Tuesday 10 July 2012
Friday 6 July 2012
Side Chapter: Forms of HIV immunity/resistance
Abstract - This interview actually concurs the concept
of innate immunity to HIV. The interviewee, Jay Levy from the University of
California talks about a particular aspect of the cellular immune response
known as CD8 cell antiviral factor which he
believes play an important role in successfully suppress the viral load of HIV
thereby limiting its progress. He also discuss the possibility that drug
manufacturing companies could perhaps develop a vaccine that could induce
similar effects on infected HIV-positive patients.
Abstract -- This articles shows that the innate immunity that some people have may be due to a
genetic defect that result in the absence of CCR5 receptor, the
receptor that HIV take advantage of to gain entrance into a host cell. Interestingly,
individuals who inherited a pair of the defected genes display apparent
immunity to HIV infection. While individuals who inherited only one of the
defected gene are not completely immune to HIV infection, they display
greater resistance to the progression of the virus.
Abstract -- This article attributed the ability to
keep the virus load in check to the ability of the immune system killer T cells
to recognize infected cells. Through a series of experiments, researchers have
found that the underlying ability of these HIV controllers (people who are able
to naturally suppress the viral load) may have to do with the unique protein
sequence of the killer T cell receptors. The researcher also discuss about the
possibility of developing a vaccine that could induce the production of these
effective killer T cells.
Wednesday 4 July 2012
Chapter II: How to kill HIV (HAART)
As promised, now that you have a greater understanding about the mechanism of HIV replication, now its time to explore some ways to counteract it or simply put kill it. Enjoy. ^^
Classes of drugs used in HIV treatment (Highly Active Antiretroviral Therapy)
1. Nucleoside
Analogs (Competitive substrate inhibitor) [1]
AIDS (acquired immunodeficiency syndrome) is caused by infection with the retrovirus HIV (human immunodeficiency virus). A key step in the life cycle of this virus is synthesis of a DNA copy of the viral RNA genome, catalyzed by a reverse transcriptase. Reverse transcriptase is a major target of chemotherapy because it is not essential for normal cells.
AZT (3’-azido-2’,3’-dideoxythymine; Zidovudine) was the first drug approved for treatment of HIV infection. It is a nucleoside analog with an azido group on the sugar. It can be phosphorylated into triphosphate from, which competes with dTTP (deoxythymine triphosphate) for incorporation into the reverse transcript. Once incorporated, it terminates the growing chain of the transcript because the azido group on the 3’ carbon of the sugar is not a substrate for nucleotide addition. AZT is much less efficient at competing with the more accurate cellular DNA polymerases, providing a therapeutic window in which the effect is primarily upon viral replication. (Since the effects of faulty DNA synthesis by AZT affects the virus more efficiently than it does human cells) Nevertheless, side effects include toxicity to bone marrow, which contains rapidly dividing cells, and myopathy that might be related to toxicity to mitochondria, which contain their own DNA polymerase (pol delta). DDI (2’, 3’ dideoxyinosine; didanosine) and dideoxycytidine (zalcitabine) also function as chain terminators after incorporation of their phosphorylated derivatives by the HIV reverse transcriptase.
2.
CCR5 receptor antagonist (Competitive
substrate inhibitor) [2]
These are the first antiretroviral drugs which do not target the virus directly. Instead, they bind to the CCR5 receptor on the surface of the T-Cell and block viral attachment to the cell. Most strains of HIV attach to T-Cells using the CCR5 receptor. If HIV cannot attach to the cell, it cannot gain entry to replicate. Currently, three pharmaceutical companies are trying to push through FDA approval with their
small molecule CCR5 antagonist however Maraviroc is the only FDA approved drug as of now.
Putative binding of Maraviroc to the CCR5 receptor
The strongest interaction is estimated to be between maraviroc and glutamic acid (Glu283) through a strong salt-bridge interaction. Types of interaction with CCR5:
* II – T-shaped π-π stacking
* III – parallel displaced interaction
* V – hydrophobic interaction
* VI – limited interaction
* VII – salt-bridge interaction
3. Reverse transcriptase inhibitor (Non-competitive
inhibitors) [3]
Non-nucleoside reverse transcriptase inhibitors inhibit reverse transcriptase by binding to an allosteric site of the enzyme. (Thereby changing its shape and loss of enzymatic activity) Examples of these inhibitors are Efavirenz and Nevirapine.
