Οι ανανεωμνες κατευθυντριες οδηγίες KDIGO 2017. Τί ... · 2020....

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Οι ανανεωμένες κατευθυντήριες οδηγίες KDIGO 2017. Τί άλλαξε στη διαχείριση του CKD-MBD. Ιωάννης Γριβέας, MD, PhD Νεφρολόγος

Transcript of Οι ανανεωμνες κατευθυντριες οδηγίες KDIGO 2017. Τί ... · 2020....

Page 1: Οι ανανεωμνες κατευθυντριες οδηγίες KDIGO 2017. Τί ... · 2020. 8. 4. · “CKD-MBD: Back to the Future A total of 12 recommendations were identified

Οι ανανεωμένες κατευθυντήριες οδηγίες KDIGO 2017.Τί άλλαξε στη διαχείριση του CKD-MBD.

Ιωάννης Γριβέας, MD, PhDΝεφρολόγος

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2017 Update2009 KDIGO Controversies Conference 2013 “CKD-MBD: Back to the Future

A total of 12 recommendations were

identified for revision.

•Work Group acknowledged the lack of high-quality evidence on which to base recommendations.

•Multiple randomized controlled trials (RCTs) and prospective cohort studies.

•KDIGO recognizesthe need to reexamine the

currency of its guidelines.

▪2017 Update3 followed a rigorousprocess of evidence review and appraisal, based on systematicreviews of results from clinical trials.

▪GRADE

Where appropriate, the Work Group issued “not graded”recommendations, based on general advice, thatwere not part of a systematic evidence

review.

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KDIGO 2017 GUIDELINE UPDATE CONTRIBUTORS

•Geoffrey Block (USA)

•Pieter Evenepoel (Belgium)

•Masafumi Fukagawa (Japan)

•Charles A. Herzog (USA)

•Linda McCann (USA)

•Sharon M. Moe (USA)

•Rukshana Shroff (UK)

•Marcello A. Tonelli (Canada)

•Nigel D. Toussaint (Australia)

•Marc G. Vervloet (The Netherlands)

Guideline Work Group

Markus Ketteler (Germany) – Co-chair

Mary B. Leonard (USA) – Co-chair

Evidence Review TeamJohns Hopkins University

Karen A. Robinson, Casey Rebholz, Lisa M. Wilson, Ermias Jirru,

Marisa Chi Liu, Jessica Gayleard, Allen Zhang

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DEXA-determined femoral BMD

BMD low in case of fracture

BMD high in case of fracture

Meta-Analysis

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Phosphate Binders in Moderate CKD

Block G et al. J Am Soc Nephrol. 2012;23:1407-1415.

ACTIVE PLACEBO PLACEB

O

LANTHANU

M

SEVELAME

R

CALCIU

M

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Phosphate Binders and Mortality

All-Cause Mortality Dialysis Inception

Di Iorio B et al. Clin J Am Soc Nephrol 2012;7:487-493

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Sevelamer vs. Calcium

Di Iorio B et al. Am J Kidney Dis. 2013;62:771-778

Arrythmias Cardiovascular Mortality

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“Hidden” Phosphate

Sherman RA et al. Clin J Am Soc Nephrol. 2009;4:1370-1373

“Hidden” Phosphate

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MOBILE PROJECTShow and explain your web, app or software projects using these gadget templates.

Place your screenshot here

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Secondary hyperparathyroidism (sHPT)

Attempt to control the disturbedcalcium, phosphorus, and vitamin Dmetabolism. sHPT causes vascular

and soft-tissue calcification and leadsto disturbances of mineral metabolismCKD-related mineral and

bone disorder (CKD-MBD).

CKD-MBD abnormalities have also been implicated as risk factors for the very rare but devastating calcific and thrombotic arteriolopathycalciphylaxis and lead to reduced health-related quality of life

(HRQoL).

.

.

sHPT-associated high FGF23 is independently associated with left ventricular hypertrophy, cardiovascular events and premature death.

The indication for sHPTtreatment results from these

clinical consequences

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Abnormalities in Metabolic Parameters Are Consequences of SHPT: Management of PTH, Ca, and P

Tomasello S. Diabetes Spectrum. 2008;21:19-25

Treatment approaches to the management of SHPT include Ca x P, PTH, and vitamin D.

Use of vitamin D and phosphate binders alone provide no direct way to control PTH levels without the risk of raising Ca and P levels.

Consequences of SHPT

Ca

PTH

PVit D

PTH

SystemicToxicity

Bone

Disease

Control Ca

• Control intake

• Adjust dialysate Ca

• Use Ca supplements or

vitamin D therapy (if Ca low)

Lower Elevated Serum P

• Control dietary intake

• Use phosphate binders

Increase Vitamin D

Levels

• Administer vitamin D

sterols to reduce PTH

Involved in homeostasis

of bone metabolism

• Maintains correct

• balance of Ca and P

• in the body

Ca = calcium; P = phosphate; PTH = parathyroid hormone; SHPT = secondary hyperparathyroidism.

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.

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The PRIMO Trial

Thadani R et al. JAMA. 2012;307:674-684

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The OPERA Trial

Wang A et al. J Am Soc Nephrol. 2014;25:175-186

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.

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EVOLVE: Lowering PTH

Chertow GM, et al. N Engl J Med. 2012;367:2482-2494

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EVOLVE Study: Cinacalcet

Chertow GM, et al. N Engl J Med. 2012;367:2482-2494

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Time to First Episode of Severe Unremitting HPT (Intent-to-Treat Analysis)

CinacalcetPlacebo

Pro

po

rtio

n E

ven

t-fr

ee

Time (months)

Hazard ratio, 0.43 (95% CI, 0.37, 0.50)Log-rank, p<0.001

0.0

0.4

0.5

0.6

0.7

0.8

0.9

1.0

0 4 8 12 16 20 24 28 32 36 40 44 48 52 56 60

Severe, unremitting HPT• Prespecified and defined

as– PTH > 1000 pg/ml

(106.0 pmol/l) withserum calcium > 10.5mg/dl (2.6 mmol/l) on2 consecutive occasionsOR

– PTH > 1000 pg/mlwith serum calcium>10.5 mg/dl on asingle occasion andsubsequent commercialcinacalcet use within 2months of thelaboratory assessmentOR

– parathyroidectomy

Chertow GM, et al. N Engl J Med. 2012;367:2482-2494

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Take home messages

• Prospective studies evaluating BMD testing inadults with CKD represent a substantialadvance since the original guideline from 2009,making a reasonable case for BMD testing if theresults will impact future treatment.

• It is important to emphasize theinterdependency of serum calcium, phosphate,and PTH for clinical therapeutic decision-making.

.

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Take home messages

▫ Phosphate-lowering therapies may only beindicated in the case of “progressive or persistenthyperphosphatemia”.

▫ New evidence suggests that excess exposure toexogenous calcium in adults may be harmful inall severities of CKD, regardless of other risk

markers.

.

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Take home messages

▫ It is reasonable to limit dietary phosphate intake, whenconsidering all sources of dietary phosphate (including“hidden” sources).

▫ The PRIMO and OPERA studies failed to demonstrateimprovements in clinically relevant outcomes but diddemonstrate increased risk of hypercalcemia. Accordingly,routine use of calcitriol or its analogs in CKD G3a-G5 is nolonger recommended.

.

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Take home messages

.

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THANKS!Any questions?