Monday, December 31, 2007

New Years Eve 2007,Alone Watchin Movies & Blogging-






So ya its new years eve and i find myself alone.Not thats not normal these days...its not to bad but it would be better if i liked myself alittle better maybe?who knows not me,New Years Resolution...i resolve to get all my ID back & get my licence & get a bike i am going to need it,off road preferably,& i have to go into Dr dube & tell him i want to start going off of this methadone at a tapered slope,hopefully to be off by 2009/10.i def want to be off by 2011 & want to be where-ever i research to be the safest area to live in the next few yrs.Earth Quakes R gonna be more & worse.Its the pandemic i am worried about~as i am HIV+ i am easily overcome by things ordinary persons can fight off.Well i wish all my fellow HIV-AIDs WARRIORS PEACE,LOVE & HAPPINESS & A GREAT NEW YEAR!!!

Monday, December 24, 2007

HIV+ WARRIORS NEED TO CREATE FRONT LINES OF ATTCK IN THE WAR ON HIV-AIDS!!1



HIV+ WARRIORS ARE NEEDED TO CREATE "FRONT LINES"OF ATTACK
WE NEED To START BLOGS,WEBSITES,PODCASTS,WEBCASTS,PODWEBCASTS,WATEVER IT TAKES TO GET OUR POINT OF VIEW OUT TO THE PUBLIC,SCREAM & YELL IF U HAVE TO!~THE MORE FRONT LINES OF ATTACK WE CREATE,THE BETTER OUR CHANCES OF WINNING-BLOG ABOUT WHAT ITS LIKE TO LIVE EVERYDAY WITH HIV OR AIDS.THE STIGMA & OUTRIGHT DISCRIMINATION WE ALL FACE BY FAMILIES,FRIENDS & EVEN LOVED ONES.THE REACT TO THEIR FEARS MOST OF THE TIME.WHO WANTS TO CATCH HIV-AIDS ON PURPOSE RIGHT?YOU WOULD BE SHOCKED TO FIND OUT THAT IN FACT THEIR ARE MANY PEOPLES THAT TRY & GET INFECTED ON PURPOSE=EXAMPLE OF THIS WAS OUT ON THE WEST COAST WHERE NATIVES TRYIED CATCHING IT ON PURPOSE & THEIR REASON?=THEY NEEDED THE 200 EXTRA DOLLARS THAT HIV+ PERSONS GET FOR A FOOD ALLOWENCE!!!IN PEOPLES THINK THAT POVERTY IS NON EXISTENT IN CANADA!!!PEOPLES ARE VERY WRONG,AS I PERSONALY KNOW MANY THAT LIVE WELL BELOW THE POVERTY LINE.PRICES OF PRODUCE HAS GONE UP DISABILITY PENSION CHECKS HAVE NOT KEPT PACE WITH INFLATION RATES.iT NEVER SEEMS TO GET ANY BETTER DOES IT?bUT HAVE FAITH & HOPE,KEEP THEM CLOSE AS THEY WILL BE NEEDED ALOT,ESPECIALLY ID U TEST hiv+!!!PEACE N LOVE NOT WARS N WALLS EH FOLKS!!!SAFE SEX SAVES LIVES SO SAVE A LIFE TODAY!THE LIFE YOU Save could be your own if your smart and use a condom!!!

Monday, December 17, 2007

(RED) AIDS Fact #2

its not up to 6,500 everyday FOLKS!!!

Saturday, November 24, 2007

Just for Now,Clean Anyhow!






So today its back to being overcast skies,& that its to the depressing feelings i am going through at this time.Finaly scored a Q of weed so i should be eating normal again soon.Seems if i dont smoke i dont have any dsesires to eat anything at all.Its boring living alone and i am longing for female companionship bigtime.I feel rough today,like i been in battle,and me bones R sore for the days.I would love to hold my mates hands while we walked along ,strolling who knows where,or when.All i know is its not happening now~~sad but truer words fer sure eh!Living with HIV is no picnic,and thats an understatement!

Now i am sure we are living in what the bible says are the END TIMES,and i am alone??shitty buzz or wat?i hate being single and am not used to being so alone all the time.I am used to peoples always being around,or used to be.now it seems like i am always alone,& christmas sucks as wellas valentines day,all these "special days that society says we must spend cash on our loved ones.Sounds like a conspiracy to me.Big corp. making monies while we grow old and die.They have us pegged from birth to death,on wat we buy,need,eat,&how our health is.Its all on record i'm sure ,somewheres theres data on us all.I see the Chinese as the next world power,& scary to think of shoddy stuff being shipped all over,and everything as well.From pills to pots to pottys,they have found a way to make everything cheaper,faster& therefore cost less to ship n sell.

Tuesday, November 20, 2007

OPEN LETTER=RESULT FROM ONE'S EMAIL CAMPAIGN A SUCCESS!!!

An Open Letter to Civil Society Organizations on the Fund's Debt Relief for Liberia
By Masood Ahmed, Director of the IMF's External Relations Department
November 14, 2007

I am pleased to inform you that on November 12, 2007, the International Monetary Fund (IMF) has secured adequate pledges from member countries for the cost of the IMF's debt relief to Liberia, amounting to SDR 530 million (US$842 million) (See Press Release No. 07/254). We have received a large volume of emails on this topic, so this letter is being posted because it is impossible to respond to each message individually.

