|
Nature Reviews Immunology 3,
503-509 (2003); doi:10.1038/nri1107
[200K]
Science and Society
THERAPEUTIC VACCINES
AGAINST HIV NEED INTERNATIONAL PARTNERSHIPS
Brigitte Autran1, Patrice Debré,1, Bruce Walker2 & Christine Katlama3 about the authors
1 Brigitte Autran and Patrice Debré
are at the Laboratoire d'Immunologie Cellulaire, Centre Hospitalier
Universitaire Pitié-Salpétrière, 75651 Paris, France.
2 Bruce Walker is at the Partners AIDS Research Center,
Howard Hughes Medical Institute, Massachusetts General Hospital and
Division of AIDS, Harvard Medical School, Boston MA02129, USA.
3 Christine Katlama is at the Service de Maladies
Infectieuses, Centre Hospitalier Universitaire Pitié-Salpétrière,
75651 Paris, France.
correspondence to: Brigitte Autran brigitte.autran@psl.ap-hop-paris.fr
The successes of anti-retroviral treatments against HIV are
limited today by the cost and toxicity of lifelong administration.
An innovative therapeutic strategy has been proposed to boost the
immune system of infected patients with HIV vaccines and to help
limit the use of anti-retroviral treatments. This perspective
article reviews the crucial questions raised by such a strategy and
the main international efforts that are already set up to provide
rapid answers — in particular, a not-for-profit international
network that is dedicated to the development of therapeutic
immunization programmes against HIV.
The recent successes in the development of anti-retroviral
therapies that contain
HIV-1 infection are, at present, challenged by the
cost of this lifelong therapy and by its toxicity. As a result of
these toxic side effects, treatment delays or interruptions are
required. In the absence of a new therapeutic breakthrough,
alternative strategies are needed. Immune-based therapeutic
strategies that boost the immune response against HIV have been
proposed to limit the use of anti-retroviral drugs. Indeed,
enhancing immune control of the virus before anti-retroviral
treatments are discontinued should help to prolong the period
without therapy. However, this new strategy raises several issues
that require rapid and efficient evaluation by the coordinated
efforts of international and multidisciplinary communities. Apart
from national agencies, private sponsorship and not-for-profit
organizations that are dedicated to the development of therapeutic
immunization against HIV will be instrumental in accelerating the
development of such a challenging enterprise — by increasing the
flexibility and rapidity of funding, as well as by enhancing the
complementarity and creativity of researchers.
Limitations of drug therapy
The course of HIV infection has changed markedly following the
introduction, in 1996, of potent new anti-retroviral regimens —
known as highly active anti-retroviral therapy (HAART) (Fig.
1). Indeed, HAART regimens reduce the immunological damage that
is caused by HIV and restore CD4+ T-cell numbers and host
defences against pathogens1. The
clinical benefits were rapidly realized, with a marked reduction in
the level of AIDS-related mortality and morbidity in countries that
have access to HAART2.
Despite these clear successes, numerous shortcomings are
emerging. First, these potent treatments do not eradicate HIV, but,
at best, result in long-term containment of infection below the
level of detection3. At present, it is
estimated that quiescent reservoirs of HIV can persist in the host
for at least 50 years, indicating the need for lifelong therapy3. Second, despite progress in providing access
to HAART in developing countries, the cost of these lifelong
therapies means that they are available to less than 2% of the 42
million individuals worldwide that are presently infected with HIV.
Although the 'Accelerated Access' initiative by the United Nations
Programme on HIV and AIDS (UNAIDS), together with drug companies,
has helped to reduce the cost of HAART in developing countries by
tenfold, at 1,300–1,500 US dollars per year the cost of
anti-retroviral treatment is still far above the average annual
income and is available to only one or two per cent of infected
individuals in these countries. Even with the reduced cost of
generic drugs, which is estimated to be as low as 300 US dollars per
year, the cost far exceeds the resources that are allocated to
health care in most countries. In Africa, where the average annual
income is below 1,000 US dollars, treatment remains unaffordable (Table 1). Third, difficulties with persistent
adherence to lifelong therapy limit the efficacy of HAART. Low
compliance and unscheduled gaps in treatment allow for bursts of HIV
replication and result in the selection of virus mutations that
confer drug resistance4. Treatment
failures owing to drug resistance are now one of the biggest
problems for the clinical management of HIV infection.
