SUPERSEDED Local Coverage Determination (LCD)

Vitamin D Assay Testing

L34051

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Proposed LCD
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Document Note

Note History

Contractor Information

LCD Information

Document Information

Source LCD ID
N/A
LCD ID
L34051
Original ICD-9 LCD ID
Not Applicable
LCD Title
Vitamin D Assay Testing
Proposed LCD in Comment Period
N/A
Source Proposed LCD
DL34051
Original Effective Date
For services performed on or after 10/01/2015
Revision Effective Date
For services performed on or after 12/01/2019
Revision Ending Date
N/A
Retirement Date
N/A
Notice Period Start Date
12/19/2016
Notice Period End Date
02/02/2017

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Issue

Issue Description
Issue - Explanation of Change Between Proposed LCD and Final LCD

CMS National Coverage Policy

Title XVIII of the Social Security Act, Section 1862(a)(1)(A) states that no Medicare payment shall be made for items or services which are not reasonable and necessary for the diagnosis or treatment of illness or injury.

Title XVIII of the Social Security Act, Section 1862(a)(7). This section excludes routine physical examinations.

Title XVIII of the Social Security Act, Section 1833(e) states that no payment shall be made to any provider for any claim that lacks the necessary information to process the claim.

42CFR410.32(a) requires a clinical diagnostic test be ordered by the physician who is treating the patient for a specific medical problem and uses the results in the management of the beneficiary’s specific problem.

MBPM Internet Only Manual(IOM 100-02), chap. 6, §20.4.3 applies 42CFR410.32 to hospitals.

Coverage Guidance

Coverage Indications, Limitations, and/or Medical Necessity

Vitamin D is called a "vitamin" because of its exogenous source, predominately from oily fish in the form of vitamin D 2 and vitamin D 3. It is more accurate to consider fat-soluble Vitamin D as a steroid hormone, synthesized by the skin and metabolized by the kidney to an active hormone, calcitriol. Clinical disorders related to vitamin D may arise because of altered availability of the parent vitamin D, altered conversion of vitamin D to its predominant metabolites, altered organ responsiveness to dihydroxylated metabolites and disturbances in the interactions of the vitamin D metabolites with PTH and calcitonin. Normal levels of Vitamin D range from 20 – 50 ng/dl. This LCD identifies the indications and limitations of Medicare coverage and reimbursement for the lab assay.

Indications:

Measurement of 25-OH Vitamin D level is indicated for patients with:

    • chronic kidney disease stage III or greater

 

    • cirrhosis

 

    • hypocalcemia

 

    • hypercalcemia

 

    • hypercalciuria

 

    • hypervitaminosis D

 

    • parathyroid disorders

 

    • malabsorption states

 

    • obstructive jaundice

 

    • osteomalacia

 

      • osteoporosis if
          • i. T score on DEXA scan
            ii. History of fragility fractures or
            iii. FRAX > 3% 10-year probability of hip fracture or 20% 10-year probability of other major osteoporotic fracture or
            iv. FRAX > 3% (any fracture) with T-score
            v. Initiating bisphosphanate therapy (Vit D level should be determined and managed as necessary

before bisphosphonate is initiated)

    • osteosclerosis/petrosis
    • rickets
    • vitamin D deficiency on replacement therapy related to a condition listed above; to monitor the efficacy of treatment.


    Measurement of 1, 25-OH Vitamin D level is indicated for patients with:

      • unexplained hypercalcemia (suspected granulomatous disease or lymphoma)

     

      • unexplained hypercalciuria (suspected granulomatous disease or lymphoma)

     

      • suspected genetic childhood rickets

     

      • suspected tumor-induced osteomalacia

     

    • nephrolithiasis or hypercalciuria


    Limitations:

    Testing may not be used for routine or other screening.