As Mr. Dominique Strauss-Kahn, Managing Director of the IMF, noted in his statement announcing the debt relief package, this breakthrough was achieved thanks to the leadership of President Johnson-Sirleaf and her economic team and the generous support from a wide group of contributors, including from low-income countries. I take this opportunity to also thank all those who have expressed their concerns about Liberia's debt situation. Their strong support to the cause of debt relief contributed to the broad donor support that made this financing possible. It is expected that Liberia will soon join the 32 countries that have already received full or partial debt relief under the HIPC Initiative.

The pledges are being formalized, following which Liberia and the IMF will initiate a process of arrears clearance and new Fund financing that will enable the delivery of IMF debt relief to Liberia.

The IMF remains committed to supporting Liberia in its efforts to achieve economic recovery and poverty reduction.

Sincerely yours,
Masood Ahmed
Director, External Relations Department
International Monetary Fund




IMF EXTERNAL RELATIONS DEPARTMENT
Public Affairs Media Relations
Phone: 202-623-7300 Phone: 202-623-7100
Fax: 202-623-6278 Fax: 202-623-6772



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Monday, November 19, 2007

HIV & ME A POEM BY JAMES JOEY GOUGH






ITS ALMOST IMPOSSABLE I WOULD VENTURE TO SAY,when will love come my way?I been poz since 2001,let me tell you it hasn't been fun!!At first i was angry,then depressed,i didnt know if i would regress,about HIV,i knew even less!!!So i read and researched on this Virus callede HIV,i wanted to know what was killing me,slowly but surely it killed my desire,but now i was off of that cokecaine highwire,and my head slowly cleared from its deep quagemire.I lost so many friends and loved ones too,HPV,HIV & hep-abc just to name a few,diseases and drugs go hand in hand like a spreading evil across this great land,Drs and scientists searching for cures,while pain and suffering are what we endure,money pours in from all kinds of places,the guilt and greed on rich mens faces,money money money,its all i hear,how shortfalls and cutbacks are always near,and of course its always the poor,that are hit that hardest and yet they endure and have no fear,could it be their faith and hope?thats brought them through the slippery slopes?of life and trials and tribulations,of the joy and love & constelations,of dreams unfulfilled & desires unmet,so many gone never to see the sunset,lost to us early ,no more to rise,Untill the end of days ,no more blue skies,this isnt the way,kindness and love are what we need,to practice and promote,love and not greed,Jesus & Bhudda & Alah too,all knew love would see them through,For isnt this what each one preached?So why the Wars,i cryed,i beseached,to stop this stigma & discrimination that has engulfed so many a nation,So wars & fighting are not the right way,to love our naybers now this we may,hope to win this end to fighting,Then this poem would need no writing,to try and change Mans love of War,into a war of love,why isnt this what He said from HIM above,that man should practice alot more LOVE,so this it it i got to go,i 'm off,I have HIV and my name is joe!JOE GOUGH!!!!typed today by james "joey"gough,sudbury ontario canada GODBLESS ALL MY FELLOW HIV-AIDS WARRIORS WITH PEACE,LOVE,AND HAPPINESS 4 EVER!!

Tuesday, November 6, 2007

THINK GREEN & VOTE NDP=THINGS THAT ARE COOL IN 07~!!!

As a PHA speaker going out into the community telling others my life story is very rewarding work.I know not everyone is able to do this & thats cool.there are other ways to be a warrior trying to stem the stigma & discrimination & bring HIV-AIDs issues to other peoples.Blogs are a great example,as you can be who-ever u want,personally i have chosen to just use my own name & face to what i type or blog as i have numerous of them things going ,it sometimes gets confusing,avoid my mistake and stick to under ten blogs.I have about 20 blog sites & it does get confusing,but i look at like this,=I am creating "Front Lines" in the War on HIV-AIDS!!!Join myself & alot of other PHA Warriors & start your own front line on the War against HIV=AIDS!!peace n love not wars n walls folks~~!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!
PS.JACL LEIGHTON SAYS HE WANTS TO LEGALIZE WEED~!I SAY I AM VOTING NDP~!!AS A PERSON LIVING WITH HIV,I NEED EASIER ACCESS TO THIS MEDICINE.JOIN ME & VOTE NDP~!!!!

Saturday, November 3, 2007

FISH OIL TO BE STUDIED=OMEGA-3 FATTY ACIDS TO HELP FIGHT HIV=AIDS







Fish oil, inflammation and metabolic complications in HIV: a clinical trial and related research
November 2, 2007

We noticed with interest that Dr. Todd T Brown, a Johns Hopkins researcher who has studied body fat changes in people with HIV, has recently started a wide-ranging investigation of fish oil / omega-3 fatty acid supplementation as a way of preventing/treating metabolic complications associated with highly active antiretroviral therapy (HAART). Metabolic complications, including fat wasting, central body fat build-up, insulin resistance, high cholesterol and triglycerides, and bone loss, have been some of the major side effects experienced by people with HIV on medication, so it’s quite interesting to see research that may “connect the dots” and find links between these various problems.