 |
|
Table 1 | Annual cost of
anti-retroviral therapies |
Finally, the long-term administration of HAART is challenged as a
result of the side effects that occur in 40–60% of patients5, 6. These side effects
include mitochondrial toxicity resulting in neuropathy and myo
pathy, severe
LIPODYSTROPHIES, and the
accumulation of triglycerides and cholesterol that leads to an
increased frequency of
MYOCARDIAL INFARCTION. In the
absence of measures to prevent these complications, the new
worldwide therapeutic guidelines7
recommend that the initiation of therapy is delayed.
Despite the continuous development of new drugs — including new
drug families such as inhibitors of virus entry — there is little
hope that a new therapeutic breakthrough that can block the
replication of HIV without producing virus resistance or cumulative
side effects will emerge soon. So, there is no question that
additional therapeutic options are required.
Immune augmentation
Enhancing the host immune response to HIV might be an alternative
strategy for controlling HIV. Indeed, adaptive cell-mediated
immunity, together with the as yet poorly understood innate
immunity, contributes to the control of chronic virus infection, and
HIV seems to be no exception. Studies in both animal models of AIDS
and HIV-infected humans indicate that HIV-specific CD4+ T
helper (TH) cells and CD8+ cytotoxic T
lymphocytes (CTLs) can contribute to this control8-11
(Fig.
1). The establishment of a virus
SET POINT after primary infection
is thought to indicate the speed and potency of the immune response.
Indeed, HIV-specific CD4+ and CD8+ T cells
help to reduce the virus load to a quasi-equilibrium level, which is
typically 10,000 fold lower than the average 10 million virus
particles per ml of plasma present during acute infection. By
contrast, HIV-specific neutralizing antibodies seem to occur too
late during infection to have a decisive role in this early control
of HIV12, although their contribution
has not yet been fully explored. Once established, the
quasi-equilibrium in virus production is mainly controlled by T
cells, although this is not complete. This partial immune selection
pressure in the face of persisting replication of virus allows for
the gradual development of immune-escape mutations and 'immune
resistance'. After years of this permanent 'predator–prey'
relationship, T cells eventually become exhausted and fail to keep
the virus at bay. There are exceptions however — less than 5% of
HIV-infected individuals are known as long-term non-progressors. The
immune responses in these individuals can maintain efficient control
of the virus for more than 20 years in the absence of treatment13, 14. The challenge is to
induce this type of long-term effective immunity in individuals who
do not achieve it on their own.
So, HIV-specific CD4+ and CD8+ T-cell
responses can be almost as efficient as HAART during the primary
infection, resulting in a reduction in virus load by several logs,
and can control the replication of HIV for years. However, they
cannot eradicate the virus and they exert pressure on the virus that
drives the selection of variants that can escape immune control.
Restoration of the immune response
Successful treatment with HAART leads to the restoration of
effective immunity to viral pathogens1
that is potent enough to allow discontinuation of prophylaxis15. Can HAART alone help to restore the immune
response to HIV? There is no question that immediate treatment with
HAART during acute HIV infection leads to increased HIV-specific CD4+
TH-cell responses16-18,
probably by limiting the infection of these activated cells19. Unfortunately, administration of HAART
alone during the chronic phase of infection does not readily restore
or even preserve HIV-specific immunity20,
21. Instead, these specific defences
usually wane with HAART — a phenomenon that is thought to indicate
the antigen-driven homeostasis of pathogen-specific immune
responses. Indeed, HAART limits the production of HIV antigens to a
threshold below that required to stimulate HIV-specific effector T
cells or to stimulate HIV-specific naive cells. Anergy or tolerance
are not to blame however, as immune responses to HIV can be restored
when the immune system is re-exposed to HIV16,
22-24.
