{"id":8286,"date":"2018-04-13T12:52:57","date_gmt":"2018-04-13T17:52:57","guid":{"rendered":"https:\/\/fomatmedical.com\/?p=8286"},"modified":"2026-05-06T10:20:49","modified_gmt":"2026-05-06T17:20:49","slug":"personalized-tumor-vaccine-clinical-trial","status":"publish","type":"post","link":"https:\/\/fomatmedical.com\/es\/blogs-updates\/personalized-tumor-vaccine-clinical-trial\/","title":{"rendered":"Una vacuna personalizada contra el tumor muestra resultados prometedores en un ensayo piloto"},"content":{"rendered":"

Personalized Tumor Vaccine Clinical Trial Shows Remarkable Promise<\/h3>\n

A groundbreaking personalized tumor vaccine clinical trial conducted at the Perelman School of Medicine at the University of Pennsylvania has yielded encouraging results in advanced ovarian cancer patients. Unlike conventional cancer vaccines, this approach uses each patient’s own immune cells to generate a broad, individualized anti-tumor response. According to the Mayo Clinic<\/a>, cancer immunotherapy works by helping the immune system recognize and attack cancer cells more effectively.<\/p>\n

What Makes This Vaccine Different<\/h3>\n

Most cancer vaccines developed to date target a single known molecule likely to appear on cancerous cells across patients with a given tumor type. The approach tested in this personalized tumor vaccine clinical trial is fundamentally different. Each vaccine is tailored to the individual patient using that patient’s own tumor, which carries a unique set of mutations and a unique immune profile. Rather than targeting one molecule, the vaccine is designed to stimulate an immune response against hundreds or thousands of tumor associated targets simultaneously.<\/p>\n

As lead author Janos L. Tanyi, MD, assistant professor of obstetrics and gynecology at Penn Medicine, explained: the goal is to mobilize an immune response that targets the tumor very broadly, hitting a variety of markers including some found only on that specific tumor.<\/p>\n

How the Personalized Tumor Vaccine Clinical Trial Was Conducted<\/h3>\n

The research team, led by Lana Kandalaft, PharmD, PhD, George Coukos, MD, PhD, and Alexandre Harari, PhD, of the Lausanne Branch of the Ludwig Institute for Cancer Research, developed a novel method for producing this type of vaccine. The process begins by isolating peripheral blood mononuclear cells from each patient and growing them in the laboratory into a large population of dendritic cells.<\/p>\n

Dendritic cells are essential drivers of T cell immunity. They ingest foreign material such as tumor cells and display pieces of that material to T cells and other immune components, triggering a targeted response. In this personalized tumor vaccine clinical trial, the dendritic cells were exposed to specially prepared extracts of each patient’s tumor, activated with interferon gamma, and then injected into the patient’s lymph nodes to prime a sustained T cell response.<\/p>\n

A total of 25 patients received doses of their individualized vaccine every three weeks, in some cases for more than six months.<\/p>\n

5 Key Results From the Pilot Study<\/h3>\n

Strong T Cell Responses in Half of Evaluable Patients<\/h4>\n

Approximately half of the patients who could be fully evaluated showed substantial increases in T cells specifically reactive to tumor material, indicating a meaningful immune response to the personalized tumor vaccine clinical trial protocol.<\/p>\n

Dramatic Survival Difference Between Responders and Non-Responders<\/h4>\n

The two year overall survival rate among responders was 100%. Among non-responders, that rate dropped to just 25%. This stark contrast suggests that the immune response generated by the vaccine may be a reliable predictor of long term outcomes.<\/p>\n

One Patient Remained Disease Free for Five Years<\/h4>\n

A 46 year old woman who entered the personalized tumor vaccine clinical trial with stage 4 ovarian cancer after five prior rounds of chemotherapy received 28 vaccine doses over two years. She then remained disease free for five additional years without further treatment.<\/p>\n

Evidence of Neoepitope Targeting<\/h4>\n

Tests on several responders identified vaccine induced T cells with high affinity for unique structures called neoepitopes on their tumors. An immune attack targeting neoepitopes is considered especially powerful because it is highly tumor specific and less likely to damage healthy cells.<\/p>\n

A Clear Path to Larger Trials<\/h4>\n

The study confirmed the vaccine’s safety and feasibility, providing a strong rationale for moving into larger Phase II and Phase III trials. Researchers also noted plans to enhance vaccine effectiveness by combining it with complementary drugs that target tumor immune defenses.<\/p>\n

Why This Research Matters<\/h3>\n

Tumors maintain a range of molecular defenses to suppress or evade immune attacks, which is why many cancer vaccines and immunotherapies have shown mixed results historically. This personalized tumor vaccine clinical trial represents a meaningful step forward by addressing each patient’s unique tumor biology rather than applying a one size fits all approach.<\/p>\n

The results, published in Science Translational Medicine, open a new chapter in cancer immunotherapy research, particularly for patients with advanced ovarian cancer who have exhausted standard treatment options.<\/p>\n

FOMAT conducts Phase I through Phase IV clinical research across a national network of investigator sites throughout the United States. To learn more about active oncology studies, visit our patient active studies page<\/a>.<\/p>\n","protected":false},"excerpt":{"rendered":"

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