iRECIST is a set of rules used to describe how a cancer changes on imaging during immunotherapy.
Traditional imaging response rules (such as RECIST 1.1) were developed mainly around chemotherapy and some targeted therapies. With immunotherapy, tumors can sometimes appear to enlarge at first or new lesions can appear before the cancer later stabilizes or shrinks. This pattern is often described as pseudoprogression<\/em> (an apparent worsening on scans that may reflect immune cells entering the tumor and inflammation rather than true tumor growth). Although pseudoprogression is not common across all cancers, it is important enough to influence how responses are reported in immunotherapy studies.<\/p>\n\n\n\n iRECIST was created to address this measurement and reporting challenge. Its core purpose is to reduce misclassification of immunotherapy responses by distinguishing:<\/p>\n\n\n\n Key benefits of iRECIST include:<\/p>\n\n\n\n Importantly, iRECIST is a response assessment framework<\/em>, not a treatment. It does not diagnose cancer, choose therapy, or replace clinical judgment.<\/p>\n\n\n\n Oncology teams may use iRECIST in situations such as:<\/p>\n\n\n\n iRECIST is not always the most suitable framework. It may be less appropriate or not applicable in situations such as:<\/p>\n\n\n\n iRECIST does not have a \u201cmechanism of action\u201d in the way a drug does. Instead, it provides a clinical pathway for interpreting imaging changes over time<\/strong> in patients receiving immunotherapy.<\/p>\n\n\n\n At a high level, iRECIST works by:<\/p>\n\n\n\n Immunotherapy can activate immune cells to recognize and attack cancer. In some patients, that immune activity can cause:<\/p>\n\n\n\n Because of these possibilities, iRECIST introduces the concept of unconfirmed progression<\/strong>:<\/p>\n\n\n\n iRECIST itself does not have an onset or duration. The closest relevant property is timing of response assessment<\/strong>:<\/p>\n\n\n\n iRECIST is not a medical procedure performed on the body. It is a structured method for applying imaging measurements and response categories<\/strong> during immunotherapy follow-up. A general workflow often looks like this:<\/p>\n\n\n\n Evaluation\/exam<\/strong> Imaging\/biopsy\/labs<\/strong> Staging<\/strong> Treatment planning<\/strong> Intervention\/therapy<\/strong> Response assessment (iRECIST application)<\/strong> Follow-up\/survivorship<\/strong> iRECIST is one standardized framework, but it sits within a broader landscape of response criteria. Common \u201ctypes\u201d and variations you may hear about include:<\/p>\n\n\n\n RECIST 1.1 vs iRECIST<\/strong> Other immune-related response criteria (research context)<\/strong> Tumor- and organ-specific response frameworks<\/strong> Clinical trial vs routine clinical care use<\/strong> Pros:<\/p>\n\n\n\n Cons:<\/p>\n\n\n\n Because iRECIST is a response assessment framework, \u201caftercare\u201d is best understood as what influences ongoing monitoring and the durability of a response<\/strong> while a patient is being treated and followed.<\/p>\n\n\n\n In general, outcomes and how long a response lasts can be influenced by:<\/p>\n\n\n\n Follow-up plans are individualized. They typically integrate imaging findings (which may be described using iRECIST in trials) with symptoms, physical exam, and relevant lab tests.<\/p>\n\n\n\n iRECIST is one way to describe what is seen on scans during immunotherapy, but it is not the only approach. Common comparisons include:<\/p>\n\n\n\n iRECIST vs RECIST 1.1<\/strong> iRECIST vs clinical judgment alone<\/strong> iRECIST vs PET-based approaches (where applicable)<\/strong> iRECIST vs disease-specific criteria<\/strong> iRECIST in clinical trials vs standard care pathways<\/strong> Q: Is iRECIST a test or a treatment?<\/strong> Q: Does iRECIST mean my cancer is getting better or worse?<\/strong> Q: Will iRECIST response assessments be painful or require anesthesia?<\/strong> Q: Are there side effects or safety concerns related to iRECIST monitoring?<\/strong> Q: How long does iRECIST follow-up take?<\/strong> Q: What does \u201cpseudoprogression\u201d mean, and does iRECIST prove it?<\/strong> Q: Can iRECIST tell whether a new spot is cancer or inflammation?<\/strong> Q: Will iRECIST affect whether I can keep working or exercising?<\/strong> Q: Does iRECIST have cost implications?<\/strong> Q: Does iRECIST affect fertility or family planning?<\/strong> iRECIST is a set of rules used to describe how a cancer changes on imaging during immunotherapy. It stands for \u201cimmunotherapy Response Evaluation Criteria in Solid Tumors.\u201d It is most commonly used in clinical trials and research studies of immune checkpoint inhibitors. It helps clinicians report tumor response in a consistent, standardized way.<\/p>\n","protected":false},"author":9,"featured_media":0,"comment_status":"open","ping_status":"open","sticky":false,"template":"","format":"standard","meta":{"footnotes":""},"categories":[],"tags":[],"class_list":["post-2641","post","type-post","status-publish","format-standard","hentry"],"yoast_head":"\n\n
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Indications (When oncology clinicians use it)<\/h2>\n\n\n\n
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Contraindications \/ when it\u2019s NOT ideal<\/h2>\n\n\n\n
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How it works (Mechanism \/ physiology)<\/h2>\n\n\n\n
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Key tumor biology context (why immunotherapy can look different on scans)<\/h3>\n\n\n\n
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Onset, duration, and reversibility (closest relevant concepts)<\/h3>\n\n\n\n
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iRECIST Procedure overview (How it\u2019s applied)<\/h2>\n\n\n\n
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Types \/ variations<\/h2>\n\n\n\n
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Pros and cons<\/h2>\n\n\n\n
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Aftercare & longevity<\/h2>\n\n\n\n
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Alternatives \/ comparisons<\/h2>\n\n\n\n
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iRECIST Common questions (FAQ)<\/h2>\n\n\n\n