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Stem cell transplant has cured HIV infection in Berlin man 
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Stem cell transplant has cured HIV infection in 'Berlin patient', say doctors
NEW AND EXPERIMENTAL TREATMENTS
Keith Alcorn
Published: 13 December 2010

Doctors who carried out a stem cell transplant on an HIV-infected man with leukaemia in 2007 say they now believe the man to have been cured of HIV infection as a result of the treatment, which introduced stem cells which happened to be resistant to HIV infection.

The man received bone marrow from a donor who had natural resistance to HIV infection; this was due to a genetic profile which led to the CCR5 co-receptor being absent from his cells. The most common variety of HIV uses CCR5 as its ‘docking station’, attaching to it in order to enter and infect CD4 cells, and people with this mutation are almost completely protected against infection.

The case was first reported at the 2008 Conference on Retroviruses and Opportunistic Infections in Boston, and Berlin doctors subsequently published a detailed case history in the New England Journal of Medicine in February 2009.

They have now published a follow-up report in the journal Blood, arguing that based on the results of extensive tests, “It is reasonable to conclude that cure of HIV infection has been achieved in this patient.”

The case history

The 'Berlin patient' is an HIV-positive man who developed acute myeloid leukaemia, received successful treatment and subsequently experienced a relapse in 2007 that required a transplant of stem cells.

Doctors chose stem cells from an individual who had an unusual genetic profile: a mutation inherited from both parents that resulted in CD4 cells that lacked the CCR5 receptor. This mutation, called CCR5 delta 32 homozygosity, is present in less than 1% of Caucasians in northern and western Europe, and is associated with a reduced risk of becoming infected with HIV.

This is because all new infecting viruses need to use the CCR5 receptor on CD4 cells when infecting an immune system cell of the CD4 type.

Later in the course of HIV infection another type of virus emerges that can use the CXCR4 receptor instead.

Before the stem cell transplant the patient received chemotherapy treatment that destroyed most immune cells and total body irradiation, and also received immunosuppressive drugs to prevent rejection of the stem cells.

Antiretroviral therapy was halted on the day of the transplant, and the patient had to receive a second stem cell transplant 13 days after the first one, due to a further relapse of leukaemia.

The patient continued to receive immunosuppressive treatment to prevent rejection for 38 months, and at 5, 24 and 29 months post-transplant colon biopsies were taken to investigate possible graft-versus-host disease in the intestine. At each investigation additional samples were taken to check for signs of HIV infection in the abundant immune cells of the gut wall.

During the 38 month follow-up period the donor CD4 cells repopulated the mucosal immune system of the gut, to such an extent that the frequency of CD4 cells was almost twice as high as in HIV-negative healthy controls, and this phenomenon was also seen in a control group of ten HIV-negative individuals who received stem cell transfers.

The repopulation of CD4 cells was accompanied by the complete disappearance of host CD4 cells, and after two years the patient had the CD4 count of a healthy adult of the same age.

One of the challenges for any approach to curing HIV infection is long-lived immune system cells, which need to be cleared before a patient can be cured. In the case of the Berlin patient CCR5-bearing macrophages could not be detected after 38 months, suggesting that chemotherapy had destroyed these longer-lived cells, and that they had also been replaced by donor cells.

The German researchers and San Francisco-based immunologist Professor Jay Levy believe that the findings point to the importance of suppressing the production of CCR5-bearing cells, either through transplants or gene therapy.
The patient did not resume antiretroviral therapy after the transplant.

Nevertheless HIV remained undetectable by both viral load testing (RNA) and tests for viral DNA within cells, and HIV antibody levels declined to the point that the patient has no antibody reactivity to HIV core antibodies, and only very low levels of antibodies to the HIV envelope proteins.

Seventeen months after the transplant the patient developed a neurological condition, which required a brain biopsy and lumbar puncture to sample the cerebrospinal fluid for diagnostic purposes. HIV was also undetectable in the brain and the CSF.

An additional indication that HIV is not present lies in the fact that the patient’s CD4 cells are vulnerable to infection with virus that targets the CXCR4 receptor. If any virus with this preference was still present, the researchers argue, it would be able to swiftly infect the large population of memory CD4 cells that has emerged.

The Berlin patient speaks to the press

The `Berlin patient`, Timothy Ray Brown, a US citizen who lives in Berlin, was interviewed this week by German news magazine Stern.

His course of treatment for leukaemia was gruelling and lengthy. Brown suffered two relapses and underwent two stem cell transplants, as well as a serious neurological disorder that flared up when he seemed to be on the road to recovery.

The neurological problem led to temporary blindness and memory problems. Brown is still undergoing physiotherapy to help restore his coordination and gait, as well as speech therapy.

Friends have noticed a personality change too: he is much more blunt, possibly a disinhibition that is related to the neurological problems.

On being asked if it would have been better to live with HIV than to have beaten it in this way he says “Perhaps. Perhaps it would have been better, but I don’t ask those sorts of questions anymore.”

Timothy Brown is now considering a move from Berlin to Barcelona or San Francisco, and, reports Stern magazine, enjoying a drink and a cigarette.

Stern also interviewed Dr Gero Hütter, who was in charge of Timothy Brown’s treatment. Dr Hütter told Stern that as a scientist he was “in the right place, at the right time” and that “for me it is important to have overthrown the dogma that HIV can never be cured. Something like this is the greatest thing one can achieve in medical research”.