On the basis of these observations, an approach known as
structured treatment interruptions (STIs), which is best explained
as a type of
AUTO-VACCINATION, has been
developed. The hope was that brief and regulated exposure to the
virus with which an individual is infected in the absence of therapy
might lead to immune augmentation and enhanced control of virus.
Indeed, marked increases in HIV-specific immunity are detected
following STIs in individuals that are treated during the acute
phase of infection16, 25,
26. Although transient control of HIV has
been achieved in small uncontrolled trials of treatment interruption
in these patients, the durability of this control remains
questionable28, 29.
The results of STIs in individuals with chronic HIV infection have
been more disappointing. Rebounds in HIV-specific CD4+
and CD8+ T-cell numbers, similar to those seen in studies
of acute-phase infection, usually follow relapses of virus
replication, but they are too weak and transient to ensure control
of the virus in the absence of treatment22-24.
Should such failures be blamed on the immune system itself or the
auto-vaccination procedure? Re-exposing a heavily pre-immunized
individual to the same virus antigens favours the growth of memory
CTL clones21, thereby limiting the
diversification of the specific repertoire, according to the theory
of
ANTIGENIC SIN. Exposing newly
activated antigen-specific CD4+ cells to live virus
rapidly impairs their function in helping to induce the
differentiation and clonal expansion of naive virus-specific CTLs19, 22.
An alternative strategy, known as therapeutic immunization, aims
to boost all components of the immune response to HIV when the virus
is still under the pressure of HAART, so that an efficient immune
barrier, which involves strong and durable CD4+ T-cell
help, and strong and diverse CTLs (and perhaps antibodies) arises
against the virus before exposure to the live virus, rather than
after27 (Fig.
1). Several animal models support the rationale for therapeutic
immunization by showing partial control of viraemia after
anti-retroviral treatment and therapeutic immunization during
primary28 or established29 infection with simian immunodeficiency
virus (SIV).
Questions for therapeutic vaccines
The new challenge is, therefore, to augment immunity to HIV while
patients are still on therapy, so that even after long periods off
therapy, the balance between HIV replication and the host immune
response can be maintained. Such a strategy, however, raises several
important questions.
First, will a vaccine be as or more effective at augmenting
immunity than live pathogenic HIV, and which vaccines are available?
A general consensus supports the use of vaccines that can
restimulate broadly directed HIV-specific CD4+ and CD8+
T cells, although, again, little attention has been paid to the role
of neutralizing antibodies. Although effective prophylactic vaccines
are not yet available, there are several candidates in the pipeline
that deserve parallel consideration as therapeutic vaccines.
Recombinant virus vectors alone, or in combination with
polynucleotide vaccines30 or peptides,
might be the best choice to achieve this goal. Results from the
first clinical trials are becoming available. Therapeutic
immunization with an HIV–recombinant canarypox virus vector has
proven to be immunogenic in acutely infected patients that are
treated with HAART31. Two recent phase
II clinical trials of chronically infected individuals immunized
with the HIV–recombinant canarypox vector, either alone32 or in combination with lipopeptides and
interleukin-2 (IL-2)33, were both
associated with a marked, although modest, extension of the
treatment-discontinuation period. Even more encouraging was the
ability of this recombinant vector to broaden the HIV-specific CD8+
T-cell repertoire, with cross-recognition of vaccine and autologous
virus sequences34, and the marked asso
ciation between the generation of CD4+ TH1-cell
responses and the delay in restarting therapy32.
Inactivated viruses and proteins that induce antibodies specific
for HIV and the CD4+ TH1 cells that are
required for the generation of CTL responses might be of interest.
An inactivated HIV vaccine was, indeed, able to augment
virus-specific TH-cell responses, but whether it confers
protection has not been tested35.
Combinations of recombinant virus vectors and these inactivated
viruses might provide even more potent regimens, and they are
presently being examined in an on-going clinical trial in acutely
infected patients that are treated with HAART36.
An alternative strategy, which has been recently illustrated using
an SIV model37, involves the use of
autologous dendritic cells that are pulsed with chemically
inactivated HIV. Converting this expensive strategy to allow for the
treatment of millions of infected individuals is not yet feasible.
