Purpose of investigation
Clinical decision-making refers to the process of deciding how to select clinical decisions. This is important when considering whether to perform a test or not.
Purpose of investigation
When one orders a test (laboratory, imaging, or otherwise), it's important to have a predetermined purpose for the test and not just ordering tests willy-nilly. Tests are often invasive as well as time-consuming and expensive, and so they should be worth the risk, time, and expense. There is no point in ordering a test if the test result does not influence how you approach the patient.
Generally, investigations can be used for:
- Screening (healthy or not healthy)
- Lab diagnosis
- Follow-up/monitoring
- Monitoring progression/response to treatment
- Evaluation of prognosis
- Information regarding the likely outcome of the disease
Value to the patient
An investigation should have some form of value for the patient (except if done in a research setting or for epidemiological purpose, in which case the investigation has value for researchers, and in turn, future patients). The value to the patient should also weigh up for any negative consequences of the investigation.
Frail patients
Many frail patients, especially elderly, cannot or do not want to undergo certain tests or invasive procedures. Is there, for example, a point in evaluating a frail elderly person for cancer, if they do not want to or cannot undergo cancer treatment anyway? Take the following example:
A frail elderly patient living in an institution (like a nursing home) has a positive faecal occult blood test. The physician considers to refer them to colonoscopy, but stops to consider: how will a colonoscopy be of value to the patient? In their current state, even if the colonoscopy would show colorectal cancer, the patient would not be a candidate for any anticancer surgery or chemotherapy, so even if a diagnosis is made, nothing will change for the patient (except the stress of knowing they have cancer). In addition, colonoscopy is an invasive investigation which requires strict patient preparation, which can be difficult for a frail elderly to perform or even survive.
If they have colorectal cancer and it grows and eventually causes intestinal obstruction, colonoscopy may be indicated for stenting the bowel, in which case the colonoscopy would have value for the patient as palliative therapy
One can also argue that even performing a faecal occult blood test in this case has no value for the patient, because the next step after a positive test would be a colonoscopy, a procedure which would not be of value to the patient anyway
Patient management is the same regardless of test result
In some cases, it may be temping to order an investigation to gain more information, but it's important to consider whether that information is of value or not. Take the following example:
A young male has had back pain for a few days. The pain is not severe, and there are no red flags for cauda equina syndrome. He wants an MRI to know what's going on, but the physician stops to consider: how will an MRI be of value to the patient? The patient may or may not have a herniated disc, but even if they do, a herniated disk without red flags isn't an indication for surgery anyway. As such, whether the MRI shows a herniated disc or not, the management will be the same (no surgery, only physical therapy and pain relief), and the MRI is therefore of no value to the patient (and it is resource-intensive)
On the other hand, if the patient has debilitating pain or there are red flags present, he may have cauda equina syndrome, in which case surgery is indicated. In this case, MRI has value: it determines whether they need surgery or not
Another example:
A middle aged woman has symptoms of an upper respiratory tract infection. After taking the anamnesis and physical examination, you're certain that it's a viral infection. You reflexively want to order a CRP or leukocyte count, but you stop to consider: will the laboratory investigation likely be of value to the patient? You know that viral URTIs only cause mildly elevated inflammatory parametres, so that's likely what you'll find anyway. And even if the CRP is higher than you expect, you're certain enough that this is not a bacterial infection, so you won't be administering antibiotics anyway. So even after making the investigation, you'll most likely not be changing your management of this patient; managing their symptoms and encouraging rest, without antibiotics
On the other hand, if the patient has symptoms which make it difficult to distinguish between viral and bacterial infection clinically, a laboratory investingation is merited, as it provides additional information which can aid in the diagnosis and therefore the treatment in this case
Consider that many laboratories can analyse a pharyngeal swab for specific airway viruses. Would making such an investigation in this case change the management of the patient? In most cases no, as there is no specific treatment for most airway viruses anyway.
Screening
Screening refers to using an investigation to detect a disease which has not yet caused symptoms, so-called subclinical disease, with the aim of initiating management as early as possible, to improve the prognosis. Examples include:
- Regular mammography or cervical cytology in women
- Used to detect early or precursor breast cancer or precursor stages for cervical cancer, respectively
- Faecal occult blood test in middle-aged/elderly
- Used to detect early colorectal cancer or bleeding colon polyps
- Screening for inborn errors of metabolism and developmental dysplasia of the hip in newborns
- Non-invasive prenatal test (NIPT) for trisomies during pregnancy
Screening is indicated if the disorder has a high mortality or morbidity, and there is treatment available. Like most things in life, screening is only viable if it can be proven that the advantages weigh up for the disadvantages.
Screening tests
A screening test is most useful when it has high sensitivity. It would be great if a screening test also had high specificity, but there is often a trade-off between sensitivity and specificity. Therefore, most screening tests have low specificity. As a result, screening tests produce few false negatives but many false positives, and many more false positives than true positives.
Because many of those who have a positive screening test are false positives, positive screening test must always be confirmed by a more specific test.
Advantages of screening
Screening may have many advantages. The main advantage, and the intention behind screening, is that treatment can be started at an earlier time, before symptoms even appear, which usually improves the prognosis considerably, and may allow for curative treatment, which may not have been an option if the disorder was not diagnosed at the asymptomatic stage.
