3.4 Response evaluation

Response Evaluation Criteria in Solid Tumours (RECIST) are designed to provide a standardised and relatively simple method for assessing the treatment effect on tumours in protocolled studies. However, RECIST criteria are also used as a tool to evaluate the treatment efficacy in most oncology patients on standard treatment (chemotherapy, targeted therapy, immunotherapy, endocrine therapy). RECIST criteria were adopted in 2000 and revised in 2009. The current standard is RECIST 1.1.¹

The following terms/definitions are important in RECIST version 1.1

Measurable disease
Non-measurable disease
Target lesions
Non-target lesions

The above can be assessed using the following measurement methods

CT or MRI scan
Clinical
Chest X-ray

It is important that the same modality is used when evaluating the effect of a treatment.

Measurable disease – tumors and lymph nodes

Tumours – measured on longest diameter where minimum size is:

≥10 mm on CT or MRI scan
≥10 mm on clinical examination – visible/cutaneous/subcutaneous metastases
≥20 mm on chest x-ray

Lymph nodes – measured on the shortest link, where the minimum size is:

≥15 mm of lymph node – pathologically enlarged lymph node

Non-measurable disease – all other lesions and truly non-measurable lesions

Other lesions:

Small tumours/lesions <10 mm
10 mm < lymph nodes <15 mm

Non-measurable lesions:

Ascites, pleural and pericardial fluid, leptomeningeal disease, inflammatory breast cancer, lymphangitis carcinomatosis of the lungs and skin, abdominal masses or organomegaly, cystic lesions, sclerosing bone metastases

Target lesions

Based on the baseline examination (most often CT scan), measurable tumours/lymph nodes are defined and target lesions to be measured/compared from examination to examination are selected with regard to assessing the efficacy of the treatment. They must be:

Representative of all involved organs
Selected based on size and suitability for repeated measurements
In the case of several measurable lesions, select up to five representative lesions in total, but no more than two lesions per organ.

The diameter of each target lesion will be added to a number – baseline sum – which will be used later to measure response.

Non-target lesions

The remaining lesions, both non-measurable lesions and the remainder of measurable lesions, should be noted:

Measurable tumours that are not selected as target lesions
Too small tumours/lymph nodes
Non-measurable lesions (bone metastases, pleural effusion, ascites, peritoneal carcinoma, etc.)
Previously irradiated lesions

Response evaluation

When evaluating response, there may be 4 outcomes:

CR – complete response
PR– partial response
PD – progressive disease/progression
SD – stable disease

CR – complete response

Shrinkage of all target lesions and all pathologically enlarged lymph nodes is reduced to <10 mm in the shortest link
Loss of all non-target lesions
No appearance of new lesions

All of the above points must be met.

PR – partial response

At least 30% reduction in the total sum of target lesions vs. baseline sum
Not concurrent unequivocal progression of non-target lesions
No appearance of new lesions

All of the above points must be met.

PD – progressive disease/progression

At least 20% increase in the total sum of target lesions vs. where the sum was lowest (nadir sum) and an absolute increase of at least 5 mm from the nadir sum
New lesion
Unequivocal progression of non-target lesions
Clinical progression

Only one of the above points needs to be met in order to call it progressive disease.

SD – stable disease

Neither PR nor PD
No new lesions

The above options are shown here in a table to provide a better overview of the overall response in accordance with RECIST 1.1.

TARGET LESION	NON-TARGET LESION	NEW LESION	OVERALL RESPONSE
CR	CR	No	CR
CR	SD	No	PR
CR	Not evaluable (NE)	No	PR
PR	SD	No	PR
SD	SD	No	SD
PD	CR, PR, SD, PD, NE	Yes or no	PD
Not all evaluated	Not PD	No	Not evaluable (NE)
Any	PD	Yes or no	PD
Any	CR, PR, SD, PD, NE	Yes	PD

Example of assessment:

	BASELINE		FIRST RESPONSE EVALUATION	SECOND RESPONSE EVALUATION	THIRD RESPONSE EVALUATION
TARGET LESIONS	ORGAN	mm	mm	mm	mm
	Liver	47	28	31	45
	Lung	30	19	19	25
	Lymph node	25	16	17	24
Sum of target lesions		102	63	67	94
% change from baseline			-38.2%
Change in % from nadir				+6.3%	+49.2%
Response for target lesions			PR	PR	PD
Non-target lesions	Multiple liver metastases		Multiple liver metastases	Multiple liver metastases	Multiple liver metastases
Response for non-target lesions			SD	SD	Unequivocal progression
New lesions			no	no
Overall response			PR	PR	PD

iRECIST – RECIST for immune-based therapy

Immunotherapy uses the body’s own immune system to target the cancer (see the section on oncological treatment immunotherapy ). In clinical studies with immunotherapy, a different/unusual response was observed in relation to what had previously been seen with other oncology treatments. I.e. initial progression in accordance with RECIST 1.1 with increasing size of target lesions and appearance of new lesions, but subsequent positive and long-lasting response. Based on this, the RECIST working group decided to create a guideline with modified RECIST criteria for clinical studies with immunotherapy (iRECIST) to ensure uniform design and data collection².

iRECIST is based on RECIST 1.1, but more concepts have been added to the response evaluation:

iCR – Immune complete response
iPR – Immune partial response
iUPD – immune unconfirmed progressive disease
iCPD – Immune confirmed progressive disease
iSD – immune stable disease
New lesions are subcategorised to:
- Target lesions
- Non-target lesions

The main differences between RECIST 1.1 and iRECIST:

	RESIST 1.1	IRECIST
Definition of measurable and non-measurable disease; number and selection of target lesions	Measurable lesions are ≥10 mm in diameter (≥15 mm for lymph nodes); maximum five lesions (two per organ); all other disease is considered non-target (must be ≥10 mm on the short axis of disease in lymph nodes)	No change from RECIST 1.1; however, new lesions will be assessed based on RECIST 1.1 but recorded separately on the appropriate case report form (but not included in the sum of lesions for target lesions identified at baseline)
Complete response, partial response or stable disease	May not have met the criteria for progression prior to complete response, partial response, or stable disease	May have had iUPD (once or more times), but not iCPD before iCR, iPR, or iSD
Confirmation of complete response or partial response	Only required for non-randomised studies	Corresponding to RECIST 1.1
Confirmation of stable disease	Not required	Corresponding to RECIST 1.1
New lesions	Results in progression; recorded but not measured	Results in iUPD, but iCPD is achieved only if the next scan detects new lesions or the new lesions on the previous scan have increased in size (≥5 mm for the sum of new target lesions or increasing size of new non-target lesions, regardless of size growth
Independent blinded review and central assessment of scans	Recommended in some cases – e.g. in some trials with progression-based endpoints for marketing approval	Collection of all scans (but not an independent review) is recommended for all studies
Confirmation of progression	Not required (unless ambiguous)	Required
Assessment of general condition	Not included in the assessment	Unchanged general condition/PS is taken into consideration when deciding whether treatment should continue after iUPD

Further information on iRECIST and the management of new lesions and iUPD can be found in “iRECIST: guidelines for response criteria for use in trials testing immunotherapeutics”, Seymour et al. Lancet Oncol 2017².

References

Eisenhauer EA et al. New response evaluation criteria in solid tumours: Revised RECIST guideline (version 1.1). EJC 2019)
Seymour et al. iRECIST: guidelines for response criteria for use in trials testing immunotherapeutics, Lancet Oncol 2017.

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