2.5.0.0 Pre­ven­tion and Man­age­ment of Di­a­betes Com­pli­ca­tions

Rec­om­men­da­tions

Nephropa­thy

13.69 Blood pres­sure should be mea­sured at every visit. A

13.70 Blood pres­sure should be op­ti­mized to re­duce risk and/‍or slow the pro­gres­sion of di­a­bet­ic kid­ney dis­ease. A

13.71 If blood pres­sure is >95th per­centile for age, sex, and height, in­creased em­pha­sis should be placed on lifestyle man­age­ment to pro­mote weight loss. If blood pres­sure re­mains above the 95th per­centile after 6 months, an­ti­hy­per­ten­sive ther­a­py should be ini­ti­at­ed. C

13.72 Ini­tial ther­a­peu­tic op­tions in­clude ACE in­hibitors or an­giotensin re­cep­tor block­ers. Other blood pres­sure–low­er­ing agents may be added as need­ed. C

13.73 Pro­tein in­take should be at the rec­om­mend­ed daily al­lowance of 0.8 g/‍kg/‍day. E

13.74 Urine al­bu­min-‍to-‍cre­a­ti­nine ratio should be ob­tained at the time of di­ag­no­sis and an­nu­al­ly there­after. An el­e­vat­ed urine al­bu­min-‍to-‍cre­a­ti­nine ratio (>30 mg/g cre­a­ti­nine) should be confirmed on two of three sam­ples. B

13.75 Es­ti­mat­ed glomeru­lar filtra­tion rate should be de­ter­mined at the time of di­ag­no­sis and an­nu­al­ly there­after. E

13.76 In non­preg­nant pa­tients with di­a­betes and hy­per­ten­sion, ei­ther an ACE in­hibitor or an an­giotensin re­cep­tor block­er is rec­om­mend­ed for those with mod­est­ly el­e­vat­ed uri­nary al­bu­min-‍to-‍cre­a­ti­nine ratio (30–299 mg/g cre­a­ti­nine) D and is strong­ly rec­om­mend­ed for those with uri­nary al­bu­min-‍to-‍cre­a­ti­nine ratio >300 mg/g cre­a­ti­nine and/‍or es­ti­mated glomeru­lar filtra­tion rate <60 mL/‍min/‍1.73 m2. E

13.77 For those with nephropa­thy, con­tin­ued mon­i­tor­ing (year­ly uri­nary al­bu­min-‍to-‍cre­a­ti­nine ratio, es­ti­mated glomeru­lar filtra­tion rate, and serum potas­si­um) may aid in as­sessing ad­her­ence and de­tecting pro­gres­sion of dis­ease. E

13.78 Re­fer­ral to nephrol­o­gy is rec­om­mend­ed in case of uncer­tainty of eti­ol­o­gy, wors­en­ing uri­nary al­bu­min-‍to-‍cre­a­ti­nine ratio, or de­crease in es­ti­mated glomeru­lar filtra­tion rate. E

Neu­ropa­thy

13.79 Youth with type 2 di­a­betes should be screened for the pres­ence of neu­ropa­thy by foot ex­am­i­na­tion at di­ag­no­sis and an­nu­al­ly. The ex­am­i­na­tion should in­clude in­spec­tion, as­sessment of foot puls­es, pin­prick and 10-g monofilament sen­sa­tion tests, test­ing of vi­bra­tion sen­sa­tion using 128-Hz tun­ing fork, and ankle reflexes. C

13.80 Pre­ven­tion should focus on achiev­ing glycemic tar­gets. C

Retinopa­thy

13.81 Screen­ing for retinopa­thy should be per­formed by di­lat­ed fun­doscopy or reti­nal pho­tog­ra­phy at or soon after di­ag­no­sis and an­nu­al­ly there­after. C

13.82 Op­ti­miz­ing glycemia is rec­om­mend­ed to de­crease the risk or slow the pro­gres­sion of retinopa­thy. B

13.83 Less fre­quent ex­am­i­na­tion (every 2 years) may be con­sid­ered if there is ad­e­quate glycemic con­trol and a nor­mal eye exam. C

Non­al­co­holic Fatty Liver Dis­ease

13.84 Eval­u­a­tion for non­al­co­holic fatty liver dis­ease (by mea­sur­ing as­par­tate aminotrans­ferase and ala­nine aminotrans­ferase) should be done at di­ag­no­sis and an­nu­al­ly there­after. B

13.85 Re­fer­ral to gas­troen­terol­o­gy should be con­sid­ered for per­sis­tent­ly el­e­vat­ed or wors­en­ing transam­i­nas­es. B

Ob­struc­tive Sleep Apnea

13.86 Screen­ing for symp­toms of sleep apnea should be done at each visit, and re­fer­ral to a pe­di­atric sleep spe­cial­ist for eval­u­a­tion and a polysomno­gram, if in­di­cated, is rec­om­mend­ed. Ob­struc­tive sleep apnea should be treat­ed when doc­u­ment­ed. B

