Human evolution: CRISPR cure for sickle cell (Introduction)

by David Turell , Tuesday, December 12, 2023, 20:18 (137 days ago) @ David Turell

In the USA:

https://www.sciencenews.org/article/first-crispr-therapy-sickle-cell-fda

"On December 8, the U.S. Food and Drug Administration approved the gene-editing therapy for use in patients age 12 years and older. In addition to offering hope of relief for people with severe forms of the painful blood disorder, the treatment, called Casgevy, is the world’s first to genetically tweak cells using the Nobel Prize–winning molecular scissors CRISPR/Cas9

"Another gene therapy for sickle cell disease, called Lyfgenia and developed by biotech company bluebird bio, based in Somerville, Mass., was also approved December 8.

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"Approximately 100,000 people in the United States, most of them Black or Latino, have sickle cell disease. It is caused by a genetic defect in hemoglobin, the oxygen-carrying protein in red blood cells. Unlike typical blood cells that are bendy enough to slip through blood vessels, sickled blood cells are inflexible and get stuck, restricting blood flow and causing debilitating pain (SN: 2/1/22). People with severe forms of the disease can be hospitalized multiple times a year.

"Having a new treatment option for sickle cell disease can give patients a “new lease on life,” says Kerry Morrone, a pediatric hematologist at Albert Einstein College of Medicine in New York City. People with the disease often miss school, work or special events due to excruciating pain. “The potential that this therapy could alleviate symptoms for patients is very exciting.”

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"Casgevy is like a transplant, but instead relies on a patient’s own cells. Using CRISPR, the treatment alters the genetic blueprint of bone marrow cells that give rise to blood cells. The edited cells make fetal hemoglobin, a type normally made by fetuses and young babies that doesn’t make red blood cells sickle and gum up vessels.

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"Casgevy is like a transplant, but instead relies on a patient’s own cells. Using CRISPR, the treatment alters the genetic blueprint of bone marrow cells that give rise to blood cells. The edited cells make fetal hemoglobin, a type normally made by fetuses and young babies that doesn’t make red blood cells sickle and gum up vessels.

"Patients first receive chemotherapy to wipe out existing bone marrow cells so the new ones, which are edited in a lab, have a chance to thrive in the body. After editing, the cells are given back to the patient through an IV. Both steps require hospitalization.

"In a clinical trial, 29 out of 30 patients given Casgevy and followed for at least 16 months didn’t have pain crises for at least a year, Vertex vice president of clinical development William Hobbs said at the FDA advisory committee meeting.

"The treatment isn’t without risks. Chemotherapy, for instance, can raise the risk of blood cancer and cause infertility. And in the short-term, chemotherapy kills immune cells, putting patients at higher risk dying from infections. (my bold)

"For some patients those risks may pale in comparison to the prospect of a year without immense pain, says Morrone, who is also director of the Sickle Cell Program at the Children’s Hospital at Montefiore. Others may want to wait and see what the outcomes are. “I think that’s fair, because it’s not without any risk.'”

Comment: note the bold showing it is risky to alter our immune system. Humans acting God-like with our God-given brains still aren't equal to God.