1.8.3.0 Celi­ac Dis­ease

Rec­om­men­da­tions

13.25 Screen chil­dren with type 1 di­a­betes for celi­ac dis­ease by mea­sur­ing IgA tis­sue trans­g­lu­tam­i­nase (tTG) an­ti­bod­ies, with doc­u­men­ta­tion of nor­mal total serum IgA lev­els, soon after the di­ag­no­sis of di­a­betes, or IgG to tTG and deami­dat­ed gliadin an­ti­bod­ies if IgA deficient. E

13.26 Re­peat screen­ing with­in 2 years of di­a­betes di­ag­no­sis and then again after 5 years and con­sid­er more fre­quent screen­ing in chil­dren who have symp­toms or a first-‍de­gree rel­a­tive with celi­ac dis­ease. B

13.27 In­di­vid­u­als with biop­sy-‍confirmed celi­ac dis­ease should be placed on a gluten-‍free diet and have a con­sul­ta­tion with a di­eti­tian ex­pe­ri­enced in man­ag­ing both di­a­betes and celi­ac dis­ease. B

Celi­ac dis­ease is an im­mune-‍me­di­at­ed dis­or­der that oc­curs with in­creased fre­quen­cy in pa­tients with type 1 di­a­betes (1.6–16.4% of in­di­vid­u­als com­pared with 0.3–1% in the gen­er­al pop­u­la­tion) (72,73,80–83).

Screen­ing for celi­ac dis­ease in­cludes mea­sur­ing serum lev­els of IgA and tis­sue trans­g­lu­tam­i­nase an­ti­bod­ies, or, with IgA deficien­cy, screen­ing can in­clude mea­sur­ing IgG tis­sue trans­g­lu­tam­i­nase an­ti­bod­ies or IgG deami­dat­ed gliadin pep­tide an­ti­bod­ies. Be­cause most cases of celi­ac dis­ease are di­ag­nosed with­in the first 5 years after the di­ag­no­sis of type 1 di­a­betes, screen­ing should be con­sid­ered at the time of di­ag­no­sis and re­peat­ed at 2 and then 5 years (82) or if clin­i­cal symp­toms in­di­cate, such as poor growth or in­creased hy­po­glycemia (83,84).

Al­though celi­ac dis­ease can be di­ag­nosed more than 10 years after di­a­betes di­ag­no­sis, there are insufficient data after 5 years to de­ter­mine the op­ti­mal screen­ing fre­quen­cy. Mea­surement of tis­sue trans­g­lu­tam­i­nase an­ti­body should be con­sid­ered at other times in pa­tients with symp­toms sug­gestive of celi­ac dis­ease (82). Mon­i­tor­ing for symp­toms should in­clude as­sessment of lin­ear growth and weight gain (83,84). A small-‍bowel biop­sy in an­ti­body-pos­i­tive chil­dren is rec­om­mend­ed to confirm the di­ag­no­sis (85). Eu­ro­pean guide­lines on screen­ing for celi­ac dis­ease in chil­dren (not specific to chil­dren with type 1 di­a­betes) sug­gest that biop­sy may not be nec­es­sary in symp­tomat­ic chil­dren with high an­ti­body titers (i.e., greater than 10 times the upper limit of nor­mal) pro­vided that fur­ther test­ing is per­formed (verification of en­domysial an­ti­body pos­i­tiv­i­ty on a sep­a­rate blood sam­ple). Whether this ap­proach may be ap­pro­pri­ate for asymp­tomat­ic chil­dren in high-‍risk groups re­mains an open ques­tion, though ev­i­dence is emerg­ing (86). It is also ad­vis­able to check for celi­ac dis­ease–as­so­ci­at­ed HLA types in pa­tients who are di­ag­nosed with­out a small in­testi­nal biop­sy. In symp­tomat­ic chil­dren with type 1 di­a­betes and confirmed celi­ac dis­ease, gluten-‍free diets re­duce symp­toms and rates of hy­po­glycemia (87). The chal­leng­ing di­etary re­stric­tions as­so­ci­at­ed with hav­ing both type 1 di­a­betes and celi­ac dis­ease place a significant bur­den on in­di­vid­u­als. There­fore, a biop­sy to confirm the di­ag­no­sis of celi­ac dis­ease is rec­om­mend­ed, es­pe­cial­ly in asymp­tomat­ic chil­dren, be­fore es­tab­lish­ing a di­ag­no­sis of celi­ac dis­ease (88) and en­dors­ing significant di­etary changes. A gluten-‍free diet was beneficial in asymp­tomat­ic adults with pos­i­tive an­ti­bod­ies confirmed by biop­sy (89).