Clinical group
The Biology of HIV Infection
Duangrat Inthorn
Mahidol University
Duangrat Inthorn
The Biology of HIV Infection
This report includes general information on HIV history, the classes of retroviruses, and HIV composition and structure. It will also provide basic information on the HIV life cycle and identify possible targets for drug development. The HIV viral genome and the cause of the disease are also described. If you want more detailed information you can find it in the subsequent reports from the clinical group.
Introduction
History
We know now that AIDS is caused by the Human Immunodeficiency Virus (HIV), but it was originally observed by its effects on the immune system. An important clue was that AIDS patients often developed a lung infection (or pneumonia) caused by fungus called Pneumocystis carinii. This infection is very rare in healthy individuals, but patients with cancers of the immune system itself (lymphomas) were known to be susceptible to this disease. In 1981, a cluster of cases of Kaposi's sarcoma were observed in patients in San Francisco and New York. Kaposi's sarcoma normally occurs in elderly Jewish men but these patients were all young male homosexuals. Other diseases associated with immuno-compromisation also occurred in this same population; particularly of note was the occurrence of Pneumocystis pneumonia (which is an opportunistic infection) and lymphadenopathy. Later, a similar immunodeficiency was found in intravenous drug users who shared needles, persons who received blood transfusions and hemophiliaces. Moreover, the sex partners of these patients also got the disease. The disease was originally termed Gay-Related Immune Deficiency (GRID) but we now know it as Acquired Immuno-Deficiency Syndrome (AIDS).
HIV causes disease insidiously. The early stages of infection are often not apparent, without visible symptoms. The infected person may feel healthy and appears to be completely normal during that time (the incubation period) but such a person is able to transmit the infection. The HIV incubation period is of variable duration and can be quite long (on average 8 to 10 years). In contrast, for most common virus infections, such as colds or influenza, an incubation period of a few days or weeks will be followed by apparent disease. This adds greatly to the difficulty of studying and controlling AIDS, because many people infected with the virus have not yet developed the disease.
Retrovirus Family
HIV-1 is the predominant AIDS virus and is found worldwide, primarily in Central Africa , Europe and North and South America. A second virus HIV-2, closely related to the simian immunodeficiency virus (SIV), is shown to be endemic in parts of West Africa with limited spread in Western Europe. HIV-2 is only now beginning to appear in the Americas, mainly in the United States, Canada, and Brazil. Infection with either HIV-1 or HIV-2 results in a number of biologic and pathologic changes
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leading to a spectrum of immune dysfunctions, neurologic disorders, enteropathy and AIDS.
The human immunodeficiency viruses are members of the retrovirus family of viruses. The retroviruses are so called because at the beginning of their life cycle they reverse the usual flow of genetic information in a cell. In all living organism and in many other viruses, genetic information is stored as DNA and later transcribed into RNA. By contrast, retroviruses store their genetic information as RNA and contain a unique enzyme, reverse transcriptase (RT), which catalyzes the reverse transcription of the RNA genome (its entire complement of genes) into a DNA copy.
The retrovirus family is composed of three subfamilies : oncoviruses, spumaviruses and lentiviruses (Table 1). The oncoviruses cause cancer and are called cancer-causing viruses. The lentiviruses and spumaviruses do not cause cancer and do not integrate into the host's germ cell line. Both the lentiviruses and the spumaviruses produce a persistent lifelong infection of the host cells. Of the two, only the lentiviruses have been identified as causes of human and animal diseases. Classification of HIV as a lentivirus is based on its fine structure, biologic properties, protein and nucleic acid sequence homology (Table 2).
Table 1 Subfamilies of retroviruses (3) .
