Follow-Up of Celiac Disease in Adults: “When, What, Who, and Where”
Abstract
:1. Introduction
2. Follow-Up
- a gastroenterologist for diagnosis and medical care;
- a registered celiac dietitian for a supervised gluten-free diet plan and for follow-ups;
- access to a social worker to help with the implementation of the diet at work, school, and in families;
- access to a clinical psychologist for support services.
2.1. Disease Monitoring (When, What, and Who?)
- Recognition of “slow responders”, which are CeD patients who still report symptoms six months to a year after initiation of a GFD. This is a common occurrence, and while some consider these patients to be “non-responsive‘’, a cause can usually be identified when a systematic approach to follow-up is undertaken. The most common cause is an ongoing gluten intake, albeit unintentional.
- Increased awareness of neurological symptoms that are related to gluten, including gluten ataxia, peripheral neuropathy, foggy mind, anxiety, and depression [32].
- Consultation is needed with a dermatologist when there is a suspicion of dermatitis herpetiformis (DH), the skin manifestation of CeD [33].
- Monitoring of people with CeD should include verification of the normalization of laboratory abnormalities detected during the initial laboratory investigation. Upper gastrointestinal (GI) endoscopy with duodenal biopsies is recommended for monitoring in cases with a lack of clinical response or relapse of symptoms despite a GFD [29,30,34].
- Metabolic syndrome and fatty liver disease should be monitored in CeD patients [35]. Abnormal liver function tests are a common finding in CeD, with the strongest association reported at presentation or diagnosis. CeD hepatitis is manifested by mild hypertransaminasemia (three to five times the upper limit of normal) and is due to a gluten-dependent liver injury that settles on a GFD [36,37]. Autoimmune liver diseases such as autoimmune hepatitis, primary biliary cholangitis, and primary sclerosing cholangitis are also more common in celiac disease. An increasingly reported complication is that of non-alcoholic fatty liver disease, which can occur as part of metabolic syndrome after starting the GFD. Long-term GFD has been associated with metabolic dysregulation and cardiovascular complications. Patients with metabolic dysfunction-associated fatty liver disease need strict counseling regarding increasing physical activity and optimizing their diet to reduce caloric intake, enrich unprocessed, naturally gluten-free foods, and minimize highly refined carbohydrates and saturated fat [38,39,40].
- The timing of bone density studies should follow a CeD-specific schedule with a defined age to start DXA screening [29]. It is important because osteopenia and, less frequently, osteoporosis are common in CeD. This applies for both females and males.
- Associated auto-immune conditions (in particular hypothyroidism) need to be checked regularly [28].
- Some CeD patients, especially young adults at diagnosis, have an increasing need for psychosocial counseling [41].
- CeD is associated with an increased risk of pneumococcal sepsis and mortality, and, therefore, pneumococcal vaccination is recommended, although practices differ widely. Some guidelines (ACG) recommend this vaccine for all adults with CeD [30], but, in some centers, it is given arbitrarily to all CeD patients with smaller spleens (125 cc) or beginning at the age of 70 years [42]. More generally, vaccination schedules for various infectious agents should be clarified for people with CeD.
- Tissue transglutaminase antibodies (IgA anti-TG2) have been shown in published studies to be insufficient for predicting relapse; other biomarkers are required, similar to the impact of fecal calprotectin measurement in the care of IBD patients [43].
- Proper data are still lacking on long-term outcomes in follow-up disease activity scores, such as the frequency of outpatient visits, histological follow-up, and cost effectiveness. CeD guidelines suggest that a full assessment of disease activity, such as antibodies and investigating for deficiency of essential elements, needs to be performed before starting GFD and after an adequate period, e.g., 12–24 months, to assess reversal or improvement in the manifestations of CeD [29,30].
- Specific attention to the possibility of refractory CeD (RCD); making the distinction between RCD type I and type II; and closely monitoring the nutritional status of both types. Clinicians require a “Red Flags” index for the diagnosis of refractory CeD, which carries a higher risk of developing lymphoproliferative malignancies [1,44]. A simple “Red Flags” index, using early signs and symptoms for family members and high-risk patients for developing CeD, might be useful. Specialist care of refractory CeD is important, and expediting review by an appropriate specialist may be aided by such a tool. It is recommended that patients with RCD II should be referred to secondary celiac centers with RCD-experienced gastroenterologists, immunologists, and hematologists [29].