Furthermore, this is a study that focuses on fish oil / omega-3 fatty acids, which have quite recently gained more respect in US medical circles, especially as a means of preventing/treating cardiovascular disease, but also for a surprising effect on depression. (You can read more about this aspect of fish oil supplementation in the “depression” category on this blog.)

Here’s the description of Dr. Brown’s research, as provided on the website of NCCAM/NIH, one of the major sponsors of the study:

Abstract: DESCRIPTION (provided by applicant): The overall goal of this proposal is to understand the role of inflammatory cytokines in the metabolic and skeletal abnormalities in HIV disease and to determine whether omega-3 fatty acid supplementation, in the form of fish oil, will alter the pathophysiology of these clinical disorders. Complementary and alternative medicines (CAM) are used widely among HIV-infected patients, often with the hope of preventing or treating complications associated with highly active antiretroviral therapy (HAART). Metabolic abnormalities, including peripheral fat wasting, central adiposity, insulin resistance, and dyslipidemia, and skeletal abnormalities (reduced bone mineral density and high bone turnover), are common in HIV-infected patients on HAART, yet their relationship is unclear. We hypothesize that these metabolic and skeletal abnormalities are related by abnormal inflammatory cytokine expression and that these conditions can be improved with fish oil, a widely-used CAM agent with anti-inflammatory properties. We have the following specific aims: 1) To understand the association between the metabolic and skeletal abnormalities in HIV-infected subjects and their relationship to inflammation, 2) To determine whether treatment with omega-3 fatty acids will have hypotriglyeridemic, anti-inflammatory, and anti-bone resorptive effects in a randomized trial of HIV-infected patients, and 3) To clarify the mechanisms of action of omega-3 fatty acids, namely the effect on lipolysis and bone turnover using stable isotope infusion techniques. To accomplish our specific aims, I intend to do a secondary analysis of data from two cohorts of HIV-infected subjects, and to then perform a randomized trial using a standardized fish oil product. These results will help to define the pathophysiology of the metabolic and skeletal abnormalities in HIV and evaluate the efficacy and potential mechanisms of action of an important complementary treatment […]

(According to the published information, the clinical trial of fish oil is scheduled to run from 2006-2010.)

Note: An interview with Dr. Brown on body fat changes in people with HIV can be found on the website of our friends at www.thebody.com.

Entry Filed under: cholesterol, diabetes, hiv, insulin resistance. Tags: cholesterol, fish oil, HAART, HAART side effects, hiv, lipodystrophy, lipodystrophy and HIV, metabolic syndrome, Omega-3 fatty acids, triglycerides.