    Both assays of vitamin D need not be performed for each of the above conditions. Often, one type is more appropriate for a certain disease state than another. The most common type of vitamin D deficiency is 25-OH vitamin D. A much smaller percentage of 1, 25-dihydroxy vitamin D deficiency exists; mostly, in those with renal disease. Although it is not the active form of the hormone, 25-OH vitamin D is much more commonly measured because it better reflects the sum total of vitamin D produced endogenously and absorbed from the diet than does the level of the active hormone 1, 25-dihydroxy vitamin D. Deficiency of 1, 25-dihydroxy vitamin D, which is present at much lower concentrations, does not necessarily reflect deficiency of 25-OH vitamin D and its measurement should be limited to the indications listed. Documentation must justify the test(s) chosen for a particular disease entity. Various component sources of 25-OH vitamin D, such as stored D or diet-derived D, should not be billed separately.

    Once a beneficiary has been shown to be vitamin D deficient, further testing may be medically necessary only to ensure adequate replacement has been accomplished. If Vitamin D level is between 20 and 50 ng/dl and patient is clinically stable, repeat testing is often unnecessary; if performed, documentation most clearly indicate the necessity of the test. If level 60 ng/dl, a subsequent level(s) may be reimbursed until the level is within the normal range.

    Summary of Evidence

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    Analysis of Evidence (Rationale for Determination)

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    Proposed Process Information

    Synopsis of Changes
    Changes Fields Changed
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    Associated Information
    Sources of Information
    Bibliography
    Open Meetings
    Meeting Date Meeting States Meeting Information
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    Contractor Advisory Committee (CAC) Meetings
    Meeting Date Meeting States Meeting Information
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    MAC Meeting Information URLs
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    Comment Period Start Date
    Comment Period End Date
    Reason for Proposed LCD
    Requestor Information
    This request was MAC initiated.
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    Contact for Comments on Proposed LCD

    Coding Information

    Bill Type Codes

    Code Description

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    Revenue Codes

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    CPT/HCPCS Codes

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    ICD-10-CM Codes that Support Medical Necessity

    Group 1

    Group 1 Paragraph:

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    Group 1 Codes:

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    ICD-10-CM Codes that DO NOT Support Medical Necessity

    Group 1

    Group 1 Paragraph:

    N/A

    Group 1 Codes:

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    Additional ICD-10 Information

    General Information

    Associated Information

    Documentation must clearly indicate the necessity for the test(s), any and all repeat testing and frequency of testing.

    The medical record must be made available to Medicare upon request.

    Sources of Information

    1. IOM (Institute of Medicine). Dietary Reference Intake for Calcium and Vitamin D.2011. Washington D.C.: the National Academies Press

    2. American Medical Association (AMA). Council on Science and Public Health "Appropriate Supplementation of Vitamin D," CSAPH Report 4-A-09.

    3. Autier P, Gandini S. Vitamin D Supplementation and Total Mortality. A Meta-analysis of Randomized Controlled Trials. Arch Intern Med. 2007;167(16);1730-1737.

    4. Bischoff-Ferrari HA, Dawson-Hughs B, Willett W, et al. Effect of vitamin D on falls a meta-analysis. JAMA April 2004;291:16:1999-2006. www.jama.com. Accessed 03/04/2009.

    5. Bischoff-Ferrari HA, Dietrich T, Orav EJ, Dawson-Hughes B. Positive association between 25-Hydroxy vitamin D levels and bone mineral density: a population-based study of younger and older adults. The American Journal of Medicine. 2004;116:634-639.

    6. Bischoff-Ferrari HA, Willett W, Wong J, Giovannucci E, Dietrich T, Dawson-Hughes B. Fracture prevention with vitamin D supplementation, a meta-analysis of randomized controlled trials. JAMA. May 2005;293:18:2257-2264. www.jama.com. Accessed 03/04/2009.

    7. Bodnar LM, Simhan HN, Powers RW, Frank MP, Cooperstein E, Roberts JM. High prevalence of vitamin D insufficiency in black and white pregnant women residing in the northern United States and their neonates. J Nutr. 2007;137:447-452. http://jn.nutrition.org. Accessed 02/10/2009.

