The role of immune responses in HIV-1 Infection Marylyn M. Addo, MD/PhD Partners AIDS Research Center Massachusetts General Hospital Harvard Medical School.

Slides:

Advertisements

Similar presentations

ARV Nurse Training Programme Marcus McGilvray & Nicola Willis

Advertisements

Emerging patterns of drug resistance and viral tropism in cART-naïve and failing patients infected with HIV-1 subtype C Thumbi Ndung’u, BVM, PhD Associate.

31.6 Diseases that Weaken the Immune System When the immune system is weakened, the body cannot fight off disease.

HIV 101 Review Evaluation Center for HIV and Oral Health Boston University School of Public Health Health & Disability Working Group.

CCR5 : and HIV Immunity Gene Variation Works for and Against HIV Ashley Alexis & Hilda Hernandez.

The branch that breaks Is called rotten, but Wasn’t there snow on it? Bartolt Brecht Haiti after a hurricane.

The branch that breaks Is called rotten, but Wasn’t there snow on it? Bartolt Brecht Haiti after a hurricane.

Bioe 109 Evolution Summer 2009 Lecture 1: Part II Evolution in action: the HIV virus.

HIV/AIDS as a Microcosm for the Study of Evolution.

HIV and AIDS Human Immunodeficiency Virus (HIV) is the virus that causes Acquired Immunodeficiency Syndrome (AIDS).

Over 50 million HIV/AIDS cases have occurred worldwide Over 40 million people are currently living with HIV/AIDS 95% of all cases are in developing countries.

The branch that breaks Is called rotten, but Wasn’t there snow on it? Bartolt Brecht Haiti after a hurricane.

Current HIV basic science research topics. Toddler "Functionally Cured" of HIV Infection- “the Mississippi Baby” First well-documented case of an HIV.

Module 1: Overview of HIV Infection. Lab workersHealth workersCounselors 2 Learning Objectives At the end of this module, you will be able to: Describe.

KITSO AIDS Training Program

I guess you think you know this story.

Pathogenesis of HIV disease and markers of progression Anjie Zhen, PhD.

1 Virology - Chapter 13 Not responsible for details of Protein & genome synthesis pp A little history… “Filterable viruses” Bacteriophages Wendell.

Biology and natural history of the virus

Types of vaccines 1 - First generation vaccines are whole-organism vaccines - either live and weakened, or killed forms. [1] Live, attenuated vaccines,

Acute HIV Infection Translating Pathogenesis into Opportunity Eric S. Rosenberg, M.D. Associate Professor of Medicine Massachusetts General Hospital Harvard.

Eric S. Rosenberg, M.D. Associate Professor of Medicine Massachusetts General Hospital Harvard Medical School

AIDS supplement. History of HIV Originated in Africa in the late 1950’s Originally found in nonhuman primates and may have mutated First documented in.

The Influence of CCL3L1 Gene- Containing Segmental Duplications on HIV-1/AIDS Susceptibility Gonzalez et al. Mar 4, 2005 :307 Science Presenter: Braydon.

Clinical Care of HIV, AIDS and Opportunistic Infections

HIV-1 evolution in response to immune selection pressures

The evolution of HIV Why is HIV fatal?. Lethal strains are favored, due to “Short sighted” evolution within hosts Transmission rate advantages.

VIRUSES Tobacco mosaic virus Influenza virus Adenovirus Bacteriophage.

HIV Cellular Pathogenesis III

THE IMMUNOPATHOGENESIS OF HIV INFECTION. THE HUMAN IMMUNODEFICIENCY VIRUS (HIV) 10359bp DNA gp120 gp41 CD4 binding Membrane fusion.

Immune System Chris Schneider. Immune System Function The purpose of the immune system is to keep infectious microorganisms, such as certain bacteria,

Diversity of Living Things

After a virus becomes active and replicates in a host cell, it destroys the host cell. Copies of the virus are then released into the host organism, where.

Immunity Notes Quarter 4 Week 3. Immune Response There are 2 categories of immunity Specific and Non Specific.

Viruses A virus is a NON-Living particle made of DNA or RNA and a protein coat. Look at table 25-1 on p. 487 in text book. VERY small. ~ 0.001micron.

Functional cure after long term HAART initiated during early HIV infection - a case study. van Lunzen J. 1,2, Schulze zur Wiesch J. 1,2, Schumacher U.

HIV Cellular Pathogenesis III Benhur Lee, M.D.. Adult v. infant (IgG v. IgA) CTL response (MHC tetramers) p24 antigenimia Ab response Viral load.

Future directions in HIV basic science research The hunt for a cure.

I guess you think you know this story. You don’t. The real one’s much more gory. The phoney one, the one you know Was cooked up years and years ago.” Roald.