Nevertheless, important proofs of concept can be established from
these studies, and dissection of the effective components of
immunity is likely to promote research into the identification of
alternative immune stimulators, other than dendritic cells, and more
cost-effective strategies that might be amenable for global use38. Finally, other adjuvants or cytokines have
still to be evaluated. Several clinical trials are presently being
carried out that test the use of recombinant virus vectors and IL-2
(Ref. 33) as a therapeutic vaccine strategy.
Second, when an efficient vaccine is found, new questions will
arise, as schedules of immunization and safety concerns might differ
for therapeutic and prophylactic vaccine approaches. Indeed,
high-dose tolerance that is induced by hyperimmunization of
individuals pre-immunized by HIV has to be avoided, and a
therapeutic approach might not require as many immunizations as the
prophylactic vaccination of seronegative naive individuals. The
safety concerns raised by the use of a live attenuated virus vector
or a growth factor might also differ when the risk of immune
deficiency exists. The use of whole virus as an immunogen is also
likely to be approved for infected persons long before it will be
tested as a prophylactic strategy.
Third, the goal and end points to be reached by therapeutic
vaccination have to be clearly defined. Is our aim to delay the
initiation of therapy? Or to prolong the time spent off therapy? Or
to reduce the number of anti-retroviral drugs that are required to
control virus replication? Even when an ideal, safe and immunogenic
candidate vaccine is found, we will still need to establish optimal
designs and appropriate end points for clinical trials. Given the
rapidity and severity of the CD4+ T-cell depletion that
is usually observed during STIs in chronic infection, are there
ethical issues in proposing the use of a placebo in these trials?
End points also vary with time and with the changing guidelines for
anti-retroviral therapy. Indeed, the clinical trials for therapeutic
vaccines that were designed in 1999 had aimed to maintain the virus
load below 10,000–30,000 copies per ml of plasma as a primary end
point, but these criteria have changed in the years since then10. New designs for clinical trials will
consider the time it takes to reach a CD4+ T-cell count
of 250–300 per mm3 after discontinuation of therapy,
which is the lower limit for the initiation of anti-retroviral
therapy according to most of the present guidelines7 (Fig.
2).
Finally, important questions that are fundamental to the concept
of therapeutic immunization have to be thoroughly evaluated. Does
restoring cellular or humoral immune responses to which the virus
has already escaped make any sense? Is durable immune augmentation
possible during the chronic phase in HIV-infected individuals who
have a history of severe immune deficiency, even if it can be
improved with HAART? Rapid answers to these questions are crucial
given the hopes raised by this exciting new field of investigation
and its consequences for the clinical management of the disease.
International efforts
There is no question that therapeutic immunization deserves
intense investigation as a potential option for the treatment of HIV
infection. The questions outlined above will not be readily solved
without an intense and collective international effort to explore
simultaneously the different strategies that have been proposed.
Rapid evaluation of many vaccine approaches in phase I and II
clinical trials requires interdisciplinary teams of experienced
immunologists, vaccinologists, virologists, clinical-trial experts
and clinicians. Indeed, to reach the goal of effective immuno
therapy for HIV-1 infection will require the expertise of many
disciplines. The traditional boundaries between basic science and
clinical medicine have begun to break down with the introduction of
HAART, and many investigative possibilities have opened up. In the
era of therapeutic vaccines, vaccinologists will have to become
increasingly familiar with the questions that are raised by the
clinical management of AIDS. A network of top-quality scientists and
clinicians will bring the complementarity that is required for the
development of these new strategies. In addition, such a network
provides a way to exploit rapidly the main research investments in
various vaccine approaches. Indeed, interaction with experienced
clinical sites should allow larger clinical trials and a greater
number of them to be carried out, thereby providing better
opportunities for the evaluation of vaccine efficacy. Collaboration
between immunology laboratories with experience in high-tech
immunology research tools will facilitate the definition of
standards and augment the evaluation of various vaccine strategies.
Periodic 'think-tank' meetings are also required to help this
community answer the questions raised by vaccine initiatives.
How can such networks be established and sponsored?
