgements:
                  SFGH CRC
NURSING                 SPECIMEN PROCESSING
Elizabeth Madruga, RN   Wendy Staub
Bernadette Tobin, RN    Benny Tong
Lorna Aquino, RN        Fabiola Carrillo
Beverly Schmidt, RN
                        BIONUTRITION
Nenette Dignadice, RN
                        Viva Tai
Rosemarie Dario, LVN
                        Jennifer Culp
Oscar Gomez Cruz, HA
                        Marilou Tarape
Antonio Everett, HA
                        Marlene Hom
Hector Vizoso, RN
                        May Yee
Eileen Magnaye, RN
Brenda Herrera, RN      ADMIN
Melinda Rowan, RN       Mark Jacobson, M.D. -Medical Director
Cory Groom, RN          Eunice Stephens -Operations Director
                        Gabriel Ortiz -Analyst

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  • 1. A Clinical Trial of CCR5 Inhibition in Treated HIV Infection: Highlighting Multidisciplinary T1 Research from the SFGH CRS Peter W. Hunt, M.D. Assistant Professor in Residence UCSF, SFGH HIV/AIDS Division
  • 2. SFGH CRC: Aā€œHubā€ for Multidisciplinary T1 Research Clinical Trials Hunt, Hatano, Hsue, Deeks Cardiovascular SCOPE Cohort (FMD, IMT, etc) Deeks/Martin Hsue Lymph Node Gut Mucosal Biopsy Biospy Core Hatano Somsouk/Hunt SFGH Neurology (CSF Biomarkers) Specimen Bank CRC Price ASB Basic Laboratories McCune/Nixon Virology Core Lab Immunology Liegler Core Lab Sinclair Clinical Lab
  • 3. HIV+ Patients Still Have a 10y Shorter Life Expectancy than HIV- Controls Survival from Age 25 Years N= 3,990 1 Probability of Survival 0.75 Population controls 0.5 Late HAART (2000ā€“2005) 0.25 Early HAART (1997ā€“1999) Pre-HAART 0 (1995ā€“1996) 25 30 35 40 45 50 55 60 65 70 Age, years Adapted from Lohse N, et al. Ann Intern Med 2007;146:87ā€“95 (See Also: ART-CC, Lancet, 2008; Lewden, JAIDS, 2007)
  • 4. Many morbidities associated with aging also appear to be increased in treated HIV disease ā€¢ Cardiovascular disease [1-3] ā€¢ Cancer (non-AIDS) [4] ā€¢ Bone fractures / osteoporosis [5,6] ā€¢ Liver disease [7] ā€¢ Kidney disease [8] ā€¢ Cognitive decline [9] ā€¢ Frailty [10] 1. Klein D, et al. J Acquir Immune Defic Syndr. 2002;30:471-477. 2; Hsue P, et al. Circulation. 2004;109:316-319. 3. Grinspoon SK, et al. Circulation. 2008;118:198-210. 4. Patel P, et al. Ann Int Med, 2008;148:728-736. 5. Triant V, et al. J Clin Endocrinol Metab. 2008;93:3499-3504. 6. Arnsten JH, et al. AIDS. 2007 ;21:617-623. 7. Odden MC, et al. Arch Intern Med. 2007;167:2213-2219. 8. Choi A, et al. AIDS, 2009;23(16):2143-49. 9. McCutchan JA, et a. AIDS. 2007 ;21:1109-1117. 10. Desquilbet L, et al. J Gerontol A Biol Sci Med Sci. 2007;62:1279-1286
  • 5. Many Chronic Diseases of Aging May Be Driven By Lifestyle Factors and ART Toxicity ART Toxicity Premature Aging Lifestyle (smoking, etc.) Deeks and Phillips, BMJ, 2009
  • 6. Persistent Immune Activation and Inflammation May Also Play Important Role ART Toxicity Premature Aging Lifestyle Persistent Inflammation Deeks and Phillips, BMJ, 2009
  • 7. An Important Clue from Nature Sooty Mangabey Rhesus Macaque ā€¢Infect with SIV ā€¢Infect with SIV ā€¢High Levels of Viral Replication ā€¢High Levels of Viral Replication ā€¢No AIDS, normal lifespan ā€¢AIDS and death ā€¢Minimal Immune Activation ā€¢Massive Immune Activation Silvestri, Immunity, 2003
  • 8. T Cell Activation Declines with ART Hunt et al, JID, 2003 and 2008
  • 9. But Remains Abnormally High During ART-mediated Viral Suppresion Hunt et al, JID, 2003 and 2008
