Health Rounds: Experimental Bayer drug eases menopause-like symptoms from breast cancer therapy

July 9 (Reuters) - (This is an excerpt of the Health Rounds newsletter, where we present latest medical studies on Tuesdays and Thursdays. To receive the full newsletter in your inbox for free sign up here.)

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The participants in the trial – similar to two-thirds of breast cancer patients overall - had tumors that use the hormones estrogen and progesterone to grow.

The goal of so-called endocrine therapy is to block those hormones, which reproduces the uncomfortable menopause symptoms. The most effective way to relieve these symptoms in healthy women is to replace the hormones, which is not feasible when tumors use the hormones to grow.

In a year-long trial involving 474 breast cancer patients experiencing daily hot flashes due to hormone-suppressing therapy, 316 received Bayer’s elinzanetant and 158 received a placebo.

The Bayer drug also significantly improved sleep quality and menopausal quality of life by week 12.

“It is important to treat vasomotor symptoms because they can negatively impact quality of life and lead to women prematurely stopping their breast cancer treatment,” said study leader Dr. Fatima Cardoso of the Champalimaud Clinical Center in Lisbon.

Elinzanetant belongs to a new class of drugs called neurokinin receptor antagonists that target the neurobiological mechanisms in the brain involved in hot flashes and night sweats.

In one large study of breast cancer survivors, half the participants reported non-adherence to endocrine therapy, the editorial says.

Bayer is awaiting approval of elinzanetant from the FDA and the European Medicines Agency.

AVAILABLE DRUGS CAN PREVENT IMMUNOTHERAPY-RELATED DIABETES

Cases of type 1 diabetes caused by cancer immunotherapy drugs can be controlled – and even reversed – by treatment with already approved medicines for autoimmune conditions like psoriasis and rheumatoid arthritis, laboratory studies suggest.

With the increased use of the blockbuster cancer drugs, “preventing long-term autoimmune damage is becoming a critical part of survivorship care,” study leader Dr. Melissa Lechner of the David Geffen School of Medicine at UCLA said in a statement.

“This is one of the first times we’ve found a way to intervene in these toxicities in a meaningful way,” she added.

Her team identified a new group of immune cells called CD4+ T follicular helper cells, or Tfh cells, which produce signaling molecules called IL-21 and IFN-gamma that fuel the immune attack on the pancreas.

In experiments in mice, the researchers found that a class of drugs known as JAK inhibitors, which block the IL-21 and IFN-gamma pathways, not only blocked the effects of the two signaling molecules but also reduced the number of Tfh cells and, in some cases, restored normal blood sugar levels.

“This is the first study to identify Tfh cells and the IL-21/IFN-gamma pathway as key drivers of checkpoint inhibitor–induced type 1 diabetes,” said Lechner.

“Importantly, we show that this pathway can be therapeutically targeted with a drug that is already FDA-approved and widely available without weakening the immune system’s ability to fight cancer.”

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Reporting by Nancy Lapid; editing by Bill Berkrot

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