A marked effort has already been made by several national research
agencies to build interdisciplinary networks that can evaluate
therapeutic vaccination programmes: the ANRS (National Agency for
AIDS research) in France, ACTG (AIDS Clinical Trials Group) in the
USA, and several other countries have already set up networks for
phase I and II trials. However, these efforts are generally limited
to certain immunogens. With the emergence of potential new vaccines,
intensified efforts are required. Moreover, the cost and technical
expertise that is required to monitor the efficacy of these
therapeutic strategies is an important obstacle. Although these
national agencies are unique in providing the investment for
infrastructures that are relevant to clinical trials, a global
approach will require an international effort and the participation
of other networks.
The international community has already set up, with the World
Health Organization (WHO), united efforts to help organize phase III
trials for various vaccine strategies. Therapeutic vaccination
against HIV might require smaller scale, high-tech interdisciplinary
teams. The European Union (EU) provides unique government facilities
to build supra-national interdisciplinary networks between academics
and industries. As an example, Theravac is an EU-funded programme
that will test the safety, immunogenicity and efficacy of new,
highly attenuated, recombinant pox-viruses with French, Dutch,
German and Swiss teams of scientists and clinicians.
Combined efforts from the public and private sectors are working
to accomplish this goal, such as CANVAC (Canadian Network for
Vaccines and Immunotherapeutics) in Canada, which is developing
vaccines and clinical trials, or the International Forum for
Collaborative HIV Research, which is organizing international
think-tank meetings that incorporate various national regulatory
agencies, academics, government departments and industries to help
solve the questions of vaccine safety, trial design and end points.
Large pharmaceutical companies that have already invested in HIV
vaccines are increasing their investments in this direction. The
QUEST study36 is an example of an
exceptional effort, in which one large pharmaceutical company is
sponsoring an international team composed of clinicians, virologists
and immunologists to evaluate a large, multicentre, international
phase II trial of a therapeutic-immunization strategy that combines
the recombinant canarypox virus and an inactivated HIV vaccine
provided by two distinct companies.
Although highly encouraging, present efforts are too limited to
allow for the systematic exploration of all the approaches that
deserve testing. Private sponsorship should also provide additional
support for these efforts. The main private sponsor IAVI
(International AIDS Vaccine Initiative) has already proven to be
highly efficient at funding the development of new prophylactic
vaccines, and clinical and laboratory facilities, as well as
clinical trials39. Similar
international efforts have to be incorporated in the field of
therapeutic vaccines, with new financing strategies to help
accelerate this research.
ORVACS and therapeutic vaccines
ORVACS (Objectif Recherche Vaccins SIDA) is an example of this
kind of international collaborative effort. It is a not-for-profit
organization, which aims to accelerate research on therapeutic
vaccines and immune-based therapeutic strategies against HIV (Box 1). ORVACS was created in 2001 with the support
of Liliane Bettencourt — the main share-holder and daughter of the
founder of l'Oréal, the giant cosmetics company — and the
Bettencourt–Schueller Foundation in Paris. ORVACS has assembled an
international network of leading researchers with extensive
experience in immunology, vaccinology, anti-viral drug development
and clinical trials in HIV infection. So, ORVACS brings to the field
of therapeutic vaccines the research complementarity that is
required to develop clinical trials for the most promising vaccine
approaches seen in the pre-clinical arena.
Interdisciplinary teams have been brought together from three
immunology laboratories with a long history of research in T-cell
immunity to HIV and vaccines, from France (B.A. and P.D.), the
United Kingdom (A. McMichael) and the United States (B.W.), and
seven clinical centres with experience in anti-retroviral
therapeutic trials, from France (C.K.), the United Kingdom (M.