Most national screening programmes are backed up by evidence that they reduce mortality or morbidity. For example, breast cancer screening reduces risk of dying from breast cancer by approximately 20-30%.[1]
Disadvantages of screening
Unfortunately, screening has many disadvantages as well.
Low specificity of tests causing worry and more testing
Because screening tests necessarily have low specificity, there will be many false positives. Testing positive on a screening test, especially for cancer, leads to considerable worry for a person. Considering that most people who test positive on a screening test is false positive, the positive predictive value is low as well, meaning that the chance of having the disorder when testing positive is low. This concept is very difficult for laypeople to understand.
Because screening tests must be confirmed by a confirmatory test, screening for a disease always leads to more testing. In many cases, these tests are invasive, either entailing radiation exposure (CT scan) or complicated patient preparation and discomfort during the procedure (colonoscopy). In some cases, for example with NIPT testing, the confirmatory test (amniocentesis or chorionic villus sampling) is invasive and increase the risk of harm (abortion of the foetus in this case), which may lead to harm for people who are actually healthy.
Early diagnosis may not always improve prognosis
It is reasonable to assume that early diagnosis always improves the prognosis, but that is not always the case. In many cases, the cancer would develop so slowly that the person would never have known of it, or possibly only developed mild symptoms. However, cancer diagnosis almost always leads to aggressive treatment, which has its own effects on quality of life.
This is especially important for prostate cancer, for example. Prostate cancer is relatively common in elderly, but research has shown that many who are treated for subclinical prostate cancer would never have developed symptoms of the cancer, and would rather have died peacefully, never knowing that they even had the cancer. Also important to consider that cancer treatment causes significant reduction in quality of life, which is especially unfortunate if the cancer would never have caused symptoms anyway.
South Korea started screening for thyroid cancer in the late 20th century. Up until relatively recently, research showed that, while the incidince increased significantly (more cases of thyroid cancer were discovered), the mortality remained the same. In other words, screening detected more cases and lead to more people being treated for cancer, which is a burden to both the healthcare system and the individual, but screening could not demonstrate a reduction in mortality, which is arguably one of the most important goals of screening. This shows that screening can lead to significant overdiagnosis.[2]
In Norway, it is estimated that for every 6 case of breast cancer that is discovered due to screening, 1 of those cases are overtreated, meaning that the cancer in that one case would not have needed treatment if it wasn't screened for.
Disorders are often rare, which reduce the predictive value
As already established, pre-test probability influences the predictive value of a test. In asymptomatic people (the target population of screening tests), the pre-test probability is equal to the prevalence of the disorder. The disorder we screen for often have a very low prevalence; for example, breast cancer has a prevalence of 0,4%.
Because the disorders we screen for is so rare, the positive predictive value decreases.
A negative screening test does not guarantee disease-freedom
Even though most tests used to screen populations have high sensitivity and therefore a low rate of false negatives, false negatives still occur, giving many people the impression that they do not have a disorder when they do. This may lead to them not seeking healthcare for new symptoms which are actually due to a disorder, because they think the screening test has cleared them.
Screening a population is expensive
For screening to be effective, it needs to screen many people, usually many thousands. This is expensive, money which could be used to research other fields of medicine.
Diagnosis
When an investigation is ordered for diagnosis, one should already have a list of differential diagnoses before ordering the test, and the test should be able to narrow down the list of differential diagnoses. It's important to consider the test's specificity, sensitivity, positive predictive value, and negative predictive value in this. There is no reason to perform an investigation if it doesn't help narrow doen the number of differential diagnoses.
Using pre-test probability wisely
Because positive and negative predictive values depend on the pre-test probability, it's important to keep the it in mind.
For example, a negative D-dimer has a high negative predictive value for VTE. However, negative predictive value decreases with increasing pre-test probability. A person with a high pre-test probability (Wells score for PE of 7 or more) have a 40+% pre-test probability of PE. If the patient has a high pre-test probability, determined by their Wells score, the patient no longer has the same pre-test probability as the general population (which is low). The negative predictive value decreases, which makes a negative D-dimer unsuitable for ruling out PE in a person with high pre-test probability.
Follow-up and monitoring
Follow-up and monitoring of a disorder is also a common use of laboratory and imaging investigations. Examples include:
- CRP or leukocyte count following antibiotic prescription to evaluate the treatment response
- Yearly brain MRI following removal of a meningeoma, to try and catch a recurrence early, before it causes symptoms
However, it's important to keep in mind the requirement of value for the patient. In the first scenario, there is value as a lack of normalisation of inflammatory parametres in a patient treated with antibiotic for a bacterial infection may be a sign that the antibiotic is ineffective, which may require administration of a different antibiotic. In the second scenario, there is also value, as the earlier one can catch recurrence of a meningeoma, the better the prognosis after treatment. However, if the patient is in a condition where they will not receive treatment anyway (for example, if they are terminal), monitoring is not of value to the patient.
Evaluation of prognosis
In some cases, performing an investigation even though it won't change patient management can be useful if it provides information on patient prognosis. This is most common in case of patients with cancer.
External resources
References
- ↑ https://pubmed.ncbi.nlm.nih.gov/32326646/
- ↑ https://www.nejm.org/doi/full/10.1056/NEJMp1409841