sickle-cell

Things like sickle-cell and neurofibromatosis are worth studying only 2-3 generations back as well for example.

To take it further, what about conditions that specifically only address a minority of people, let's say that we made a drug that cures sickle-cell anemia, but gives a 100% chance of getting cancer by age 70.

This could obviously have far more important impacts as well: such an RV could reprogram cancerous cells to die off like proper cells, or disable their angiogenic capability; and of course it could be programmed to rewrite genes implicated in diseases like sickle-cell anemia or multiple sclerosis.

In the same way that certain non-psych heritable "diseases" confer some advantages and disadvantages (sickle-cell anemia and malaria, for instance).

There are countless people dying from sickle-cell anemia, and, if regulated as a "last resort" treatment it would be a true life saver.

About a hypothetical "drug that cures sickle-cell anemia, but gives a 100% chance of getting cancer by age 70": it should obviously be on the market.

In the same way that certain non-psych heritable "diseases" confer some advantages and disadvantages (sickle-cell anemia and malaria, for instance).

There are countless people dying from sickle-cell anemia, and, if regulated as a "last resort" treatment it would be a true life saver.

About a hypothetical "drug that cures sickle-cell anemia, but gives a 100% chance of getting cancer by age 70": it should obviously be on the market.