  • 10. CCR5 Inhibition: A Potential Intervention to Reduce T Cell Activation ā€¢ Maraviroc is a CCR5 inhibitor and the only currently approved ARV drug that targets a host element. ā€¢ In addition to blocking HIV entry, maraviroc blocks binding of natural CCR5 ligands. ā€“ Contribute to T cell and monocyte trafficking and activation ā€¢ Potential immunologic benefit to blocking CCR5 supported by: ā€“ CCR5 āˆ†32 causes delayed HIV disease progression. ā€“ Natural hosts of non-pathogenic SIV have low CCR5 on central memory T cells and low T cell activation. ā€¢ Hypothesis: Adding maraviroc to a suppressive regimen will decrease T cell activation in treated HIV infection
  • 11. Maraviroc Intensification Trial Schematic Randomize ART alone (N=42) Add Maraviroc BID x 24 weeks x 12 weeks ART>1y VL<75 ART alone CD4<350 Add Placebo BID x 24 weeks x 12 weeks Study Visits at Weeks: -2 0 1 2 4 6 8 12 16 20 22 24 28 36 T Cell Activation, biomarkers, Low-level Viremia (SCA), FMD (Cardiovascular) Clinical monitoring, CD4 count Flexible Sigmoidoscopy, Rectosigmoid Biopsy (UCSF only)
  • 12. CCR5 Expression is Much More Common on T Cells in Rectal Mucosa
  • 13. Baseline Characteristics Placebo Maraviroc Characteristic Median (IQR) Median (IQR) N=22 N=23 Age, years 50 (43 to 57) 50 (46 to 56) Male Gender, No. (%) 20 (91) 23 (100) CD4 count, cells/mm3 202 (161 to 256) 206 (131 to 260) Plasma HIV RNA level, copies/ml <48 <48 Duration of current ART regimen, months 31 (15 to 43) 30 (21 to 42) Hepatitis C Virus Antibody Positive, No. (%) 2 (14) 3 (20)
  • 14. Early Decline in Plasma HIV RNA Levels by Single Copy Assay in Both Arms
  • 15. Similar CD4 Count Increase in Both Arms No evidence for difference in the rate of CD4+ T cell recovery between arms, P=0.97
  • 16. CD8+ T Cell Activation Declined Significantly in the Placebo Arm
  • 17. While CD8+ T Cell Activation Tended to Increase in the Maraviroc Arm
  • 18. Maraviroc Increases CD8 Activation Compared to Placebo P values represent difference between groups in the change from baseline at each timepoint.
  • 19. Maraviroc Prevents the Decline in CD4 Activation Compared to Placebo P values represent difference between groups in the change from baseline at each timepoint.
  • 20. No Change in Rectal T Cell Activation on Placebo CD4+ CD8+
  • 21. But Maraviroc Causes a Nearly 2-fold increase in Rectal T Cell Activation CD4+ CD8+
  • 22. MVC intensification increases sCD14 levels Ī” Wk 24-36 Ī” Wk 0-4 Ī” Wk 0-24 P=0.31 P=0.053 P=0.017 MVC arm had a mean 0.33 Āµg/mL greater increase in sCD14 from baseline to week 24 (95%CI: 0.06, 0.61, p=0.017) Interestingly, sCD14 levels tended to increase further after discontinuation of MVC.
  • 23. Why does CCR5 inhibition increase T cell and monocyte activation in vivo?
  • 24. Ligand approaches CCR5 Binding and Signaling Ligand-Receptor Internalization Lederman, JAMA, 2006 ā€¢ Maraviroc blocks internalization of receptor-ligand complexes leading to: ā€¢ Increased CCR5 expression on cell surface ā€¢ Increase in soluble ligands in plasma and tissues (Lin/Corbeau, AIDS, 2007; Nakata/Mitsuya, Antiviral Threrapy, 2010) ā€¢ CCR5 ligands (MIP-1Ī±, MIP-1Ī² and RANTES) also bind other chemokine receptors (CCR1 on monocytes/neutrophils, CCR4/CCR4 on T cells) (Wolpe, J Exp Med, 1988; Fahey, JI, 1992) ā€¢ Current Hypothesis: Activation of monocytes via CCR1 and T cells via CCR3/CCD4 might explain increased T cell and monocyte activation.