Tuesday, October 30, 2007

HIV EXPLAINED

Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 1 June 2005
Answers to questions from Sections 1-7 of Treatment training for advocates.
This manual is available online in English and Russian from:
HIV i-Base
http://www.i-Base.info
Section 1
1. AIDS stands for:
- Acquired
- Immune
- Deficiency
- Syndrome
2. A CD4 cell is a white blood cell (lymphocyte) that signals CD8 cells to destroy a virus.
HIV uses CD4 cells as factories to reproduce in.
3. A CD8 cell is a white blood cell (lymphocyte) that kills cells that are infected with
viruses (i.e. HIV).
4. The ‘normal’ range for CD4 count in an HIV-negative adult is between 600 and 1600
5. CD4 cell is also called a helper cell, a CD4+ T-lymphocyte, CD4+ T-cell, and
sometimes just T4 cell); CD8 is also called a killer cell
6. CD4% is the percentage of total lymphocytes that are CD4 cells. It is used as a more
stable indication of whether there has been a change in the immune system. Children
are monitored using CD4%.
7. Cellular immune responses are based on CD4 and CD8 responses. Humoral immune
responses are based on antibodies.
8. A surrogate marker is an indirect measure for something else that cannot be easily
measured directly (i.e. the CD4 count is a measure for the disease progression).
9. US and UK treatment guidelines recommend routine CD4 and viral load monitoring
every three months, whether on treatment or not on treatment. These tests should also
be done before any treatment change, and 2-4 weeks after any treatment change. i.e.
4 weeks after starting treatment. Is any one test result produces an unexpectedly high
or low results, it should be repeated. In some countries with limited access to these
tests, they are performed less frequently – perhaps every 6 months.
10. Some guidelines (WHO, UK) would recommend starting treatment before the CD4
count has fallen below 200, while others (US) would recommend before 350.
11. A few weeks after the infection, the CD4 count usually falls, then the immune system
fights back and the count goes back again but not to the levels that it was before HIV
infection. From then on the CD4 count goes down gradually and it takes from 2 to 10
years usually to drop down to 200.
12. Please see graph on page 15.
13. The following OIs become more common below these CD4 levels:
CD4<300 - diarrhoea from microsporidia and cryptosporidia
- skin problems-candida (thrush), dry skin, etc.
<200 - PCP (pneumonia) and chest infection
- toxoplasmosis-a parasitic infection that commonly causes brain
lesions
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 2 June 2005
<100 - MAI/MAC-bacterial infection similar to TB
- Cryptococcus infection-fungal infection that can cause meningitis in the
brain and PCP-like symptoms in the lungs
<50 - CMV (cytomegalovirus)-a viral infection that can cause permanent
vision loss or blindness
14. Children have much higher CD4 counts than adults. Babies have higher CD4 counts
than children. Over time and as the people age their CD4 count drops gradually.
15. An antigen is the term for infectious material produced by a virus or bacteria.
16. Antibodies are cells in the immune system that recognise antigens.
Section 2
1. HIV is a virus. HIV stands for Human Immunodeficiency Virus.
2. Only 2% of HIV or HIV-infected CD4 cells are in blood.
3. HIV and HIV-infected CD4 cells are mostly in the lymph system and lymph nodes.
4. Blood is the most accessible compartment for regular monitoring.
5. A sanctuary site is the term for a compartment of the body that has barriers that limit
both HIV and HIV drugs from moving freely. The main compartments are the genital
tract, the cerebral spinal fluid and the brain.
6. Viral load levels can be different to blood in each compartment. For example someone
can have undetectable viral load in blood but detectable viral load in semen.
Resistance can also develop independently in different sites.
7. Four main causes of illness include
- Bacteria
- Fungi
- Viruses
- Parasites/protozoa
8. During the first few days and weeks after the infection, the viral load (VL) goes very
high, very quickly. Its levels can reach over 1,000,000 copies. Then, during the
seroconversion, the immune system starts producing antibodies in order to fight back.
As a result the viral load goes down (sometimes to below 50 copies). During the
chronic infection the viral load progressively and consistently goes up to the point when
the person starts ARV therapy. After that, with proper treatment regimen the VL
becomes ‘undetectable’ (below 50 copies).
9. Please see the graph on page 26.
10. The viral load test was developed as a research tool during the 1990s. The first test in
1995 could only measure down to 10’000 copies/mL. By 1996-7 the tests were able to
measure down to 400-500 copies/mL. Since 1998 the most routinely used test
measure down to 50 copies/mL, although some tests are even more sensitive and can
measure down to 5 copies/mL.
11. i) PCR (Polymerase Chain Reaction) – the most widely used test
ii) bDNA (branched DNA)
iii) NASBA (Nucleic Acid Sequence Based Amplification)
12. All tests have an approximately 3-fold margin of error (i.e. a test result of 30’000 means
that the real number could potentially be anywhere between 10,000 and 90,000)
13. Firstly, the viral load test shows whether the drugs work in a combination are initially
working. You need to see a minimum –1log reduction in the first month and aim to be
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 3 June 2005
<50 by 3-6 months. In someone who is on treatment with an undetectable viral load,
continued monitoring confirms that the drugs are still working.
14. If the levels are very high (>100,000), then this might be seen as a reason to start
treatment at a higher CD4 count than 200, even though the VL is not as important at
predicting the risk of opportunistic infections as the CD4 count.
15. HIV makes mistakes when replicating. Those mistakes are called mutations. When on
treatment, some mutations will not be affected by the drugs. If these mutations
develop, they will continue to reproduce. The ‘selective pressure’ from the drugs will
force the resistant virus to eventually become the major type of HIV in the individual.
He/she then becomes is said to be resistant to those drugs and cross=resistant to
similar drugs that have the same resistance pathway.
Section 3
1. ARV stands for ‘Antiretroviral’
2. A minimum of three drugs, but can be more
3. i) NRTI-Nucleoside Reverse transcriptase Inhibitors (‘nucleosides’ or ‘nukes’)
ii) NNRTI-Non-Nucleoside Reverse Transcriptase Inhibitors
iii) PI-Protease Inhibitors
iv) EI-Entry Inhibitors
4. Entry inhibitors
5. In June 2005 22 including co-formulated drugs (ie AZT+3TC; tenofovir+FTC etc)