School: Shrimati Indira Gandhi SSS, Mauritius Age group: Form 4, yrs Subject: Art and Design.

Chapter 47 Section 3 pp HIV AND AIDS. VACCINES  Vaccines artificially produce acquired immunity  Vaccine- substance that contains antigen.

Blood Tests (“Labs”) 1. “Labs” Regular blood tests are a crucial part of HIV health care. They are often referred to as “bloods” or “labs” Several important.

Retrovirus. Retroviridae –Retrovirus HTLV (human T-cell lymphotropic virus) –Lentivirus HIV.

Evolution of the Functional Profile of HIV-Specific CD8+ T cells in a Cohort of Long Term Nonprogressors M López, N Rallón, A Peris, M Salgado, B Rodés,

THE IMMUNOPATHOGENESIS OF HIV INFECTION Lymphotropic virus.

Lecture 19 November 16 th 2010 Quiz 2 scheduled for November 23 rd not November 18th.

“Neutralizing Antibodies Derived from the B Cells of 1918 Influenza Pandemic Survivors” (Yu et. al) Daniel Greenberg.

Immune reconstitution Anjie Zhen, PhD

HUMAN IMMUNODEFICIENCY VIRUS AND ACQUIRED IMMUNODEFICIENCY SYNDROME (AIDS)

CATEGORY: VACCINES & THERAPEUTICS HIV-1 Vaccines Shokouh Makvandi-Nejad, University of Oxford, UK HIV-1 Vaccines © The copyright for this work resides.

Lesson Overview Lesson Overview Immune System Disorders Lesson Overview 35.4 Immune System Disorders.

Impact of immune-driven sequence variation in HIV- 1 subtype C Gag-protease on viral fitness and clinical outcome Thumbi Ndung’u, BVM, PhD HIV Pathogenesis.

HAART Initiation Within 2 Weeks of Seroconversion Associated With Virologic and Immunologic Benefits Slideset on: Hecht FM, Wang L, Collier A, et al. A.

Chapter 2: The Path from HIV to AIDS

Viruses :Tiny Biological Particles Size video.

IMMUNODEFICIENCIES HIV2 324 PHT Dr. Sarah I. Bukhari PhD in Clinical Microbiology Department of Pharmaceutics Office: rd floor

Create a concept map of the adaptive immune system.

Antiviral Medications

HIV-1 Vaccines Shokouh Makvandi-Nejad, University of Oxford, UK

Immune Responses to HIV

Partners AIDS Research Center Massachusetts General Hospital

Characteristics of Viruses

AIDS supplement.

Immunodeficiency (2 of 2)

Abnormal Immunity Continued

Immunodeficiency (2 of 2)

Human Immunodeficiency Virus Controllers: Mechanisms of Durable Virus Control in the Absence of Antiretroviral Therapy Steven G. Deeks, Bruce D. Walker

Module 1: Overview of HIV Infection

Presentation transcript:

The role of immune responses in HIV-1 Infection Marylyn M. Addo, MD/PhD Partners AIDS Research Center Massachusetts General Hospital Harvard Medical School Boston, MA USA

Time (years) CD4 per mm 3 Natural History of HIV-1 VZVTB Kaposi Sarcoma PCP 15 CMV MAC Crypto Lymphoma symptoms CD4 HIV RNA HIV RNA copies/ml

The level of HIV in the blood stream predicts subsequent survival RNA particles/ml plasma One year Rapid Progression Slow Progression Viral set point

What influences viral load in HIV infection?

Viruses are not able to reproduce on their own

New virus assembly 2-3 Days

Viral set point is determined by number of viruses produced by infected cells

Potential factors influencing the viral set point Attenuated virus Host genetic factors Host immune response

Potential factors influencing the viral set point Attenuated virus Host genetic factors Host immune response HAART

New virus assembly 2-3 Days Attenuated viruses Example: Sidney blood bank cohort Virus had a “mistake” in the nef gene

Attenuated viruses Host genetic factors

CD4 CCR5 Co-receptor polymorphisms can prevent entry of virus into cells 32 base pair deletion in CCR5

B27 B57 Migueles, PNAS 97:2709, 2000 Some molecules on the cell of an individual are associated with improved viral control and slow disease progression

Attenuated viruses Host immune responses Host genetic factors

New virus assembly Humoral Immune System: Neutralizing Antibodies B cell

New virus assembly CTL Soluble factors Cellular immune system: Killer T cells Cytotoxic T cell

New virus assembly CTL Soluble factors B cell Th

B cell Th CTL

The Generals (T helper cells trained to target HIV)

Generals (T Helper cells) Infantry (CTL) Enemy Infected cell

Why are the generals absent in most infected persons?