4. Protease inhibitor (Non-competitive inhibitor}
Protease inhibitors (PIs) target viral assembly by inhibiting the activity of protease, an enzyme used by HIV to cleave nascent proteins for the final assembly of new virions. (Thereby resulting in immature HIV that is non-infectious)
5. Integrase inhibitor (Non-competitive inhibitor)
Integrase inhibitors inhibit the enzyme integrase, which is responsible for integration of viral DNA into the DNA of the infected cell. There are several integrase inhibitors currently under clinical trial, and raltegravir became the first to receive FDA approval in October 2007.
Reverse transcriptase do not carry out proofreading, thus their
error rate is much higher than that of cellular DNA polymerases. This high
error rate complicates the treatment of AIDS, because the population of viruses
carried by any one patient contains many mutants. Some of these mutants are
likely to be resistant to any given therapeutic agent. Thus, many drugs
initially reduce the viral load, but later become ineffective due to the
selective growth of the viruses in which the drug target is mutated to an
insensitive form. Combination therapy, with multiple drugs that target
different viral proteins, is an attempt to circumvent this problem.
How reverse transcriptase inhibitor works? (Animation)
How protease inhibitor works? (Animation)
References
[1] Glitz, D.(2006). Textbook of Biochemistry With
Clinical Correlations Sixth Edition. Canada: Wiley-Liss.
Chapter I: The Inner Workings of HIV
As far as the
phrasing goes: Know your enemy and know your enemy well in order to win the
day. It's a little cliche but a touche ^^
In order to fully fathom the premise of HIV treatment or possibly
cure, we must first be able to understand how this little midget works
Entry (This virus do know how to make an entrance^^): [1]
HIV
infection is specific to certain human immune cells (helper T-cell) due to the
presence of the protein CD4 (exclusive to helper T cells) which acts as a
receptor that allow the virus to enter the cell; other than the CD4 receptor, a
secondary receptor CCR5*
(Chemokine Co-receptor) is also needed. After the virus attaches itself to
these cell-surface receptors, it then fuses the viral membrane and the cell
membrane and inject the viral particles into the cell while leaving its
membrane protein behind.
Reverse Transcription
and Integration
After
the virus make its way into the cell, its matrix and capsid protein break down
to release the viral genetic material. Then the enzyme, reverse transcriptase* that the
virus brings along with it starts acting on the viral mRNA to transcribe a
complementary DNA or cDNA. Now, another enzyme that the virus brought along, integrase* would bring the
viral DNA into the cellular nucleus and integrate that piece of viral DNA into
the human DNA, which dawns upon the start of a life-long infection as the virus
take advantage of the cellular machinery to create more copies of itself and
infect neighboring cells. Once integrated, the HIV DNA is known as provirus.
Transcription and
Translation
HIV
provirus may lie dormant within a cell for a long time. But when the cell
becomes activated, it treats HIV genes in much the same way as human genes.
First it converts them into messenger RNA (using human enzymes). Then the
messenger RNA is transported outside the nucleus, and is used as a blueprint
for producing new HIV proteins and enzymes.
[2]Interesting tidbits: While
HIV only has 9 genes, it’s able to take advantage of mRNA slippage and a change
in reading frame to generate different protein from the same message
(Programmed frameshifting in biosynthesis of HIV protein). A single mRNA,
designated gag-pol, encodes for two polyproteins that overlap by about 200
nucleotides and are in different reading frames. The gag polyprotein is
translated from the initiation codon to an in-frame termination codon near the
gag-pol junction.; gag polyprotein is then cleaved to generate several
structural proteins of the virus. However about 5% of the time a one-nucleotide
frameshift occurs within the overlapping segment of the mRNA and the
termination codon is bypassed because it is no longer in the reading frame. A
gag-pol fusion polyprotein is produced; proteolytic cleavage of the pol
polyprotein produces the viral reverse transcriptase and other proteins needed
in virus replication.