    8. Cannell JJ. Autism and Vitamin D. Med Hypothese. 2008;70:4:750-759. http://www.ncbi.nlm.nih.gov/pubmed/17920208. Accessed 02/10/2009.

    9. Cannell JJ, Hollis BW, Zasloff M, Heaney RP. Diagnosis and treatment of vitamin D deficiency. Expert Opin Pharmacother. 2008;9:1-12.

    10. Chapuy M, Arlot M, Duboeuf F, et al. vitamin D3 and calcium to prevent hip fractures in elderly women. The New England Journal of Medicine. December 1992;327:23:1637-1641.

    11. Chronic Kidney Disease 2006: A Guide to Select NKF-KDOQI Guidelines and Recommendations.

    12. Woolcott CG, Wilkens LR, Nomura AM et al. Plasma 25-hydroxyvitamin D levels and the risk of colorectal cancer: the multiethnic cohort study. Cancer Epidemiol Biomarkers Prev 2010; 19(1):130-134.

    13. Vitamin D and Calcium Systematic Review of Health Outcomes. Structured Abstract. Agency for Healthcare Research and Quality. Rockville, MD. http://www.ahrq.gov/clinic/tp/vitadcaltp.htm

    14. MacLean C, Alexander A, Carter J et al. Comparative Effectiveness of Treatments to Prevent Fractures in Men and Women with Low Bone Density or Osteoporosis Executive Summary. No.12 (Prepared by Southern California/RAND Evidence-based Practice Center under Contract with the Agency for Healthcare Research and Quality. December 2007.

    15. Vitamin D Evidence-based Monograph. The Natural Standard Research Collaboration. (Last updated June 1, 2010.) http://naturalstandard.com; and http://www.mayoclinic.com/health/vitamin-d

    16. Bjelakovic, Goran, Gluud et al. Vitamin D supplementation for prevention of mortality in adults. (Protocol) Cochrane Database of Systematic Reviews 2008, Issue 4. Art. No,: CD007470. DOI:10.1002/14651858.CD007470. [Last review 2010; no changes to last published edit 03 May 2009.]

    17. Giovannucci E, Liu Y, Hollis BW, Rimm EB. 25-Hydroxyvitamin D and Risk of Myocardial Infarction in Men; A Prospective Study. Arch Intern Med.2008:168(11):1174-1180.

    18. Wagner CL, Greer FR, and the Section on Breastfeeding and Committee on Nutrition. Prevention of Rickets and Vitamin D Deficiency in Infants, Children, and Adolescents. [published correction appears in Pediatrics 2009;123;197.]. Pediatrics 2008;122;1142-1152.

    19. Lafferty, FW. Differential diagnosis of hypercalcemia. J Bone Miner Res 1991; 6 Suppl 2:S51.

    20. Silverberg S, Bilezikian. Primary Hyperparathyroidism. In: Primer on Metabolic Bone Diseases and Disorders of Mineral Metabolism. 7th ed., 2008:7:302-306.

    21. Horwitz M, Hodak S, Stewart A. Non-Parathyroid Hypercalcemia. In: Primer on Metabolic Bone Diseases and Disorders of Mineral Metabolism. 7th ed., 2008:7:307-312.

    22. Am. J. Med. 107(6):561-567(1999), "The effects of vitamin D insufficiency in patients with primary hyperparathyroidism", Silverberg, S.J., et.al.

    23. Schilling, T, Pecherstorfer, M, Blind, E, et al. Parathyroid hormone-related protein (PTH-rP) does not regulate serum 1,25-dihydroxyvitamin D levels in hypercalcemia of malignancy. J Clin Endocrinol Metab 1993; 76:801.

    24. Jacobus, CH, Holick, MF, Shao, Q, et al. Hypervitaminosis D associated with drinking milk. N Engl J Med 1992; 326:1173.

    25. Goltzman, D, Cole, DEC. Hypoparathyroidism. In Primer on the Metabolic Bone Diseases and Disorders of Bone Metabolism, American Society of Bone and Mineral Research 2006; 6:216.