6. In June 2005 there were four combinations recommended by the WHO for first-line
treatment
7. 3TC + d4T + nevirapine
3TC + d4T + efavirenz
3TC + AZT + nevirapine
3TC + AZT + efavirenz
8. – If the person is not ready or does not want to start treatment – delaying
treatment may give more time for them to become more psychologically prepared so
that they adhere to treatment better when they do start
- If the person has an opportunistic infection like TB where starting two different
treatments at the same time will increase side effects. With TB someone with a CD4
count <100 will delay ARVs for 1-2 weeks, and someone with a CD4 count 100-200 will
delay ARVs until after the first 2-months of TB treatment
- If they do not fulfil the guidelines recommended for starting treatment i.e. if their
CD4 count is still much higher than 200.
9. – How regularly a drug is taken and the time it is taken
- Speed of metabolism – how quickly an individual processes drugs – the are
wide ranges of individual differences in the drugs levels absorbed by different people.
Sometimes this can relate to body weight – i.e. larger people need a larger dose – but
more usually it is because of biological differences – i.e. different people have different
levels of the enzymes that the liver uses to process drugs.
- Diet – many drugs are absorbed more quickly or more slowly depending on
whether they are taken with food or on an empty stomach
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 4 June 2005
- Drug interaction (including some recreational drugs) – one drug can speed up
the metabolism of another drug (therefore reducing those levels) or can slow down the
metabolism (increasing the drug levels).
- Pre-existing liver damage (or kidney damage for some drugs) - ie someone with
liver damage is likely to process drugs much more slowly.
10. Adherence refers to taking the drugs exactly as they are prescribed-at the right time
and following any special diet restriction.
11. Six things that could help adherence include: (there are many others)
– Keeping a daily chart
- Using a pillbox
- Using a Pill beeper or alarm watch
- Having medications for the side effects
- Asking a friend to remind you
- Keep a small supply of drugs at an easy to reach place
12. Drug resistance refers to changes in the structure of an individuals HIV which means
that the drugs no longer work as well or even at all
13. Clinical failure refers to a when an HIV-positive person feels ill and gets symptoms (i.e.
other illnesses), which means that the drugs are not preventing him/her from getting ill.
14. Virological failure relates to the results of viral load blood tests – i.e. if viral load levels
never reach undetectable, or if they rebound and become detectable again.
15. The consensus from many studies seems to show that getting to <50 copies/mL stops
HIV from developing as a virus. After 5 years on treatment with a viral load <50 copies,
the virus will be the same as at the start of treatment. Viral load above 50 copies/mL
continues to evolve, and allows resistance to develop.
16. Please imagine that you are a counsellor and need to explain to your client what is
adherence, why adherence is important and how to improve adherence.
Section 4
1. Side effects are secondary effects of a drug other than the reason it is prescribed. Side
effects are also called adverse events or drug toxicity.
2. In some cases they are, but generally there is not a big difference. One of the most
important differences is with nevirapine and liver toxicity. Women should not start
treatment with nevirapine if their CD4 count is over 250, compared to men who should
not start if it their count is over 400.
3. Both of these options are possible but not without a discussion with the doctor. Quality
of life is very important and any drug that causes side effects can usually be changed
to an alternative that may be easier to tolerate.
4. Grade 1-mildest; grade 4-most serious.
5. Lipodystrophy has to do with the way the body processes fats and sugars. Symptoms
of lipodystrophy include lipoatrophy, fat accumulation and increased blood cholesterol
and triglycerides. Lipoatrophy is a state where the person has a reduced subcutaneous
fat on the arm; legs or face.
6. Peripheral neuropathy refers to damage to the nerves in the hands or feet It starts in
the fingers and/or toes but can spread into the arms and legs (‘peripheral to the central
body), usually with tingling, numbness, or increased sensitivity.
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 5 June 2005
7. d4T, ddI and very rarely 3TC. Hydroxyurea increases the risk of neuropathy with ddrugs.
ddC is now discontinued by had a high incidence of neuropathy.
8. AZT is associated with anaemia,
9. Nevirapine, efavirenz are both associated with liver toxicity
10. Symptoms of liver toxicity include; Feeling sick (nausea) or being sick (vomiting), Poor
appetite, If your eyes or skin looks more yellow, Light coloured stool or dark coloured
urine, Tenderness or swelling in your liver - your liver is just below your stomach.
11. Nevirapine, efavirenz, abacavir, fosamprenavir and T-20 can all be associated with
severe rash
12. A severe rash s defined as if the rash covers more than 10% of the body or if it breaks
the skin. However you would show any rash to a doctor or health advisor as soon as
you notice it, if you have recently started a drug associated with this as a side effect.
13. Two examples of Grade 4 side effects are: Diarrhoea requiring hospitalisation, liver
toxicity with AST or ALT levels above 7.5 ULN. Any side effect that requires
hospitalisation is classified as Grade 4.
14. The risk of lactic acidosis increases when d4T is used with ddI. These two drugs
should not be used together by pregnant women as the risk increases even higher.
15. Efavirenz (Sustiva) causes mood changes and vivid dreams in at least 50% people
when they first start treatment.
Section 5
1. Protozoa are tiny parasites. Giardia, cryptosporidia, and microsporidia.
2. A CD4 count fewer than 300 cellls/mm3 increases the risk of gastric infections.
3. - Drink bottled water sourced from underground sources
- Wash vegetables and salads thoroughly
- Cook meet thoroughly
4. Candida (thrush) is a fungal yeast infection that commonly affects the mouth and
throat, gullet, sinuses, genital organs, and much more rarely the brain.
5. Symptoms of candida include white or red patches (especially in the mouth),
sometimes cracks at the corners of the mouth, headaches and possible vomiting,
difficulty eating, and tast changes.
6. - Ketoconazole
- Itraconazole
- Fluconazole
7. PCP stands for Pneumocystis Carinii Pneumonia
8. Risk for PCP increases when CD4 counts is below 200 cells/mm3
9. Prophylaxis treatment against PCP includes co-trimoxazole or dapsone or aerosolised
pentamidine, etc.