2.2. Assessment of Dietary Adherence during the Follow-Up
2.3. Nutritional Education
2.4. Indications for Follow-Up Small Bowel Biopsy after GFD
2.5. Screening for Celiac Disease in Family Members
2.6. Interdisciplinary Team Membership
2.7. Celiac Disease Center and Coordinated Care Models
2.8. Celiac Disease Patient Registries
3. The Setting of Clinics
3.1. Face-to-Face
3.2. Virtual Clinics and Dietitians in the Lead
3.3. General Practitioners’ Key Roles in the Future
3.4. Patient Preferences
4. Gluten-Free Food in Outpatient Clinics and during Admission to Hospitals
5. Conclusions
Key Points
- ○
- Follow-ups of patients with CeD are important and include ensuring symptom resolution, optimization of nutrition and weight, normalization of serology, nutrient levels and bone density, preventive care, and minimization of long-term morbidity.
- ○
- Dieticians as well as psychosocial professionals should be an integral part of the multi-disciplinary follow-up team.
- ○
- CeD patient follow-ups are inconsistent and variable, and more studies are needed to inform on the best approach.
- ○
- An important surrogate endpoint of progress on a GFD is small bowel mucosal healing.
- ○
- There is a requirement for a “Red Flags” index for the diagnosis of refractory CeD, which carries a higher risk of developing lymphoproliferative malignancies.
- ○
- RCD II should be referred to secondary CeD centers with RCD-experienced gastroenterologists, immunologists, and hematologists.
- ○
- GPs will be a solution if the critical number of diagnosed celiacs in a local population is high enough.
- ○
- There is a need for models of care for CeD patients that facilitate effective follow-up and utilize health care resources in an efficient manner; the use of technologies such as video calls and smart phone apps carry a lot of appeal, but more research is needed.
- ○
- A CeD-Monitoring Index (consisting solely of patient-reported outcomes) might reduce time to recovery, increase GFD adherence, and reduce the number of F2F-outpatient visits.
Author Contributions
Funding
Institutional Review Board Statement
Informed Consent Statement
Data Availability Statement
Conflicts of Interest
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Time | What Is Needed | Who *? How? |
---|---|---|
At diagnosis | Physical Examination (BMI) | Physician and dietician. Face-to-face |
Counselling by a “celiac” dietician | ||
Discuss family screening | ||
Recommend Celiac Society or Support group | ||
Serology (IgA-anti TG2), lab, DXA (30–35 years start) or at diagnosis in special scenarios | ||
Visit 3–4 months | Assess symptoms and compliance | Gastroenterologist and/or dietician; Face-to-face, telephone, or video call |
Serology (IgA-anti TG2) | ||
Routine tests (if previously abnormal) | ||
At 12 months | Assess Weight, symptoms | Physician and/or dietitian Face-to-face, telephone, or video call |
Diet review | ||
Celiac serology, routine tests | ||
Thyroid function tests | ||
Metabolic status | ||
Small bowel biopsy (not routinely) | ||
At 24 months | Symptoms and dietary review | Physician and/or dietitian Face-to-face, telephone, or video call |
Celiac serology | ||
Other tests if clinically indicated | ||
Thereafter every 1–2 years | Assess symptoms | Physician or dietitian Face-to-face, telephone, or video call |
Consider dietary review | ||
Celiac serology | ||
Thyroid function tests | ||
Other tests as clinically indicate | ||
Bone densitometry (if abnormal) |
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Mulder, C.J.J.; Elli, L.; Lebwohl, B.; Makharia, G.K.; Rostami, K.; Rubio-Tapia, A.; Schumann, M.; Tye-Din, J.; Zeitz, J.; Al-Toma, A. Follow-Up of Celiac Disease in Adults: “When, What, Who, and Where”. Nutrients 2023, 15, 2048. https://doi.org/10.3390/nu15092048
Mulder CJJ, Elli L, Lebwohl B, Makharia GK, Rostami K, Rubio-Tapia A, Schumann M, Tye-Din J, Zeitz J, Al-Toma A. Follow-Up of Celiac Disease in Adults: “When, What, Who, and Where”. Nutrients. 2023; 15(9):2048. https://doi.org/10.3390/nu15092048
Chicago/Turabian StyleMulder, Chris J. J., Luca Elli, Benjamin Lebwohl, Govind K. Makharia, Kamran Rostami, Alberto Rubio-Tapia, Michael Schumann, Jason Tye-Din, Jonas Zeitz, and Abdulbaqi Al-Toma. 2023. "Follow-Up of Celiac Disease in Adults: “When, What, Who, and Where”" Nutrients 15, no. 9: 2048. https://doi.org/10.3390/nu15092048
APA StyleMulder, C. J. J., Elli, L., Lebwohl, B., Makharia, G. K., Rostami, K., Rubio-Tapia, A., Schumann, M., Tye-Din, J., Zeitz, J., & Al-Toma, A. (2023). Follow-Up of Celiac Disease in Adults: “When, What, Who, and Where”. Nutrients, 15(9), 2048. https://doi.org/10.3390/nu15092048