Generals (T Helper cells) Infantry (CTL) Enemy Infected cell

Virus-Specific T Helper Cells: Essential for Maintenance of Effective CTL Th cells absent Th cells present Relative magnitude CTL Viremia CTL

Is there any way to enhance the immune response against HIV?

Generals (T helper cells) Infantry (CTL) Enemy (Infected cells)

HAART Generals (T Helper cells) Infantry (CTL) Enemy (Infected cell)

Magnitude of Helper Cells Effect of Early Treatment on the Generals (HIV-Specific T Helper Cells) Weeks on Treatment

What happens if you stop treatment?

Weeks after first treatment interruption viral load (copies RNA/mL) HAART Early treatment of acute HIV infection followed by treatment interruption

Very early treatment with HAART leads to enhanced natural control of HIV

Where else do we find evidence for immune control in AIDS virus infection ? n In monkey studies, removing killer cells led to dramatic increases in viral load and restoring Killer T cells in those same monkey studies led to suppression of viral load n Individuals with high levels of Killer T cells have been shown to have low viral loads n Two interesting groups of individuals —HIV-1 long-term nonprogressors (LTNP) —HIV-1 exposed, but uninfected individuals (HEPS)

Infected 21 years Normal T cells Undetectable viral load Never on anti-HIV meds LTNP LTNP have strong and broadly directed killer cell responses and helper cell responses

HEPS n Most well known: —Nairobi sex worker cohort (Rowland-Jones et al.) —Found killer T cell responses in these HEPS, that may contribute to protection from HIV —Our group: collaboration with Lusaka, Zambia (PI: Susan Allen) studying killer cells in discordant couples and their partners Poster session Thursday 12-2 pm (Addo)

Vaccine development n Based on these pieces of data, it is felt that an effective HIV-1 vaccine needs to elicit cellular immune responses, in particular Killer T cell responses +/- Helper T cell responses n Most recent and compelling data derive from monkey studies demonstrating that Killer T cell have an impact on vaccine efficacy in this setting (Robbinson, Barouch/Letvin, Shiver) n Many vaccine approaches/trials currently in study

Our current Research n Understanding of total the killer T cell and helper cell response against HIV, not only to single proteins like previous studies. n Analysis of the virus by sequencing Bruce Walker morning Tuesday plenary Addo A05 Tuesday 14-15:30

More research needed for other virus types and other ethnicities n Durban, RSA n Immune responses in Clade C-Infection n Mother to child transmission and pediatric treatment and treatment interruption studies n NIH contract Epitope mapping in Non-Caucasians

Nelson Mandela School of Medicine University of Natal Lab

Why is HIV not controlled by the immune system like other chronic viral infections? Mono Chicken pox Herpes simplex

Problems n VIRAL ESCAPE n VIRAL DIVERSITY

How HIV mutates to escape Killer T-cells

Examples: n Goulder et al, Nature 2001 —Viral escape mutants can be transmitted from mother to child n Barouch et al, Nature 2002 —Loss of viral control in a vaccinated animal associated with viral escape in one epitope Viral escape

Viral Diversity Comparing Viruses: How much does HIV evolve compared to Flu? Less Variation More Variation

Influenza variation compared to HIV variation Canadian Flu 1996 Global Flu

Influenza variation compared to HIV variation Amsterdam 1997 Dem Rep of Congo Canadian Flu 1996 Global Flu

The extreme variability of HIV over time is a major impediment to immune control, effective drug therapy and vaccine development

Acknowledgements n Marcus Altfeld n Xu Yu n Almas Rathod n Cecily Fitzpatrick n Paul Lee n Philip Goulder n Christian Brander n Eric Rosenberg n Bruce Walker Funding Sources: German Research Council (DFG) amfAR Concerned Parents for AIDS Research (CPFA)

HLA-B27 is associated with slow progression to AIDS Viral Load n = 10 HLA-B27+

HLA B27 molecule I W K I L K G L The dominant CTL response in HLA-B27+ individuals: HIV Gag p24 KK10 epitope L R

B27-KK10 escape is associated with elevated viral load Non-controllers p=0.025 All Arg/Lys at P Controllers Viral Load

HIV Gag p24 KK10 epitope HLA B27 molecule I W K I L K G L R L K M I W K I L K G L

100% 80% 60% 40% 20% 0% n=21 86% n=6 33% p=0.02 PediatricAdult 2.73% CD8s 1.55% pbmc IFN-  CD8 B27-KK10 is recognized more frequently in adult than in pediatric HIV infection

B27-ve motherB27+ve mothers C C048-C 049-C IFN-  SFC/ million PBMC 1925 B27-KK10 is not recognized in children of B27-positive mothers

B27-ve motherB27+ve mothers 043-C C048-C049-C B27-KK10 non-recognition associated with P2 anchor mutation IFN-  SFC/ million PBMC P2 anchor mutation shared with mother No P2 anchor mutation