10. First line PCP treatment is co-trimoxazole by continuous drip or injection for 3-4 days
and then switch to tablets.
11. Alternative PCP treatments include trimethoprim plus dapsone, pentamidine,
trimetrexate, atovaquone and clindamycin plus primaquine.
12. TB stands for Tuberculosis – it is a microbacterial infection that commonly affects the
lungs but can also affect many other organs
13. A person with active TB is infectious, while a person with inactive TB is not.
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 6 June 2005
14. First line TB treatment is a 2-month course of a combination of four antibiotics (I.e.
isoniazid, rifampicin, pyrazinamide and ethambutol), followed by a 4-month course of a
combination of 2 antibiotics (i.e. isoniazid and ethambutol)
15. Any PI or nevirapine.
16. TB prophylaxis is recommended for people who share the same confined living or
working place as someone with active TB.
17. Mycobacterium avium /Mycobacterium intracellulare-bacterial organisms closely
related to mycobacterium tuberculosis.
18. A combination of two or more antibiotics; usually clarithromycin or azithromycin plus
ethambutol.
19. Hepatitis is an infection that causes liver inflammation or damage.
20. Hepatitis C takes approximately 20-25 years to progress to in HIV-negative people but
progresses more quickly in people coinfected with HIV.
21. Drugs that are active against hepatitis B include adefovir, 3TC, tenofovir, FTC and
interferon-alpha. Drugs that are also active against HIV can only be used in a
combination with other HIV drugs. Please refer to current HBV treatment guidelines for
recommendations for treatment in HIV coinfected people, (i.e. www,bhiva.org)
22. When CD4 count drops below 50 cells/mm3 the risk of CMV retinitis increase to 30-
40% over 3 years.
23. Active CMV retinitis is diagnosed by eye examination, and anyone with a CD4 count
below 50 whether on or off treatment should have monthly eye checks. CMV while in
other organs is usually by biopsy sample. Viral load tests for CMV are generally only
used in research.
24. Toxoplasmosis is transmitted by eating raw or undercooked meat. Exposure to cat
faeces that is over 1 day old also is infectious and is a source of toxoplasmosis.
25. Toxoplasmosis treatment has to continue until CD4 count rises above 200.
26. Main AIDS-defining cancers include NHL (Non-Hodgkin Lymphoma), KS (Kaposi’s
Sarcoma) and cervical cancer.
27. It depends on the cancer. Some improve dramatically and go into remission (ie KS) but
others do not dramatically improve.
28. Liver cancer is associated with hepatitis C.
29. AIDS wasting is symptom of different diseases including HIV infection and OIs that
results in weight loss, principally loss of lean muscle mass.
Section 6
1. Without treatment for either the mother or baby, about 25% babies would be born HIVpositive
2. The mothers viral load at delivery is the most predictive of whether the baby with be
born HIV-positive. The lower the viral load, the lower the risk, and risk becomes less
than 1% when viral load is undetectable.
3. No, the fathers HIV status does not directly affect the status of the baby. An HIVnegative
mother cannot have an HIV-positive baby.
4. Pregnancy may cause a drop in a woman’s CD4 count. This is usually about 50
cells/mm3 but it can vary a lot.
5. There is a risk of resistance from using AZT monotherapy (that is not very high), and
the mother might be strongly advised to have a C-section as a mode of delivery.
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 7 June 2005
6. Less than 1% babies are born HIV-positive in mothers that use combination ARV
therapy with three or more ARVs.
7. A short course of triple combination therapy after the second trimester at 24 to 28
weeks is recommended for mothers who do not need ARV treatment for their own
health
8. Cons for C-section include:
- More probable complications like infections
- Having a natural birth after a C-section is more complicated and difficult
- Babies delivered by C-section are more likely to receive ventilatory support
Pros for C-section include:
- Reduced risk of HIV transmission when the pregnant woman receives only AZT
9. ARV drugs not recommended in pregnancy are efavirenz-generally in pregnancy and
the caution is strongest during the first trimester (12 weeks); nevirapine is not
recommended for women with a high CD4 count (above 250) because of risk of liver
toxicity; ‘ d‘ drugs together as they can cause fatal side effect in pregnant women
10. ARV drunks can contribute to morning sickness, nausea, anaemia, diabetes, lactic
acidosis.
11. A HIV positive woman who is pregnant should avoid amniocentesis, chorionicvillus
sampling, foetal scalp sampling, cordocentis, percutaneous umbilical cord sampling,
and internal foetal labour monitoring.
12. Acyclovir prophylaxis during labour will reduce the risk of transmitting herpes to the
baby.
13. The day the baby is born, one month after that and three months after that, using HIV
PCR DNA test.
14. HIV-positive mothers should not breastfeed. The risk of transmitting HIV from motherto-
baby can be as high as 28%.
15. The baby should take ARV prophylaxis for four to six weeks after birth.
16. After the birth, the mother has to be especially careful of her own adherence and
health.
Section 7
1. IDUs were frequently excluded form ARV treatment due to the wrong but widespread
belief that they are less likely to be adherent to treatment and less likely to have a good
response to treatment.
2. Excluding IDUs form treatment is not based on scientific evidence. Several studies
showed that drug users could achieve high levels of adherence and benefit from
treatment just like any other group of people with HIV.
3. Access to treatment, access to substitution therapy, OI prophylaxis and treatment,
accessible, non-judgemental healthcare team, needle exchange, adherence support
and counselling, strong link with community based programmes, food programmes and
public transport, outreach strategies.
4. Yes. 2 to 3 fold increase in ecstasy levels because of an interaction with ritonavir.
5. Yes. About 50% decrease in blood levels of heroin because of an interaction with
ritonavir.
Treatment training for advocates: Answers to questions in Sections 1-7 www.i-Base.org.uk
HIV i-Base 8 June 2005
6. Yes. People using methadone and efavirenz will have a reduced dose of methadone
(of up to 60 % in blood concentration) and may need to increase the dose of their
methadone.
7. Yes. AZT concentrations are increased by approximately 2-fold.
8. A dose reduction of 50% of the drug is recommended when used with methadone.
9. Those symptoms that develop within 2-3 days are more likely to be a result of ARV
toxicity, and those that develop after 6 days are more likely to be associated with drug
withdrawal.