    26. Bernstein, CN, Leslie, WD, Leboff, MS. AGA technical review on osteoporosis in gastrointestinal diseases. Gastroenterology 2003; 124:795.

    27. Johnson, JM, Maher, JW, Demaria, EJ, et al. The Long-term Effects of Gastric Bypass on Vitamin D Metabolism. Ann Surg 2006; 243:701.

    28. American Gastroenterological Association medical position statement: guidelines on osteoporosis in gastrointestinal diseases. Gastroenterology 2003; 124:791.

    29. Hahn, TJ. Drug-induced disorders of vitamin D and mineral metabolism. Clin Endocrinol Metab 1980; 9:107.

    30. Sotaniemi, EA, Hakkarainen, HK, Puranen, JA, Lahti, RO. Radiologic bone changes and hypocalcemia with anticonvulsant therapy in epilepsy. Ann Intern Med 1972; 77:389.

    31. Välimäki, MJ, Tiihonen, M, Laitinen, K, et al. Bone mineral density measured by dual-energy X-ray absorptiometry and novel markers of bone formation and resorption in patients on antiepileptic drugs. J Bone Miner Res 1994; 9:631.

    32. Compston, JE. Hepatic osteodystrophy: Vitamin D metabolism in patients with liver disease. Gut1986; 27:1073.

    33. Holick, MF. Vitamin D deficiency. N Engl J Med 2007; 357:266.

    34. Am. J. Kidney Dis.50(1):59-68(2007) "Changes in serum 25-hydroxyvitamin D and plasma intact PTH levels following treatment with ergocalciferol in patients with CKD", Al Aly, Z, et. al.

    35. Bone, (2008), "Serum 25-hydroxyvitamin D as an independent determinant of 1-84 PTH and bone mineral density in non-diabetic predialysis CKD patients", Tomida, K., et. al.

    36. Ceglia L. Vitamin D and skeletal muscle tissue and function. Mol Aspects Med. 2008 Dec;29(6):407-14. Epub 2008 Aug 8. Review.

    37. Ward KA, Das G, Berry JL, Roberts SA, Rawer R, Adams JE, Mughal Z. Vitamin D status and muscle function in post-menarchal adolescent girls. J Clin Endocrinol Metab. 2009 Feb;94(2):559-63. Epub 2008 Nov 25.

    38. Gordon PL, Sakkas GK, Doyle JW, Shubert T, Johansen KL. Relationship between vitamin D and muscle size and strength in patients on hemodialysis. J Ren Nutr. 2007 Nov;17(6):397-407. PubMed PMID: 17971312.

    39. Hollick MF High Prevalence of Vitamin D Inadequacy and Implications for Health Mayo Clin Proc. 2006;81(3):353-373.

    40. Buischoff-Ferrari, HA et al Estimation of optimal serum concentrations of 25-hydroxyvitamin D for multiple health outcomes Am J Clin Nutr (2006) 84:18.

    41.Ybarra J, Sánchez-Hernández J, Pérez A. Hypovitaminosis D and morbid obesity. Nurs Clin North Am. 2007 Mar;42(1):19-27, v. Review.

    42. Goldner WS, Stoner JA, Thompson J, Taylor K, Larson L, Erickson J, McBride C. Prevalence of vitamin D insufficiency and deficiency in morbidly obese patients: a comparison with non-obese controls. Obes Surg. 2008 Feb;18(2):145-50.

    43. Sánchez-Hernández J, Ybarra J, Gich I, De Leiva A, Rius X, Rodríguez-Espinosa J, Pérez A. Effects of bariatric surgery on vitamin D status and secondary hyperparathyroidism: a prospective study. Obes Surg. 2005 Nov-Dec;15(10):1389-95.