Polycys­tic Ovary Syn­drome

13.87 Eval­u­ate for polycys­tic ovary syn­drome in fe­male ado­les­cents with type 2 di­a­betes, in­clud­ing lab­o­ra­to­ry stud­ies when in­di­cated. B

13.88 Oral con­tra­cep­tive pills for treat­ment of polycys­tic ovary syn­drome are not contrain­di­cated for girls with type 2 di­a­betes. C

13.89 Met­formin in ad­di­tion to lifestyle modification is like­ly to im­prove the men­stru­al cyclic­i­ty and hy­per­an­dro­genism in girls with type 2 di­a­betes. E

Car­dio­vas­cu­lar Dis­ease

13.90 In­ten­sive lifestyle in­ter­ven­tions fo­cus­ing on weight loss, dys­lipi­demia, hy­per­ten­sion, and dys­g­lycemia are im­por­tant to pre­vent overt macrovas­cu­lar dis­ease in early adult­hood. E

Dys­lipi­demia

13.91 Lipid test­ing should be per­formed when ini­tial glycemic con­trol has been achieved and an­nu­al­ly there­after. B

13.92 Op­ti­mal goals are LDL choles­terol <100 mg/dL (2.6 mmol/‍L), HDL choles­terol >35 mg/dL (0.905 mmol/‍L), and triglyc­erides <150 mg/dL (1.7 mmol/‍L). E

13.93 If LDL choles­terol is >130 mg/dL, blood glu­cose con­trol should be max­i­mized and di­etary coun­sel­ing should be pro­vided using the Amer­i­can Heart As­so­ci­a­tion Step 2 diet. E

13.94 If LDL choles­terol re­mains above goal after 6 months of di­etary in­ter­ven­tion, ini­ti­ate ther­a­py with statin, with goal of LDL <100 mg/dL. B

13.95 If triglyc­erides are >400 mg/dL (4.7 mmol/‍L) fast­ing or >1,000 mg/dL (11.6 mmol/‍L) nonfast­ing, op­ti­mize glycemia and begin fibrate, with a goal of <400 mg/dL (4.7 mmol/‍L) fast­ing (to re­duce risk for pan­cre­ati­tis). C

Car­diac Func­tion Test­ing

13.96 Rou­tine screen­ing for heart dis­ease with elec­tro­car­dio­gram, echocar­dio­gram, or stress test­ing is not rec­om­mend­ed in asymp­tomat­ic youth with type 2 di­a­betes. B

Co­mor­bidi­ties may al­ready be pre­sent at the time of di­ag­no­sis of type 2 di­a­betes in youth (122,163). There­fore, blood pres­sure mea­sure­ment, a fast­ing lipid panel, as­sessment of ran­dom urine al­bu­min-‍to-‍cre­a­ti­nine ratio, and a di­lat­ed eye ex­am­i­na­tion should be per­formed at di­ag­no­sis. There­after, screen­ing guide­lines and treat­ment rec­om­men­da­tions for hy­per­ten­sion, dys­lipi­demia, urine al­bu­min ex­cre­tion, and retinopa­thy are sim­i­lar to those for youth with type 1 di­a­betes. Ad­di­tion­al prob­lems that may need to be ad­dressed in­clude polycys­tic ovary dis­ease and other co­mor­bidities as­so­ci­at­ed with pe­di­atric obe­si­ty, such as sleep apnea, hep­at­ic steato­sis, or­tho­pe­dic com­pli­ca­tions, and psy­choso­cial con­cerns. The ADA po­si­tion state­ment “Eval­u­a­tion and Man­age­ment of Youth-‍Onset Type 2 Di­a­betes” (2) pro­vides guid­ance on the pre­ven­tion, screen­ing, and treat­ment of type 2 di­a­betes and its co­mor­bidities in chil­dren and ado­les­cents.

Youth-‍onset type 2 di­a­betes is as­so­ci­at­ed with significant mi­crovas­cu­lar and macrovas­cu­lar risk bur­den and a sub­stan­tial in­crease in the risk of car­dio­vas­cu­lar mor­bid­i­ty and mor­tal­i­ty at an ear­li­er age than those di­ag­nosed later in life (164). The high­er com­pli­ca­tion risk in ear­li­er-‍onset type 2 di­a­betes is like­ly re­lat­ed to pro­longed life­time ex­po­sure to hy­per­glycemia and other athero­genic risk fac­tors, in­clud­ing in­sulin re­sis­tance, dys­lipi­demia, hy­per­ten­sion, and chron­ic inflam­ma­tion. There is low risk of hy­po­glycemia in youth with type 2 di­a­betes, even if they are being treat­ed with in­sulin (165), and there are high rates of com­pli­ca­tions (139-142). These di­a­betes co­mor­bidities also ap­pear to be high­er than in youth with type 1 di­a­betes de­spite short­er di­a­betes du­ra­tion and lower A1C (163). In ad­di­tion, the pro­gres­sion of vas­cu­lar abnor­malities ap­pears to be more pro­nounced in youth-‍onset type 2 di­a­betes com­pared with type 1 di­a­betes of sim­i­lar du­ra­tion, in­clud­ing is­chemic heart dis­ease and stroke (166).