Sunday, October 28, 2007

POT SMOKIN HELPS EASE PAIN-STUDY FINDS

Smoked Cannabis Proven Effective In Treating Neuropathic Pain
ScienceDaily (Oct. 25, 2007) — Smoked cannabis eased pain induced in healthy volunteers, according to a study by researchers at the University of California, San Diego (UCSD) Center for Medical Cannabis Research (CMCR.) However, the researchers found that less may be more.


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See also:
Health & Medicine
Pain Control
Controlled Substances
Fibromyalgia
Mind & Brain
Marijuana
Brain Injury
Illegal Drugs
Reference
Analgesic
Narcotic
Tension headache
Back pain
In the placebo controlled study of 15 subjects, a low dose of cannabis showed no effect, a medium dose provided moderate pain relief, and a high dose increased the pain response. The results suggest a "therapeutic window" for cannabis analgesia, according to lead researcher Mark Wallace, M.D., professor of anesthesiology at UCSD School of Medicine and Program Director for the UCSD Center for Pain Medicine.

The study used capsaicin, an alkaloid derived from hot chili peppers that is an irritant to the skin, to mimic the type of neuropathic pain experienced by patients with HIV/AIDS, diabetes or shingles -- brief, intense pain following by a longer-lasting secondary pain. The subjects were healthy volunteers who inhaled either medical cannabis or a placebo after pain was induced. The marijuana cigarettes were formulated under NIH supervision to contain either zero, two, four or eight percent delta-9-tetrahydrocannabinol (THC.)

"Subjects reported a decrease in pain at the medium dose, and there was also a significant correlation between plasma levels of THC, the active ingredient in cannabis, and decreased pain," said Igor Grant, M.D., F.R.C.P.(C), professor and Executive Vice-Chair of the Department of Psychiatry, the director of the CMCR. "Interestingly, the analgesic effect wasn't immediate; it took about 45 minutes for the cannabis to have an impact on the pain," he said.

The results, showing a medium-dose (4% THC by weight) of cannabis to be an effective analgesic, converged with results from the CMCR's first published study, a paper by UCSF researcher Donald Abrams, M.D. published in the journal Neurology in February 2007. In that randomized placebo-controlled trial, patients smoking the same dose of cannabis experienced a 34% reduction in HIV-associated sensory neuropathy pain--twice the rate experienced by patients receiving a placebo.

"This study helps to build a case that cannabis does have therapeutic value at a medium-dose level," said Grant. "It also suggests that higher doses aren't necessarily better in certain situations -- something also observed with other medications, such as antidepressants."

The researchers stated that more and larger studies need to be conducted to measure the efficacy of cannabis, noting that medical marijuana could play an important role in treating patients who don't respond well to the usual pain relievers or can't tolerate drugs such as ibuprofen or opioids used for severe pain.

"The results of this study might help guide others doing clinical research into pain management," said Wallace

Sunday, October 21, 2007

JACK SAYS LEGALIZE POT,I SAY I AM VOTING NDP!!






Dear James, Thank you for writing. I appreciate your thoughtful comments. The federal NDP has long advocated for the decriminalization ofmarijuana. We are the only national party that actually has a resolutionand a policy for decriminalization. And, in advocating that position, weunderstand that we need a drug policy that does not rely primarily onour legal system. This policy must be part of a broader drug strategythat focuses on a health based approach, as recommended by a 2002Special Committee on the Non-Medical Use of Drugs on which NDP MP LibbyDavies played an important role. We want Canada to take steps that reflect a more intelligent andcompassionate direction on marijuana use. Not only have our courts ruleddifferently on medical marijuana and our government respondedaccordingly but also there is a growing chorus of established opinionfor a different approach to the possession of marijuana for personaluse. Decriminalization, we believe, is a first step, but it is not the onlystep. It is a first step to what needs to be an open debate about thefailure of the current practices and the need to focus on the realissues such as: avoiding needless criminalization of citizens; andworking with youth on health and social effects - particularly impaireddriving. Once again, James, thank you for contacting me this matter. Sincerely, Jack Layton MP (Toronto-Danforth)Leader, New Democratic Party of Canada

Friday, October 19, 2007

LEADERSHIP TRAINING PROGRAM HUGE SUCCESS!!OAN HAS MATURED!