Implications for future approaches to curing HIV infection

If a cure has been achieved in this patient, it points the way towards attempts to develop a cure for HIV infection through genetically engineered stem cells.

The German researchers and San Francisco-based immunologist Professor Jay Levy believe that the findings point to the importance of suppressing the production of CCR5-bearing cells, either through transplants or gene therapy.

Scientists were sufficiently intrigued by the Berlin patient that they met in Berlin in 2009 to discuss how they could coordinate efforts to identify CCR5-delta32 homozygous donors and expand the supply of stem cells from these donors, for example through sampling blood cells from the umbilical cord of babies born to mothers who are homozygous for CCR5-delta32, in order to eventually facilitate stem-cell therapy.

Gene therapy techniques which can transform stem cells – and all their descendents – into cells resistant to HIV entry may be a more practical option than looking for matching donors.

Several US research groups announced in October 2009 that they had received funding to explore techniques for engineering and introducing CCR5-deficient stem cells.

If these approaches prove successful they will be expensive, so in the early stages it is likely that they would be reserved for people with no remaining treatment options or a cancer requiring bone marrow or stem cell transfer.

As Timothy Brown’s experience shows, curing HIV infection through ablative chemotherapy, immunosuppressive drugs and stem cell transfer is not a course of treatment for the faint-hearted. It has required courage, determination and a lot of support to become the first person to be pronounced `cured` of HIV infection.


http://www.aidsmap.com/page/1577949/

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Wed Dec 15, 2010 9:59 am
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Yay! Free and easy sexual intercourse is back on the menu, folks! They've found a cure for AIDS!

:roll:

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Wed Dec 15, 2010 10:29 am
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Just HIV, perhaps, if stem cell research is permitted to continue.
There's still lots of nasties out there, of course, which makes thoughtless sexual promiscuity a dangerous game. And perhaps a fond pipe dream.

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Wed Dec 15, 2010 10:36 am
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I know. I was pre-empting tomorrow's Daily Fail/Daily Excess/Sun/Star headlines.

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Wed Dec 15, 2010 10:38 am
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Let's hope this works.

And we need to keep the religious nutters from banning it.

:x

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Wed Dec 15, 2010 11:10 am
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rustybucket wrote:
Let's hope this works.
And we need to keep the religious nutters from banning it.
:x

The same religious nutters who think HIV/AIDS is a punishment from God on people who are 'deviants'? Good luck with that.

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Wed Dec 15, 2010 11:30 am
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ProfessorF wrote:
There's still lots of nasties out there, of course, which makes thoughtless sexual promiscuity a dangerous game.


Like waking up with an ugly chick you swore was fit 10 pints ago ;)

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Wed Dec 15, 2010 12:00 pm
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jonbwfc wrote:
rustybucket wrote:
Let's hope this works.
And we need to keep the religious nutters from banning it.
:x

The same religious nutters who think HIV/AIDS is a punishment from God on people who are 'deviants'? Good luck with that.

Jon

The same people who do not want stem cell research either.

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Wed Dec 15, 2010 12:11 pm
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Wasn't the last similar claim a result of the cured subject not actually having HIV in the first place? Poor testing or record keeping FTW!

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Wed Dec 15, 2010 4:14 pm
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Amnesia10 wrote:
jonbwfc wrote:
rustybucket wrote:
Let's hope this works.
And we need to keep the religious nutters from banning it.
:x

The same religious nutters who think HIV/AIDS is a punishment from God on people who are 'deviants'? Good luck with that.

Jon

The same people who do not want stem cell research either.


I wouldn’t worry. This will be an expensive treatment that only the rich can afford anyway.

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Wed Dec 15, 2010 4:26 pm
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paulzolo wrote:
I wouldn’t worry. This will be an expensive treatment that only the rich can afford anyway.

Only for a few years then once the costs have been solved then it could lead to an eradication of the disease. Hopefully.

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Wed Dec 15, 2010 4:46 pm
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Amnesia10 wrote:
paulzolo wrote:
I wouldn’t worry. This will be an expensive treatment that only the rich can afford anyway.

Only for a few years then once the costs have been solved then it could lead to an eradication of the disease. Hopefully.

Probably not is a smallpox kind of way. AIDS has a very long incubation period (it's the wrong term with a virus, but you understand what I mean). You can pass it on before you express symptoms and you won't get treated until you do express symptoms, unless you get lucky with a blood test for some other reason.
What it will mean is it'll end up being treatable, taking on the same level of seriousness as other life-threatening but not necessarily critical conditions, like say malaria or some of the run-of-the-mill cancers. Essentially it won't be 'scary' any more. However completely destroying your immune system followed by treatment of genetically modified stem cells is always going to be hard work, so I don't think we're quite back to the swinging 60s yet.

Jon


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Destroying the immune system to reboot it with a new one will mean that people will be vulnerable to diseases that they were immune to before.

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Wed Dec 15, 2010 10:26 pm
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nothing new here, apparently cancer is curable too as its nothing but a simple "fungus" or something but governments dont want to cure to make more money off people or something (apparently) :(

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brataccas wrote:
(apparently)


Hmmm....

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Thu Dec 16, 2010 12:37 am
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