Youle), Germany (S. Staszewsky), Spain (J. Gatell and B. Clotet) and
the United States (R. Murphy), and include the largest and most
respected clinical centres that concentrate on AIDS research. By
creating a critical mass of top-quality researchers and clinicians,
establishing a network of laboratories that are able to carry out
standardized, quality controlled immunology and providing funding
for clinical trials of immune-based therapies, ORVACS is able to
integrate experts in HIV research with large vaccine companies or
small biotech companies with innovative HIV vaccine candidates. By
offering a unique platform of large and experienced clinical centres
and laboratories, ORVACS will ensure that the quality of clinical
trials required by regulatory and registration agencies is met. By
directly funding the clinical trials that are proposed by this
scientific network, ORVACS provides a unique opportunity to
accelerate this research and bring candidate vaccines to the
clinical programmes. Its independent status allows ORVACS to study
different vaccine candidates that might belong to different
pharmaceutical groups or biotech companies. Autonomy in financial
resources allows the ORVACS network to set up new therapeutic
projects rapidly that usually take months to be funded by
conventional means. The ORVACS network is developing a scientific
programme that aims to translate new vaccine concepts from
pre-clinical to clinical studies.
So, the purpose of ORVACS is to complement existing national and
international efforts in the field to increase research on new
immunological concepts or products for therapeutic intervention
against HIV. The private sponsorship that funds ORVACS (representing
half the budget of the Bettencourt–Scueller Foundation) gives this
relatively small network the rapidity and flexibility that is
required to investigate the most promising vaccine approaches.
Conclusions
At a time when general access to an expensive lifelong treatment
for HIV infection is not yet a reality, when virus eradication does
not seem to be obtainable and when lifelong HAART is becoming too
toxic, it is time to rethink the clinical management of HIV
infection. There is no doubt that maximal virus suppression is the
only way to restore immune functions. However, the ultimate goal of
therapeutic strategies is now to restore an immune response to HIV
that would help to control virus progression without anti-retroviral
treatment, prolong the time 'off' therapy and decrease the toxicity
and costs of anti-retroviral therapies for HIV-infected individuals
throughout the world. Promising vaccine studies indicate that immune
augmentation might be a realistic goal. Given the magnitude of the
present AIDS problem and the need for durable solutions, all
promising avenues must be pursued with the utmost haste.
International networks that combine all research forces and sponsors
are required to help solve these new issues. The ORVACS initiative
provides an incentive to expand present efforts in therapeutic
immunization, and to enhance the international partnerships that are
required to achieve, as quickly as possible, effective new
immune-based interventions for the durable control of HIV-related
immune defects.
Boxes
References
| 1. |
Autran, B., Carcelain, G., Li., T. S.,
Blanc, C. & Mathez, D. Positive effects of combined
anti-retroviral therapy on CD4+ T cell
homeostasis and function in advanced HIV disease.
Science 277, 112-116 (1997). | Article | PubMed | ChemPort | |
| 2. |
Palella, F. J. et al. Declining
morbidity and mortality among patients with advanced
human immunodeficiency virus infection. N. Engl. J.
Med. 338, 853-860 (1998). | Article | PubMed | |
| 3. |
Finzi, D. et al. Latent
infection of CD4+ T cells provides a
mechanism for lifelong persistence of HIV-1, even in
patients on effective combination therapy. Nature
Med. 5, 512-517 (1999). | Article
| PubMed | ChemPort | |
| 4. |
Shafer, R. W. et al. Multiple
concurrent reverse transcriptase and protease mutations
and multidrug resistance of HIV-1 isolates from heavily
treated patients. Ann. Intern. Med. 128,
906-911 (1998). | PubMed | ChemPort | |
| 5. |
Carr, A. et al. A syndrome of
peripheral lipodystrophy, hyperlipidemia and insulin
resistance in patients receiving protease inhibitors.
AIDS 12, 51F-58F (1998). | Article | |
| 6. |
Brinkman, K. et al.
Mitochondrial toxicity induced by nucleoside-analogue
reverse transcriptase inhibitors is a key factor in the
pathogenesis of antiretroviral-therapy-related
lipodystrophy. Lancet 354, 1112-1114
(1999). | Article | PubMed | ChemPort | |
| 7. |
Yeni, P. G. et al.
Antiretroviral treatment for adult HIV infection in
2002: updated recommendations of the International AIDS
Society-USA Panel. JAMA 288, 222-235
(2002). | Article | PubMed | ChemPort | |
| 8. |
Koup, R. A. et al. Temporal
association of cellular immune responses with the
initial control of viremia in primary human
immunodeficiency virus type 1 syndrome. J. Virol.
