Groundbreaking skin cancer treatment gives hope to millions of patients

Professor Nikola Bowden in the lab at Hunter Medical Research Institute (Credit: Image courtesy of Hunter Medical Research Institute)

HMRI and University of Newcastle researchers have discovered that treating patients who have late-stage treatment resistant melanoma with a combination of two existing drugs significantly increases their survival times.

Led by Professor Nikola Bowden and Dr Andre van der Westhuizen from HMRI’s Drug Repurposing and Medicines Research program, the project’s findings have been published in the American Association for Cancer Research journal Cancer Research Communications.

The drug repurposing trial focused on patients with end stage melanoma whose cancers had become resistant to frontline immunotherapy treatment, a class of drugs known as Immune Checkpoint Inhibiters (ICB). ICBs interfere with a cancer cells’ ability to ‘hide’ from the body’s immune system allowing a patient’s own body to fight the cancer.

The team found that by treating patients with a combination of two already approved chemotherapy drugs, Azacitidine and Carboplatin, they were able to re-sensitize the cancer cells to ICB treatment.

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Professor Bowden said the study provided a potential new treatment for patients who, until now, had run out of options

“In this paper we have shown in a phase II study that treatment with Azacitidine and Carboplatin could be effective in priming for anti-immunotherapy (Avelumab) in patients with advanced ICB-resistant melanoma,” Professor Bowden said.

The team has been investigating these drugs since 2015 and, between 2017 and 2021, 20 patients, were given the two repurposed chemo drugs in order to ‘prime’ them for a subsequent immunotherapy treatment.

The patients survived an average of 47 weeks, with four of the patients still alive today following the treatment they received in the trial.

Tumor response, PFS, and OS. A, Spider plot of tumor burden change of target lesions in reference to the baseline tumor burden in 18 patients with measurable tumor burden. RECIST/iRECIST, biopsies, and translational bloods were collected at week 9 after azacitidine/carboplatin and week 22 after six cycles of avelumab (indicated by dashed lines). B, Waterfall plot of the tumor burden change of target lesions at best response (%) in reference to the baseline tumor burden in 18 patients with measurable tumor burden. Dashed lines at +20% and −30% represent the threshold used for progression (PD) and PR. C, PFS in weeks. The median PFS from start of treatment was 18.0 weeks (95% CI: 14.87–21.13 weeks). D, OS in weeks. The median OS was 47.86 weeks (95% CI: 9.67–86.06 weeks). Credit: Cancer Research Communications (2022). DOI: 10.1158/2767-9764.CRC-22-0128

“For some of the patients, it was like the tumors were frozen in time and they stayed the same for a very long time. Some patients even experienced a reduction in tumor size and number,” Professor Bowden said.

The drug repurposing trial was combined with a new form of immunotherapy.

Professor Nikola Bowden in the lab at Hunter Medical Research Institute (Credit: Image courtesy of Hunter Medical Research Institute)

Professor Bowden explains: “Melanoma cells send out a signal to the immune system that says, ‘I’m meant to be here’. The chemo drug combination we used mobilize the immune system to attack the tumors while the immunotherapy blocks that signal.”

This trial was initially funded by the Hunter Melanoma Foundation and generous community donations, including a $20,000 donation from the late Valerie Ryan.

The second stage of clinical trials are underway using updated immunotherapy drugs.

“Initial results suggest that this group of patients are doing even better on the new drugs,” Professor Bowden said.

Melanoma signs and symptoms

According to the Mayo Clinic, melanoma can develop anywhere on your body, in otherwise normal skin or in an existing mole that becomes cancerous. Melanoma most often appears on the face or the trunk of affected men. In women, this type of cancer most often develops on the lower legs. In both men and women, melanoma can occur on skin that hasn’t been exposed to the sun.

Melanoma can affect people of any skin tone. In people with darker skin tones, melanoma tends to occur on the palms or soles, or under the fingernails or toenails.

Melanoma signs include:

  • A large brownish spot with darker speckles

  • A mole that changes in color, size or feel or that bleeds

  • A small lesion with an irregular border and portions that appear red, pink, white, blue or blue-black

  • A painful lesion that itches or burns

  • Dark lesions on your palms, soles, fingertips or toes, or on mucous membranes lining your mouth, nose, vagina or anus

Signs and symptoms of less common skin cancers

Other, less common types of skin cancer include:

  • Kaposi sarcoma. This rare form of skin cancer develops in the skin’s blood vessels and causes red or purple patches on the skin or mucous membranes.

  • Kaposi sarcoma mainly occurs in people with weakened immune systems, such as people with AIDS, and in people taking medications that suppress their natural immunity, such as people who’ve undergone organ transplants. Other people with an increased risk of Kaposi sarcoma include young men living in Africa or older men of Italian or Eastern European Jewish heritage.

  • Merkel cell carcinoma. Merkel cell carcinoma causes firm, shiny nodules that occur on or just beneath the skin and in hair follicles. Merkel cell carcinoma is most often found on the head, neck and trunk.

  • Sebaceous gland carcinoma. This uncommon and aggressive cancer originates in the oil glands in the skin. Sebaceous gland carcinomas — which usually appear as hard, painless nodules — can develop anywhere, but most occur on the eyelid, where they’re frequently mistaken for other eyelid problems.

For more science news stories check out our New Discoveries section at The Brighter Side of News.

Note: Materials provided above by Hunter Medical Research Institute. Content may be edited for style and length.

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