SubfamilyExamples
Oncoviruses: associated with the activation of certain cell genes leading to tumor develop
Type AMouse intracisternal type A
Type BMouse mammary tumor virus
Type CMurine leukemia virus
Human T cell leukemia virus type I and II
Feline leukemia virus
Bovine leukemia virus
Type DMason-Pfizer virus
SAIDS virus
Spumavirus: readily isolated from humans and other primates, but have not been associated with any specific disease
Simian foamy virus
Human foamy virus
Lentiviruses: produce acute cytocidal infection followed by a slowly developing multisystem disease
Visna maedi virus
Caprine arthritis encephalitis virus
Equine infectious anemia virus
Feline immunodeficiency virus
Bovine immunodeficiency virus
Simian immunodeficiency virus
Human immunodeficiency virus type 1 (HIV-1) and type (HIV-2)
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Table 2 HIV characteristics resembling those of lentiviruses (3).
Biologic characteristics
Persistent or latent infection
Cytopathic effects (syncytia formation) on selected cells
Capable of infecting macrophages
Associated with immune suppression
Long incubation period
Central nervous system involvement
Affects hematopoietic system
Molecular biologic characteristics
Similar genomic organization
Morphology of virus (cone nucleoid)
Accumulation of unintegrated proviral DNA
Polymorphism, particularly in the envelope gene
Primer binding site (tRNAlys)
Origins of HIV-1 and HIV-2
The genetic similarity between HIV-1 and HIV-2 is significantly less (40-50% nucleotide identity) than is found among different HIV-1 isolates (>85% nucleotide identity). HIV-1 and HIV-2 and other lentiviruses have been discovered in a wide variety of nonhuman primates (Table 3). The nonhuman primate lentiviruses are collectively know as simian immunodeficiency viruses (SIVs). To date, natural SIV infections have not been shown to cause disease in the infected animal. HIV-1 and HIV-2 appear to be closely related to the primate lentiviruses isolated from chimpanzees and sooty mangabey monkeys.
Table 3 Primate lentiviruses (3)
VirusHost
HIV-1Human
HIV-2Human
SIVCPZChimpanzee
SIVSMSooty mangabey
SIVMACRhesus macaque
SIVMNEPig-tailed macaque
SIVSTMverStump-tailed macaque
SIVAGMgriVervet monkey
SIVAGMsabGrivet monkey
SIVAGMtanSabaeus monkey
SIVAGMTantalus monkey
SIVMNDMandrill
SIVSYKSykes' monkey
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Studies of the African green monkey and
their related simian virus (SIVagm) yield
important information in our understanding
of HIV-1 and HIV-2. As see in Fig.1 there are
three major species of African green monkeys
indigenous to Africa.
Fig. 1 African green monkeys (2)
Fig. 2 Geographic domain of African
green monkeys (2)
Fig. 2 shows a map of Africa and indicates
the native locations of different species
of the African green monkey. Within
each species, a unique family of SIVagm
has been show to exist
Structure of HIV
The structure of HIV resembles that
of all retroviruses but particularly that
of the lentiviruses (Fig.3). HIV
has a cycindrical eccentric nucleoid
or core. The nucleoid contains the
HIV genome, which is diploid.
Outer lipid bilayer coat studded with
Surface (SU, gp120), transmembrane
(TM, gp41) glycoprotein complexes.
Beneath the lipid bilayer are matrix
proteins (MA), the virion consist of
Internal capsular (CA) and nuclear
Capsular (NC) proteins which
surround the single stranded RNA
genome.Fig. 3 Structure of HIV (2)
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HIV virion
Fig. 4 shows the components and their
genetic source, the matrix (MA) internal
capsular (CA), and nuclear capsid (NC)
proteins produced by the gag region
contain gene products of the pol
region-RT, integrase and protease.
Fig. 4 HIV Virion (2)
Life cycle of the human immunodeficiency virus
Fig. 4 Life cycle of HIV (2)
HIV and related lentiviruses have growth cycles that are typical of all retroviruses. It is convenient to think of viral growth as four distinct stages:
- Infection: The HIV-1 virus binds to the CD4 receptor complex on the surface of CD4+ cells. The virion then enters the cell, and uncoats.