68, 4650-4655 (1994). | PubMed | ChemPort | |
| 9. |
Schmitz, J. E. et al. Control of
viremia in simian immunodeficiency virus infection by
CD8+ lymphocytes. Science 283,
857-860 (1999). | Article | PubMed | ChemPort | |
| 10. |
Rosenberg, E. S. et al. Vigorous
HIV-1-specific CD4+ T cell responses associated with
control of viremia. Science 278, 1447-1450
(1997). | Article | PubMed | ChemPort | |
| 11. |
Lyles, R. H. et al. Natural
history of human immunodeficiency virus type 1 viremia
after seroconversion and proximal to AIDS in a large
cohort of homosexual men. Multicenter AIDS cohort study.
J. Infect. Dis. 181, 872-880 (2000). | Article | PubMed | ChemPort | |
| 12. |
Parren, P. W., Moore, J. P., Burton, D.
R. & Sattentau, Q. J. The neutralizing antibody response
to HIV-1: viral evasion and escape from humoral
immunity. AIDS 13 S137-S162 (1999). | Article | PubMed | ChemPort | |
| 13. |
Rinaldo, C. R. et al. High
levels of anti-human immunodeficiency virus type 1
(HIV-1) memory cytotoxic T-lymphocyte activity and low
viral load are associated with lack of disease in HIV-1
infected long-term non progressors. J. Virol.
69, 5838-5842 (1995). | PubMed | ChemPort | |
| 14. |
Harrer, T. et al. Cytotoxic T
lymphocytes in asymptomatic long-term nonprogressing
HIV-1 infection. Breadth and specificity of the response
and relation to in vivo viral quasispecies in a
person with prolonged infection and low viral load.
J. Immunol. 156, 2616-2623 (1996). | PubMed | ChemPort | |
| 15. |
Jouan, M. et al. Discontinuation
of maintenance therapy for cytomegalovirus retinitis in
HIV-infected patients receiving highly active
antiretroviral therapy. AIDS 15, 23-31
(2001). | Article | PubMed | ChemPort | |
| 16. |
Rosenberg, E. S. et al. Immune
control of HIV-1 after early treatment of acute
infection. Nature 407, 523-526 (2000). | Article
| PubMed | ChemPort | |
| 17. |
Altfeld, M. et al. Cellular
immune responses and viral diversity in individuals
treated during acute and early HIV-1 infection. J.
Exp. Med. 193, 169-180 (2001). | Article | PubMed | ChemPort | |
| 18. |
Oxenius, A. et al. Early highly
active antiretroviral therapy for acute HIV-1 infection
preserves immune function of CD8+ and CD4+ T
lymphocytes. Proc. Natl Acad. Sci. USA 97,
3382-3387 (2000). | Article | PubMed | ChemPort | |
| 19. |
Douek, D. C. et al. HIV
preferentially infects HIV-specific CD4+ T cells.
Nature 417, 95-98 (2002). | Article
| PubMed | ChemPort | |
| 20. |
Ogg, G. S. et al. Decay kinetics
of human immunodeficiency virus-specific effector
cytotoxic T lymphocytes after combination antiretroviral
therapy. J. Virol. 73, 797-800 (1999). | PubMed | ChemPort | |
| 21. |
Mollet, L. et al. Dynamics of
HIV-specific CD8+ T lymphocytes with changes in viral
load. J. Immunol. 165, 1692-1704
(2000). | PubMed | ChemPort | |
| 22. |
Carcelain, G. et al. Transient
mobilization of human immunodeficiency virus
(HIV)-specific CD4 T-helper cells fails to control virus
rebounds during intermittent antiretroviral therapy in
chronic HIV type 1 infection. J. Virol. 75,
234-241 (2001). | Article | PubMed | ChemPort | |
| 23. |
Ruiz, L. et al. HIV dynamics and
T-cell immunity after three structured treatment
interruptions in chronic HIV-1 infection. AIDS
15, F19-F27 (2001). | Article | PubMed | ChemPort | |
| 24. |
Oxenius, A. et al. Stimulation
of HIV-specific cellular immunity by structured
treatment interruption fails to enhance viral control in
chronic HIV infection. Proc. Natl Acad. Sci. USA
99, 13747-13752 (2002). | Article | PubMed | ChemPort | |
| 25. |
Markowitz, M. et al.
