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Medicine United States

FDA Approves CRISPR-Based Medicine For Treatment of Sickle Cell Disease (statnews.com) 43

An anonymous reader quotes a report from STAT: The Food and Drug Administration on Friday approved the world's first medicine based on CRISPR gene-editing technology, a groundbreaking treatment for sickle cell disease that delivers a potential cure for people born with the chronic and life-shortening blood disorder. The new medicine, called Casgevy, is made by Vertex Pharmaceuticals and CRISPR Therapeutics. Its authorization is a scientific triumph for the technology that can efficiently and precisely repair DNA mutations -- ushering in a new era of genetic medicines for inherited diseases.

In a clinical trial, Casgevy was shown to eliminate recurrent episodes of debilitating pain caused by sickle cell, which afflicts approximately 100,000 people in the U.S., a vast majority of whom are Black. The therapy, whose scientific name is exa-cel, is described as a potential cure because the genetic fix enabled by CRISPR is designed to last a lifetime, although confirmation will require years of follow-up. The FDA decision comes three weeks after regulators in the U.K. were the first to clear the drug. Approval in the European Union is expected next year. The FDA is also expected to rule on exa-cel as a treatment for beta thalassemia, another inherited blood disorder, by March 30.

The FDA on Friday also approved another sickle cell treatment, a gene therapy from Bluebird Bio called Lyfgenia. Patients will now have the option of two cutting-edge therapies that provide potentially curative benefits. Scientists Emmanuelle Charpentier and Jennifer Doudna published their first CRISPR paper just over a decade ago. In 2020, the research won the pair a Nobel Prize. Reflecting on the approval of Casgevy, Charpentier told STAT via email that she was "excited and pleased" for what it means for patients and their families.

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FDA Approves CRISPR-Based Medicine For Treatment of Sickle Cell Disease

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  • by Baron_Yam ( 643147 ) on Saturday December 09, 2023 @12:58AM (#64067927)

    Wait until we have enough confidence to edit the germline so your kids can't get it.

    • Wait until we have enough confidence to edit the germline so your kids can't get it.

      Sickle cell disease is not normally directly inherited.

      It is a recessive gene. The disease only manifests if both copies carry the trait.

      About 8% of African Americans have a single copy, and 0.2% have two copies.

      So if an African American with the disease mates with another African American, there is a 4% chance a child will have the disease.

      • Umm... That's 1/20 black kids with sickle cell. I suspect you made an error multiplying 0.08 * 0.08, which should have come out to 0.0064 or 0.64% and not 4%

        Which would still seem to indicate a LOT of people are getting tested or checking family history prior to having kids (and good on them for being so responsible!), because that's 1/3 the rate you'd expect based on random pairings.

        Unless I've ALSO made a math error somewhere, which I am prone to do.

        • Umm... That's 1/20 black kids with sickle cell.

          No. It is 1/20 of kids of ONE PARENT WHO HAS THE DISEASE, not of the general black population.

          multiplying 0.08 * 0.08, which should have come out to 0.0064 or 0.64%

          Nope. The rate for the general AA population is 0.08*0.08/4 = 0.0016 or 0.16%.

          You need to divide by four because only a quarter of such pairings result in two copies of the bad gene.

        • I wasn't aware black people only mate with black people.

          • Re:Baby steps (Score:4, Informative)

            by ShanghaiBill ( 739463 ) on Saturday December 09, 2023 @08:57AM (#64068367)

            I wasn't aware black people only mate with black people.

            They mostly do.

            95% of black women mate with black men.

            90% of black men mate with black women.

            That is a higher rate of endogamy than other minorities such as Asian-Americans and Hispanics.

            • by mattkime ( 8466 )

              How many black women mate with black women?

              How many black men mate with black men?

              • How many black women mate with black women?

                How many black men mate with black men?

                We are talking about passing genes, which means children.

                Men mating with men rarely results in offspring.

      • Um...that is the very definition of "directly inherited". It literally is inherited from the parents, either by receiving the single recessive gene that both parents carry (e.g. Ss + Ss = ss) or from a carrier parent + expressed parent (e.g. Ss + ss = ss) or even two expressers (e.g. ss + ss = ss). Yes, I have seen parents who both had the disease have children and yes they did so knowing their child would 100% inherit the disease.

    • If you'd read anything about the therapy, you'd realize it involves removing stem cells from the patients' bone marrow, editing the genes in them, then transplanting them back into the patient.

      At no point do they remove a patient's testicles/ovaries and edit the genes there.

      It is literally impossible for this treatment to be passed on to a child.

      • If you'd ready anything about my post, you'd realize it involves talking about the future.

        At no point does it suggested the current treatment is heritable.

        It is literally impossible to interpret the post otherwise.

  • It is a brave new world. How long until we will need to patch our DNA with a Signed and Secure DNA Bootloader?

    • There's no point. The human dna boot sequence occurs only once per unit, often in an unscheduled and haphazard manner such as in a back seat or club bathroom after heavy alcohol or other substance consumption.

      • There's no point. The human dna boot sequence occurs only once per unit, often in an unscheduled and haphazard manner such as in a back seat or club bathroom after heavy alcohol or other substance consumption.

        And usually with unknown random accompanying birth defects added at not charge.

  • by paugq ( 443696 ) <pgquiles@@@elpauer...org> on Saturday December 09, 2023 @10:47AM (#64068519) Homepage
    CRISPR was originally discovered by Spanish scientist Francis Mojica. He is the Rosalind Franklin of CRISPR: he was excluded from the Nobel Price that Charpentier and Doudna won, and most papers don't name him. What a shame.

    https://en.wikipedia.org/wiki/Francisco_Mojica
    • He didn't discover its DNA editing properties nor was he first to spot the existence of CRISPR sequences.

  • Go ahead and mark this troll, but I gotta say it...

    We gonna try it on black people first?

    I hope it's just a low-hanging fruit, good test case for CRISPR and not that.

    • You aren't wrong but I literally just had to sit through a training on this subject. Yes, it is potentially highly problematic to pick your trial subjects from a pool which is, statistically, economically and socially disadvantaged compared to the researchers. However, it is still considered potentially ethical if there is a high benefit and if the research requires involvement of the vulnerable group. Yes, appropriate safeguards and considerations must be made.

      But you're in a Catch-22 if you can't perform

Make sure your code does nothing gracefully.

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