- reverse transcription and integration : The HIV-1 virus undergoes the process of reverse transcription in which viral RNA is transcribed into complementary DNA. This is the portion of the life cycle at which all currently available antiretroviral agents are designed to intercede.
- viral gene expression : After reverse transcription, the DNA becomes double-stranded and migrates to the cell nucleus, where it is integrated into the host genomic DNA as a provirus.
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- virus assembly and maturation: The virus can then be transcribed back into mRNA and genomic RNA, and the resultant proteins and genomic RNA are assembled near the surface of the cell and packaged into a new virion, which buds from the cell membrane (2).
Soon after infection of the cells, the viral RNA genome is reverse transcribed into a DNA copy, transported to the nucleus and integrated at random sites in the chromosome. Once integrated, the proviral genome is subject to transcriptional regulation by the host cell, as well as its own transcriptional control mechanisms. The later stages of the life cycle involve expression of the viral genes and eventual assembly and release of virus particles
How it might be stopped (Drug develpoment )
- RNA is converted into double strand DNA by RT
-Drugs called RT inhibitors can interrupt this process. ART inhibitor drugs, such as AZT and 3TC, can disrupt the early stage of viral reproduction.
- The integrase enzyme incorporates the virus genetic material into the T cell's DNA
-Drugs called integrase inhibitors, which are designed to halt this process, are in development
- Disrupting the assembly line
The protease enzyme cuts viral proteins into shorter pieces so that they can become functional proteins and allow the infection of other cells.
-Protease inhibitors block this stage of reproduction by neutralizing the enzyme. They are even more effective when combine with RT inhibitors.
In this electron micrograph
(see Fig. 5), the virus can be seen
budding forth from the surface of
a cell. Note how the outer membrane
of the virus is composed of the lipid
bilayer membrane of the host cell
studded with integrated protein
products (envelop proteins) of
the virus (2).
Fig. 5show viral budding (2)
The Genome of HIV
The HIV genome is 9749 nucleotides, about the same size as any other retrovirus, for example Rous sarcoma virus (RSV). But the genome of HIV is more complex than RSV since it has extra open reading frames that clearly code for small proteins. Some of these are protein synthesis controlling proteins.
The HIV genome has nine open reading frames but 15 proteins are made in all.
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The GAG/POL polyprotein and the ENV polyprotein are cleaved into several proteins:
GAG is cleaved to : MA (matrix), CA (capsid), NC (nucleocapsid), p6
POL is cleaved to: PR (protease), RT (reverse transcriptase), IN (integrase)
ENV is cleaved to: SU (gp120) and TM (gp41)
Of the other proteins, three are incorporated into the virus (Vif, Vpr and Nef) while three are not found in the mature virus: Tat and rev are regulatory proteins and Vpu indirestly assists in assembly.
TAT: Trans-Activator of Transcription
REV: Regulator of Virion protein expression
NEF: Negative Regulatory Factor
VIF: Virion Infective Factor
VPU: Viral Protein U
VPR: Viral Protein R
These genes encode small proteins. They overlap with the structural genes (especially ENV) but are different reading frames. Note some are encoded by two exons (unlike the structural genes) and therefore their mRNAs can be derived by alternative splicing of structure gene mRNAs. Mutants in the TAT and REV genes show that they are both vital to any production of virus.
TAT gene product binds to a sequence in all the genes and positively stimulates transcription. It is thus a positive regulator of protein synthesis, including its own synthesis.
REV bind to an element only in the mRNA of structural proteins (GAG/POL/ENV) and regulates the ratio of GAG/POL/ENV to non-structural, controlling protein (TAT/REV) synthesis.
NEF despite its small size NEF has several functions
a)Homeostasis leads to several problem for the parasitic: super-infection by other HIV particles.
b)By a different mechanism from its down regulation of CD4 antigen, NEF reduces surface expression of MHC class molecules. This alters antigen presentation by the infected cell and is proposed to protect the infected cell from attack by cytotoxic T cells.
c)NEF is important for HIV replication in vivo but there seems to be little effect of NEF in an in vitro cell culture situation.