Discontinuation of antiretroviral therapy commenced
early in the course of human immunodeficiency virus type
I infection, with or without adjunctive vaccination.
J. Infect. Dis. 186, 634-643 (2002). | Article | PubMed | ChemPort | |
| 26. |
Altfeld, M. et al. HIV-1
superinfection despite broad CD8+ T cell responses
containing replication of the primary virus. Nature
420, 434-439 (2002). | Article
| PubMed | ChemPort | |
| 27. |
Autran, B. & Carcelain, G. AIDS.
Boosting immunity to HIV: can the virus help? Science
290, 946-949 (2000). | Article | PubMed | ChemPort | |
| 28. |
Hel, Z. et al. Viremia control
following antiretroviral treatment and therapeutic
immunization during primary SIV231 infection
of macaques. Nature Med. 6, 1140-1146
(2000). | Article
| PubMed | ChemPort | |
| 29. |
Tryniszewska, E. et al.
Vaccination of macaques with long-standing SIVmac251
infection lowers viral set point after cessation of
antiretroviral therapy. J. Immunol. 169,
5347-5357 (2002). | PubMed | |
| 30. |
MacGregor, R. R. et al. First
human trial of a DNA-based vaccine for treatment of
human immunodeficiency virus type 1-infection: safety
and host response. J. Infect. Dis. 100,
178-192 (1998). |
| 31. |
Jin, X. et al. Safety and
immunogenicity of ALVAC vCP 1452 and recombinant gp 160
in newly human immunodeficiency virus type I infection,
with prolonged highly active antiretroviral therapy.
J. Virol. 76, 2206-2216 (2002). | Article | PubMed | ChemPort | |
| 32. |
Tubiana, R. et al. Therapeutic
vaccination with ALVAC-HIV vCP1433: a recombinant
canarypox vaccine in chronically HIV-1 infected patients
treated with HAART: VACCITER (ANRS 094) Abstr. 61, 10th
Conference in retroviruses and opportunistic infections,
Boston (2003). |
| 33. |
Levy, Y. et al. Immunological
and virological efficacy of ALVAC-VIH 1433 and HIV
lipopeptides (lipo-6T) combined with SC IL-2 in
chronically HIV-infected patients - results of the ANRS
093 randomized study. Abstr. 62, 10th Conference in
retroviruses and opportunistic infections, Boston
(2003). |
| 34. |
Le Garff, M. et al. Cross
recognition of HIV-specific CD8 responses in chronically
HIV-1 infected patients immunized by an HIV-1-LAI
recombinant canarypox vector (vCP1433) Abstr. 646, 10th
Conference in retroviruses and opportunistic infections,
Boston (2003). |
| 35. |
Robbins, G., Walker, B. & Rosenberg, E.
Augmentation of HIV-1-specific TH cell
responses in chronic HIV-1 infection by therapeutic
immunization. AIDS (in the press) |
| 36. |
Goh, L. E. et al. The QUEST
trial, a paradigm of HIV collaborative research.
Nature Med. 11, 1194 (2000). | Article
| ChemPort | |
| 37. |
Lu, W. et al. Therapeutic
dendritic-cell vaccine for simian AIDS. Nature Med.
9, 27-32 (2003). | Article
| PubMed | ChemPort | |
| 38. |
Bhardwaj, N. & Walker, B. Immunotherapy
for AIDS virus infections: cautious optimism for
cell-based vaccine. Nature Med. 9, 13-14
(2003). | Article
| PubMed | ChemPort | |
| 39. |
Dove, A. IAVI advances AIDS vaccine
research. International AIDS Vaccine Initiative.
Nature Med. 1, 5 (1999). | Article
| ChemPort | |
|
|