    44. Lee JH, O’Keefe JH, Bell D et al. Vitamin D deficiency. JACC. 2008; 52(24):1949-56.

    45. Lapp JL. Vitamin D: bone health and beyond. Am J Lifestyle Med. 2009;3:386-93.

    46. Binkley N, Krueger D, Gemar D, Drezner MK. Correlation among 25-hydroxy-vitamin D assays. J Clin Endocrinol Metab. 2008; 93:1804–1808

    47. Bolland MJ, Bacon CJ, Horne AM et al. Vitamin D Insufficiency and Health. Am J Clin Nutr 2010; 91:82-89.

    48. Other Contractor(s)' Policies.

    Bibliography

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    Revision History Information

    Revision History Date Revision History Number Revision History Explanation Reasons for Change
    12/01/2019 R10

    The LCD is revised to remove CPT/HCPCS codes in the Keyword Section of the LCD.

    At this time 21st Century Cures Act will apply to new and revised LCDs that restrict coverage which requires comment and notice. This revision is not a restriction to the coverage determination; and, therefore not all the fields included on the LCD are applicable as noted in this policy.

    • Other (The LCD is revised to remove CPT/HCPCS codes in the Keyword Section of the LCD.
      )
    12/01/2019 R9

    12/01/2019: At this time 21st Century Cures Act will apply to new and revised LCDs that restrict coverage which requires comment and notice. This revision is not a restriction to the coverage determination; and, therefore not all the fields included on the LCD are applicable as noted in this policy.

    As required by CR 10901, all billing and coding information has been moved to the companion article, this article is linked to the LCD.

    • Provider Education/Guidance
    • Revisions Due To Code Removal
    10/01/2018 R8

    At this time 21st Century Cures Act will apply to new and revised Articles that restrict coverage which requires comment and notice. This revision is not a restriction to the coverage determination; and, therefore not all the fields included on the Article are applicable as noted in this policy.

    08/09/2018 - For the following ICD-10 code descriptions were changed in the ICD-10 Codes that Support Medical Necessity field:
    Z68.43 descriptor was changed in Group 1 Effective 10/01/2018

    • Revisions Due To ICD-10-CM Code Changes
    02/03/2017 R7 Added ICD-10 Codes A15.0, A15.4, A15.5, A15.6, A15.7, A15.8, Z79.3, Z79.4, Z79.51, Z79.52, Z79.810, Z79.811, Z79.818, Z79.82, Z79.83, Z79.84, Z79.890, Z79.891, Z79.899
    • Creation of Uniform LCDs Within a MAC Jurisdiction
    02/03/2017 R6 Addition of codes from 2016 ICD-10 Coding updates added to Final E89.820; E89.821; E89.822; E89.823
    • Revisions Due To ICD-10-CM Code Changes
    02/03/2017 R5 This LCD version was created as a result of DL34051 being released to a Final LCD.
    • Creation of Uniform LCDs Within a MAC Jurisdiction
    10/01/2016 R4 Typographical Error
    • Typographical Error
    10/01/2015 R3 The following ICD-10 Codes were added from the ICD-10 2016-2017 update: E89820, E89821, E89822, E89823, K9041, K9049. Code K90.4 was deleted.
    • Revisions Due To ICD-10-CM Code Changes
    10/01/2015 R2 The LCD is revised to add M85.80 and M85.88 to the ICD-10 Codes that Support Medical Necessity section; CPT 82306 only.
    • Reconsideration Request
    10/01/2015 R1 This LCD is revised to remove the paragraph, “When requesting an individual consideration through the written redetermination (formerly appeal) process, providers must include all relevant medical records and any pertinent peer-reviewed literature that supports the request. At a minimum two (2) Phase II studies (human studies of efficacy, pivotal) or one (1) Phase III study (evidence of safety and efficacy, pivotal) must be submitted for the Medical Director’s review.“ from the Associated Information field.
    • Other (Removed the paragraph, “When requesting an individual consideration through the written redetermination (formerly appeal) process, providers must include all relevant medical records and any pertinent peer-reviewed literature that supports the request. At a minimum two (2) Phase II studies (human studies of efficacy, pivotal) or one (1) Phase III study (evidence of safety and efficacy, pivotal) must be submitted for the Medical Director’s review.”)
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