Cancer
Researchers develop nasal therapeutic HPV vaccine

Researchers have created a therapeutic HPV vaccine delivered through the nose that could offer a non-invasive treatment for cervical cancer.
Screening for HPV and preventive vaccines lower risk, but there are no approved therapies for existing HPV infections or HPV-linked cancers.
Current treatments include surgery, radiotherapy and chemotherapy.
Researchers from Chiba University, Japan, led by associate professor Rika Nakahashi-Ouchida and Ms Hiromi Mori of Chiba University Hospital, have developed an intranasal therapeutic option.
Unlike injectable vaccines, nasal vaccines trigger immunity at the mucosal surface — the protective lining of the upper airway.
This mucosal response can also protect distant sites, including the reproductive tract.
Building on earlier work showing nasal immunisation can elicit strong genital-tract responses against herpes simplex virus type 2, the team used cationic nano-sized hydrogel particles (cCHP nanogels) to deliver HPV antigens to nasal tissues.
These positively charged spheres adhere to the negatively charged nasal surface and slowly release antigens, which prompt an immune response.
Nakahashi-Ouchida said: “We have developed an intranasal therapeutic vaccine as a non-surgical alternative to conventional treatments that can compromise women’s quality of life.
“This novel nasal vaccine activates the mucosal homing pathways of lymphocytes, allowing it to trigger an immune response in the cervical mucosa, a site from the nasal administration.”
The formulation targets the E7 oncoprotein from HPV16, which inactivates pRb, a key tumour suppressor.
To strengthen responses, the researchers added cyclic-di-AMP, an adjuvant that boosts T-cell-mediated immunity so T cells can attack infected or cancerous cells.
The resulting cCHP-E7 + c-di-AMP showed what the researchers describe as strong anti-tumour activity in mice and macaques. In mouse models, it significantly slowed tumour growth versus controls.
In macaques, a nasal spray device (usable in humans) delivered four doses.
Vaccinated animals developed high levels of E7-specific helper and killer T cells producing molecules linked to tumour control; controls did not.
Immune activity was detected in cervical tissue, and E7-specific killer T cells persisted for at least four months, suggesting lasting defence.
According to the World Health Organization, cervical cancer caused an estimated 660,000 new cases and 350,000 deaths in 2022.
If proven safe and effective in humans, intranasal therapy could offer a non-invasive, fertility-preserving alternative to surgery for some patients.
The cCHP nanogel platform may also support nasal vaccines against other pathogens and wider clinical uses.
Nakahashi-Ouchida said: “Immunotherapies such as intranasal therapeutic vaccines may help establish a new category of non-invasive treatment.
“These approaches could be extended to recurrence prevention and chronic disease management, offering patients safer and more accessible options.”
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