  • 25. >2-fold Increase in Plasma MIP-1Ī² (CCR5 Ligand) Levels During Maraviroc Intensification
  • 26. MVC-mediated Increases in CCR5 ligands are associated with increases in sCD14 Spearmanā€™s rho: 0.34, P=0.017
  • 27. Brachial Artery Flow-Mediated Dilation Endothelial Stimulus: Reactive hyperemia after five minute cuff occlusion. Stimulates functioning endothelial cells to release NO. NO diffuses into vascular smooth muscle. Muscle relaxes. Control stimulus: Nitroglycerin, an endothelium-independent vasodilator Quantity measured: Diameter of artery, using B- mode ultrasound
  • 28. Normal Brachial Artery Endothelium-Dependent Vasomotion Vasodilation Brachial Artery Baseline Reactive Hyperemia
  • 29. Despite MVC-mediated Increases in T cell and Monocyte Activation, No difference in FMD Ī” Wk 24-36 Ī” Wk 0-24 Ī” Wk 0-4 P=0.89 P=0.61 P=0.40 ART + Study Drug ART only Mean +0.46% greater week 24 change from baseline in MVC arm (95% CI: -0.36% to +1.28%, P=0.61)
  • 30. Conclusions Maraviroc intensification in HIV+ subjects with incomplete ART-mediated CD4 recovery: ā€¢ Causes a nearly 2-fold increase in T cell activation in GALT, and more modest increases in peripheral blood. ā€¢ Also increases monocyte activation. ā€“ CCR5 ligand signaling through other chemokine receptors should be explored as a possible causal mechanism. ā€¢ No clear effect on vascular function (by FMD) ā€“ Could decreased chemotaxis abrogate a negative effect of monocte and T cell activation? ā€¢ The clinical implications of these findings are unclear. ā€“ CADIRIS, ANRS studies with clinical endpoints ongoing
  • 31. SFGH CRC: Aā€œHubā€ for Multidisciplinary T1 Research Clinical Trials Hunt, Hatano, Hsue, Deeks Cardiovascular SCOPE Cohort (FMD, IMT, etc) Deeks/Martin Hsue Lymph Node Gut Mucosal Biopsy Biospy Core Hatano Somsouk/Hunt SFGH Neurology (CSF Biomarkers) Specimen Bank CRC Price ASB Basic Laboratories McCune/Nixon Virology Core Lab Immunology Liegler Core Lab Sinclair Clinical Lab
  • 32. Acknowledgements Clinical Trial Sites Lederman Laboratory (CWRU) UCSF Rush/CORE Center Brian Clagett Nicholas Funderburg Lee Gilman Oluwatoyin Adeyemi Kathy Medvik Joy Madamba Julia Lee Melissa Krone Mieoak Bahk Karolinska Instituet Victor Dahl Jeffrey Martin Hamid Bouiri Sarah Palmer Steven Deeks Alan Landay UCSF/SFGH GI Division Ma Somsouk CWRU Stanford UCSF/SFGH Cardiology Division Benigno Rodriguez Debbie Slamowitz Priscilla Hsue Jane Baum Robert Shafer Amanda Schnell Michelle Gallagher Cindy Padilla UC Davis Mucosal Immunology Michael Banchy Martha Hamilton Timothy Hayes Michael Lederman Nancy Shulman Barbara Shacklett This trial was supported by investigator-initiated grants from: Pfizer labs, Inc., and AMFAR
  • 33. Acknowledgements: SFGH CRC NURSING SPECIMEN PROCESSING Elizabeth Madruga, RN Wendy Staub Bernadette Tobin, RN Benny Tong Lorna Aquino, RN Fabiola Carrillo Beverly Schmidt, RN BIONUTRITION Nenette Dignadice, RN Viva Tai Rosemarie Dario, LVN Jennifer Culp Oscar Gomez Cruz, HA Marilou Tarape Antonio Everett, HA Marlene Hom Hector Vizoso, RN May Yee Eileen Magnaye, RN Brenda Herrera, RN ADMIN Melinda Rowan, RN Mark Jacobson, M.D. -Medical Director Cory Groom, RN Eunice Stephens -Operations Director Gabriel Ortiz -Analyst

Editor's Notes

  1. Consistent with this hypothesis, maraviroc-treated patients experienced a significantly greater increase in sCD14 levels than placebo-treated subjects through week 24.
  2. Will clean up this slide and try to crop away text.
  3. Thesedata are consistent with the hypothesis that increasing CCR5 ligands during maraviroc intensification are causing monocyte/macrophage activation.
  4. Despite these treatment-mediated increases in monocyte/macrophage activation, we observed no evidence for any clinically meaningful changes in vascular function ā€“as assessed by FMD ā€“ at any timepoint. Specifically, we can confidently exclude harmful decreases in FMD of greater than 0.36% and beneficial increases of greater than 1.28%.