Assembly, Budding and Maturation
Among the strands of messenger RNA produced by
the cell are complete copies of HIV genetic material. These gather together
with newly made HIV proteins and enzymes to form new viral particles. The HIV
particles are then released or 'bud' from the cell. The enzyme protease* plays a vital role at
this stage of the HIV life cycle by chopping up long strands of protein into
smaller pieces, which are used to construct mature viral cores.
The newly matured HIV particles are ready to
infect another cell and begin the replication process all over again. In this
way the virus quickly spreads through the human body. And once a person is
infected, they can pass HIV on to others in their bodily fluids.
If you are too
lazy to read the whole process, here's an olive branch ^^:
References:
[2] Glitz, D.(2006). Textbook of Biochemistry With
Clinical Correlations Sixth Edition. Canada: Wiley-Liss.
Preface: Introduction to blog
This blog would be dedicated to NP Medical Biochemistry project, and we would be working on Blood-borne disease: HIV infection. Hope you enjoy^^
What is HIV? [1]
HIV or the Human Immunodeficiency Virus targets vital cells (helper T-cells, specifically CD4+ T-cells, macrophages and dendritic cells) in the human immune system thereby compromising one's ability to fight off infection. While someone may be HIV-positive (infected with HIV), the signs and syntomns of the infection may not be obvious or it may not even present any syntomns of unwell; which in the words of a virologist - HIV is a very good (elusive) virus or rather it presents an interesting set of problems. While there are therapies and drugs (High Active Antiviral Therapy HAART) that can specifically target the proliferating virus, a lot of times it just ends in empty hope; as that small window of being "cured" of the virus is but a brief respite, or a guise for the virus latency as it awaits safely within the host for another chance to start propagating. So while being infected may not affect a person in one or two day's time, it sure as hell would do a lot of damage as the AIDS becomes fully-blown, as the immune system give way to your daily interaction with a cocktail of diseases. (Perfect condition in which opportunistic infections and cancer thrives)
Signs & Syntomns of HIV infection [2]
As the HIV come out of it latency and it can start infecting the healthy cells that carry the protein CD4 (e.g macrophage , dendritic cells and CD4+ T cells). As the CD4+ T cells population dwindles due to HIV infection, the body's capability to recognize pathogens and target them also starts to fail; which enables these opportunistic pathogens that would normally elicit an immune response from the helper T-cell to bypass the screening process completely. This then increase the likelihood for opportunistic infections:
References
[1] http://en.wikipedia.org/wiki/HIV
[2] http://www.ucsfhealth.org/conditions/aids/signs_and_symptoms.html
What is HIV? [1]
HIV or the Human Immunodeficiency Virus targets vital cells (helper T-cells, specifically CD4+ T-cells, macrophages and dendritic cells) in the human immune system thereby compromising one's ability to fight off infection. While someone may be HIV-positive (infected with HIV), the signs and syntomns of the infection may not be obvious or it may not even present any syntomns of unwell; which in the words of a virologist - HIV is a very good (elusive) virus or rather it presents an interesting set of problems. While there are therapies and drugs (High Active Antiviral Therapy HAART) that can specifically target the proliferating virus, a lot of times it just ends in empty hope; as that small window of being "cured" of the virus is but a brief respite, or a guise for the virus latency as it awaits safely within the host for another chance to start propagating. So while being infected may not affect a person in one or two day's time, it sure as hell would do a lot of damage as the AIDS becomes fully-blown, as the immune system give way to your daily interaction with a cocktail of diseases. (Perfect condition in which opportunistic infections and cancer thrives)
Signs & Syntomns of HIV infection [2]
As the HIV come out of it latency and it can start infecting the healthy cells that carry the protein CD4 (e.g macrophage , dendritic cells and CD4+ T cells). As the CD4+ T cells population dwindles due to HIV infection, the body's capability to recognize pathogens and target them also starts to fail; which enables these opportunistic pathogens that would normally elicit an immune response from the helper T-cell to bypass the screening process completely. This then increase the likelihood for opportunistic infections:
Opportunistic Infections: Brain
References
[1] http://en.wikipedia.org/wiki/HIV
[2] http://www.ucsfhealth.org/conditions/aids/signs_and_symptoms.html
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