Fig. 6 HIV genomic map (2)
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This genetic map of the HIV-1 viral genome depicts the structural and regulatory genes in their relative position as well as their products and functions. The 9-kb RNA virus is flanked by a long terminal repeat (LTR) section on both the 5' and 3' ends of the virus, which serves as a promoter and binding site for host and viral transactivating factors. The TAR element exists within the R region of the LTR and serves as a binding point for the tat gene product (a potent transcriptionalactivator). The gag region encodes the nucleocapsid core and matrix proteins. The pol gene codes the reverse transcriptase, protease, and integrase enzyme. The envelope region (env) is responsible for the viral-coat glycoproteins, gp120 and gp41, which mediate CD4 binding and membrane fusion. The remaining genes (vif, vpr, vpu, rev and nef) are regulatory genes whose products play critical roles in controlling viral expression, trafficking of viral gene products within the infected cell, and viral infectivity. The rev-responsive element (RRE) is the binding site for the rev gene product, which is important for the transport of unspliced and singly spliced RNA massage from the nucleus (2).
HIV subtype
The two types of HIV can be distinguished genetically and antigenically.
HIV-1 is the cause of the current pandemic while HIV-2 is found in west Africa and rarely elsewhere. The HIV-2 type is closely related to simian immunodeficiency virus (SIV) found in west Africa. There are also 10 different HIV-1 subtypes. The major one in the US and Europe is type B. In some countries, mosaics between different subtypes have been found.
HIV binding via CD4 receptor
The HIV virus binds to the cell surface of a CD4
Lymphocyte. The binding attachment occurs
through an interaction of the viral glycoprotein
gp120/gp41 and the CD4 receptor complex on
the cell surface (see in Fig. 7).
Fig. 7 HIV binding via CD4 receptor (2)
The gp41 fragment consists of cytoplasmic
tail and a hydrophobic membrane-spanning
domain and is joined with the larger gp120
component via a fusion domain. The gp120
glycoprotein has several glycosylation sites
and hypervariable loops (eg. V3), which lead
to antigenic variation between viral strains.
The cd4-binding region is located toward
the center of the complex and consists of
components from both the gp120 and gp41
fragment.
Fig.8 Envelope glycoprotein complex of HIV-1 (2)
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The couse of the disease (5)
Usually from the time of infection till the clinical manifestation of AIDS a period of 8-10 years goes by. However, in certain cases this period may be two year or less. Approximately 10% of patients succumb to AIDS within 2 to 3 years.
- Acute infection (acute retroviral syndrome)
HIV infection produces a mild disease that is self-limiting. This is not seen in all patients. In the period immediately after infection, virus titer rises (about 4 to 11 days after infection) and continues at a high level over a period of a few weeks. The patient experiences some mononucleosis-like symptom (fever, rash, swollen lymph glands but none of these are life-threatening. The result is an initial fall in the number of CD4+ cells and a rise in CD8+ cells but the numbers quickly return to near normal levels.
- A strong cell-mediated and humoral anti-HIV immune defense
Cytotoxic B and T lymphocytes mount a strong defense and the virus largely disappears from circulation. During this period, more than 10 billion new particles are produced each day but they are rapidly cleared by the immune system and have a half life of only 5-6 hours. The infected cells that are producing this virus are destroyed either by the immune system or by the virus (half life about 1 day). However, the rate of production of CD4+ cells can compensate for the loss of cells and a steadstate is set up in which a very small fraction of the resting memory CD4+ cells carry an integrated HIV genome. Most CD4 cells at this stage are uninfected.
The virus disseminates to other regions including lymphoid and nervous tissue. This is the most infectious phase of the disease. Seroconversion occurs between one and four weeks after infection.