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Breakthrough in HIV Cure Research: Single-Mutation Stem Cell Transplant Leads to Long-Term Remission


Kernekoncepter
A patient has achieved long-term HIV remission after receiving a stem cell transplant from a donor with a single CCR5 delta 32 mutation, expanding the potential donor pool for HIV cure efforts.
Resumé

The content discusses a breakthrough in HIV cure research, where a patient has achieved long-term HIV remission after receiving a stem cell transplant from a donor with a single CCR5 delta 32 mutation. This is significant because previous HIV cure cases have involved donors with two copies of the CCR5 delta 32 mutation, which are harder to find.

The anonymous patient, referred to as the "next Berlin patient," is the first to achieve long-term HIV remission (approaching 6 years) after receiving a CCR5 wild-type, delta 32 transplant, known as a heterozygous transplant, for acute myeloid leukemia. Other cured patients have received stem cell transplants from donors with two copies of the CCR5 delta 32 mutation, known as homozygous.

Researchers are hopeful that this case will expand the pool of potential donors and the availability of allogeneic stem cell transplantation for HIV cure efforts. The key mechanism in a cure is the depletion of the HIV reservoir, and this case suggests that HIV remission and potential cure can be achieved independently of the CCR5 status.

The content also discusses the case of the "Geneva patient," who received a stem cell transplant from a wild-type CCR5 donor and experienced long-term HIV remission. Researchers emphasize the need for further research to understand the underlying mechanisms and translate the findings of these cases for HIV cure research globally.

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Statistik
The patient has achieved long-term HIV remission, approaching 6 years, after receiving a stem cell transplant from a donor with a single CCR5 delta 32 mutation. Four other patients have experienced long-term HIV remission after receiving stem cell transplants from donors with two copies of the CCR5 delta 32 mutation. The "Geneva patient" received a stem cell transplant from a wild-type CCR5 donor and experienced long-term HIV remission.
Citater
"When we don't find a donor with these delta 32 mutations — and it's hard to find them, especially in geographical regions outside western or northern countries where it's almost impossible to find a homozygous delta 32 donor — it may be beneficial to take a heterozygous donor. They're easier to find." "This case is giving us hope that there is still a cure and underlying mechanisms that we're currently not understanding."

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by Richard Mark... kl. www.medscape.com 07-29-2024

https://www.medscape.com/viewarticle/latest-hiv-cure-case-comes-twist-2024a1000dvr
Latest HIV Cure Case Comes With a Twist

Dybere Forespørgsler

What are the potential implications of this breakthrough for the broader HIV/AIDS community, particularly in regions with limited access to stem cell transplants?

The breakthrough in utilizing a donor with a single CCR5 delta 32 mutation for achieving long-term HIV remission has significant implications for the broader HIV/AIDS community, especially in regions with limited access to stem cell transplants. By expanding the donor pool to include individuals with single mutations, the availability of allogeneic stem cell transplantation could be increased. This means that individuals in regions where finding donors with double mutations is challenging, such as in non-western or non-northern countries, may have a better chance of accessing potentially curative treatments. The use of heterozygous donors could make the procedure more feasible and accessible to a larger population, potentially leading to more successful HIV cure cases in diverse geographic regions.

How might the findings from this case challenge or complement existing theories about the role of the CCR5 receptor in HIV cure research?

The findings from this case challenge existing theories about the role of the CCR5 receptor in HIV cure research by demonstrating that a single CCR5 delta 32 mutation in the donor can also lead to long-term HIV remission. Previous cases of HIV cure involved donors with double mutations, leading to the belief that homozygous mutations were necessary for successful outcomes. However, this case shows that heterozygous donors can also achieve similar results, challenging the notion that only homozygous mutations are effective. This finding complements existing theories by expanding the understanding of the potential impact of CCR5 mutations on HIV cure, suggesting that both single and double mutations can play a role in achieving remission and potentially a cure.

What other genetic or biological factors, beyond the CCR5 receptor, could be explored as potential targets for future HIV cure strategies?

In addition to the CCR5 receptor, other genetic or biological factors could be explored as potential targets for future HIV cure strategies. One promising area of research is the investigation of host genetic factors that influence HIV infection and disease progression. For example, genetic variations in genes encoding immune response proteins, such as HLA genes, could impact the ability to control HIV replication and influence the effectiveness of potential cure interventions. Furthermore, exploring the role of immune cell subsets, viral reservoirs, and epigenetic modifications in HIV persistence and latency could provide valuable insights into developing novel cure strategies. Additionally, targeting viral factors like viral entry mechanisms, replication processes, and immune evasion strategies could offer alternative approaches to achieving HIV remission and ultimately a cure. By broadening the scope of genetic and biological factors under investigation, researchers can uncover new avenues for developing innovative HIV cure therapies.
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