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Ok so now i am back from the LEADERSHIP TRAINING PROGRAM put on by the Ontario Aids Network-huge success as 100 persons have already graduated to level 2 & many more to join & many more to insprire.THESE 2 GUYS HAVE GONE ON TO INSPIRE SO MANY GOOD PERSONS,ALL SPECIAL IN THEIR OWN RIGHT,EACH WITH A COMPELLING STORY,EACH WITH DIFFERING BACKGROUNDS & CULTURES.THESE TOW GUYS HAVE TRAINED 100 & STILL GOING STRONG.I HOPE TO GO ONTO LEVEL 3 AS SOON AS POSSABLE TO ENHANCE MY SPEAKING SKILLS.UPON RETURNING I JOINED 2 DIFFERENT GROUPS,ONE SPIRITUAL,& TOASTMASTERS INTERNATIONIAL.I am not sure i can afford the 190.00 that it costs for a year long membership.Guess we'll have to see wat santa says huh folks?Well my talk at CTS for future ambulence drivers went well as thyey asked me back for another class.iTS COOL HOW EACH PERSON I MET HAS SOMEKIND OF GOAL,DREAM,IDEA,OR THINKS OF A WAY TO IMPROVE SERVICES OR TO CREATE MORE SERVICES TO HELP THOSE IN NEED.I CAN REMEMBER MANY YEARS AGO PATIENTS WERE WORRIED ABOUT WASTING-NOW ITS BEING OVERWHEIGHT!!GO FIGURE EH FOLKS!I MEAN WE HAVE GONE FROM SKINNY TO OVERWHEIGHT .mY HEP-C IS CURED & I THANK JEHOVA GOD & HIS SON JESUS CHRIST!!!MY FAITH IN THEM IS NOT MISPLACED !!FOR THY ROD & THEY STAFF COMFORT ME.& THE WORDS SPOKEN SO LONG AGO BY A DYEING MAN ON THE CROSS=FORGIVE THEM FATHER-FOR THEY KNOW NOT WHAT THEY DO-BUSH & HARPER ARE SO TIED TOGETHER NOW HARPER IS TRYING TO INTRODUCE & ADOPT THE FAILED US POLICY!!I THOUGHT CANADA WAS A MORE FREE & DEMOCRATIC,WITH SOCIAL PROGRAMS FACING CUTS FROM THE HARPER GOV.I AM DEF NOT VOTING PC THIS YEAR.IT WILL BE GREEN OR NDP!!I REALLY HOPE NDP COMES OUT WITH A BILL TO TRY & LEGALIZE IT FOR SICK & DYEING PEOPLES.THE CAN AIDS FOUNDATION HAS BEEN TRYING TO GET IT LEGALIZED FOR THE LAST 10 YEARS WITH NO LUCK STILL.THE USA IS CONTROLLING CANADA & I THINK IT SUCKS AS I THOUGHT WE WERE AN INDEPENDENT COUNTRY,WITH OUR OWN GOALS & HOPES!SOMEONE SHOULD SUE THE USA OVER ALL THE POLLUTION THEY ARE DOING.I MEAN HUGE MOUNTAINS OF TIRES & LETHAL GAS,BOMBS,& LORD KNOWS WHAT OTHER DEADLY CHEMICALS THEY ADDED TO THE OCEANS WATERS.WELL I AM GLAD I AM CURED & THANKS BE TO JEHOVA & HIS SON JESUS CHRIST!AMEN!~HALELUYA!!CHRIST WAS BORN,CHRIST HAS DIED,& ROSE UP ON THE 3 DAY TO BE SEATED AT THE RIGHT HAND OF GOD,AND HE WILL BE COMEING AGAIN,BUT I THINK HE WILL BE DIFFERENT & I PRAY I GIVE MY LIFE THAT ANOTHER MIGHT LIVE.ITS THE ONLY WAY I CAN SEEK REDEMPTION FOR THE LIFE I TOOK .I HAVE TO STRIVE TO DO BETTER & NOT TO BE SO LAZY.iTS JUST THAT I HAVE NO ENERGY THESE DAYS.LIVE N LEARN EH FOLKS!~PEACE NOT WARS!

Sunday, September 30, 2007

Cool Pics & HIV Logos


SAFE SEX SAVES LIVES SO SAVE A LIFE TODAY!THE LIFE YOU SAVE COULD BE YOUR OWN IF YOUR SMART & USE A CONDOM~!PEACE N LOVE NOT WARS N WALLS EH FOLKS~~!!!!

Monday, September 17, 2007

Just fer today,Thanks to GOD fer all!







Note created September 17, 2007
So,its monday night & i have to try to get some sleep early as i have to be up at 8:am,Mornings are hard on me.Just feel so shitty in the mornings.Well at least i will know if i am to start meds or wat.was nice out today with the temp hitting 21c & tomorrow is going to be even warmer!!Well folks,have a good night eh!!!!Well am back ,as i cant sleep.Well it seems that each day we learn of new meds breakthroughs in drugs or treatment & other areas as well.We must keep up this war,& it is a war!!!Peace n love NOT Wars n Walls eh folks!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!

Sunday, September 9, 2007





SO LIVING IN SUDBURY ISNT ALL BAD,ALTHOUGH winters can be harsh,that might change with global warming i think,but ya if anyone needs to be inspired,go to TLC channel & watch the many educational & diocumentrys & all round good stuff to expand yer minds.It always makes me feel alittle better & i find myself in better moods not watching so much violence on TV,as i think too much will just numb your mind to it.So ,live & learn,laugh & love!Peace nlove not wars n walls eh folks~~~!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!!