Post on 02-Jan-2020
Tips & tricks bij diagnostiek van erfelijke nieraandoeningen
Prof Dr B Bammens, dienst nefrologie UZ LeuvenProf Dr K Claes, dienst nefrologie UZ Leuven
CASUS
Autosomal Dominant Polycystic Kidney Disease
Autosomal Dominant Polycystic Kidney Disease1/400 tot 1/1000 geboortes – progressieve cystische omvorming en groei nieren
nierfalen (mediaan): 58j PKD1, 79j PKD2 - 5-7% incidentie ESRD Vlaanderen
First reports: descriptive
Fogazzi et al. Nephrol Dial Transplant 13: 1039-1040, 1998
First reports: descriptive
Anatomie pathologique du corps humain, 1829Traité des maladies des reins, 1841
First reports: descriptive
“La polykystose rénale sera peut-être un jour traitable”
F. Lejars, 1888
Genetics: a giant step forward!
PKD 1 (± 80%)
cytogenetische locatie16p13.3
Genetics: a giant step forward!
PKD 2 (± 20%)
cytogenetische locatie4q22.1
Genetics: a giant step forward!
PKD1 > polycystin 1, een receptorPKD2 > polycystin 2, een transmembranair calcium kanaal
Genetics: a giant step forward!
PKD1 truncating vs. PKD1 non-truncating vs. PKD2
Cornec-Le Gall et al. J Am Soc Nephrol 24: 1006-1013, 2013
Cornec-Le Gall et al. J Am Soc Nephrol 24: 1006-1013, 2013
mediane leeftijd nierfalen
55j PKD1 truncating
67j PKD1 non-truncating
79j PKD2
Sometimes the story is not “typical”and/or
genetic evaluation is not straigthforward.
Casus: meisje, 6 jaar consultatie pediatrie nefrologieEchografie nav buikpijnklachtenMultipele cysten rechter nier
DD dysplastische/multi-cystische nierenPUJ stenosemaligniteitADPKD (cf. familiaal verhaal)
Casus: meisje, 6 jaar
StamboomPaternele grootmoeder
55j: borst carcinoma70j: sigmoid carcinoma
60j: geïnfecteerde levercystewaarvoor drainage
INDEX
StamboomPaternele grootmoeder
Hepatomegalie, multipele cystenNormale niergrootte, 1 (corticale) cyste
INDEX
StamboomPaternele grootvader
Normale leverMeerdere corticale niercysten
(passend bij leeftijd)Geen organomegalie
INDEX
StamboomVader
Multipele verspreide levercystenMeerdere niercysten van enkele mm tot 4.4cm
Geen organomegalie
INDEX
Genetics
INDEX
TSC1 en TSC2 eveneens negatief
Genetics: is there more than PKD1 & 2?
Paul et al. Kidney Int 85: 383-392, 2014
Genetics: there is more than PKD1 & 2
Porath et al. Am J Hum Gen 98: 1193-1207, 2016
cytogenetische locatie 11q12.3
Genetics: there is more than PKD1 & 2
Cornec-Le Gall et al. J Am Soc Nephrol 29: 13-23, 2018
StamboomZus
Enkele kleine cystjes linker nier
ND mut
mutND
mut
GANAB c.890 del exon 9
INDEX
Genetics: there is more than PKD1 & 2
Cornec-Le Gall et al. Am J Hum Gen 102: 832-844, 2018
normale niergrootte, cystische omvorming evoluerend naar schrompelnierenhistologisch interstitiële fibrose in niet-cystisch parenchymrecidiverend jicht in 1 van de families
fenotypischoverlapADTKD
cytogenetische locatie 3q27.3
Genetics: there is more than PKD1 & 2
Besse et al. J Am Soc Nephrol, 2019 https://doi.org/10.1681/ASN.2019030298
normale niergrootte, multipele niercysten in meerderheid dragerslevercysten eerder uitzonderlijkgeen notie van nierfalen
cytogenetische locatie 11q23.1
Need to go that extra mile!
Translational research in ADPKDPediatric Nephrology Department UZ LeuvenPKD Group (Lab of Pediatrics)
Lab of Ion Channel Research (KU Leuven/VIB)
Center for Human Genetics UZ LeuvenLaboratory for Genetics of Human Development
Djalila Mekahli
Rudi Vennekens
Koen Devriendt
Adult Nephrology Department UZ LeuvenNephrology & Renal Transplanation Research Group
Tips & tricks bij diagnostiek van erfelijke nieraandoeningen
Prof Dr B Bammens, dienst nefrologie UZ LeuvenProf Dr K Claes, dienst nefrologie UZ Leuven
CASUS
Some facts and figures• -25% of patients with CKD family history
• 10%-20% of patients with CKD mendelian causes
• 10% of patients with CKD “others” or “unknown”
Pediatric population
05
1015202530354045
Causes of ESRD (%)
Causes of ESRD
Pediatric population (<24 yr)
Exome sequencing in CKD Adult population
Family 1
• 1: haematuria, no proteinuria, no CKD
• 2: haematuria, proteinuria, w/wo CKD
• 3: ESRD due to focal andsegmental glomerulosclerosis
3
2
3 3
21
1
Family 1
• 1: haematuria, no proteinuria, no CKD
• 2: haematuria, proteinuria, w/wo CKD
• 3: ESRD due to focal andsegmental glomerulosclerosis
Biopsy: FSGS familial FSGS
3
2
3 3
21
1
Phenotype: new roles for old genes
• 1: haematuria, no proteinuria, no CKD• 2: haematuria, proteinuria, w/wo CKD• 3: ESRD due to focal and segmental
glomerulosclerosis
10-30% of adult onset familial FSGS (COL3A4, COL3A3 and COL3A5 mutations are found)
………
Collagen (COL4A) mutations are the most frequent mutations underlying adult focal segmental glomerulosclerosis; Gast C NDT 2015
3
2
3 3
21
1
Family 2• Outpatient clinic: Man, 60 y old:
o CKD 3A, bland sediment, no proteinuriao Diabetes, hypertensiono Ultrasound: 9,6 cm bilateral, no cystso Family history:
• pregnancy daughter: cysts on the kidney; follow-up OK • Diabetes • Cousin with severe learning disabilities Blood test
Family 3• ♀, 24 y old• 2008: Pyelonephritis: diagnosis of ADPKD based on
bilateral renal cortical cysts, kidneys normal size(family:negative)
• 2015: increase in cysts but echographic not typical
Blood test
Family 4• ♂, 50 y• Outpatient clinic: creat 2,5 mg/dl, 29 ml/min/1,73m²• Ultrasound: small kidneys; proteinuria 0,5 g/g• Medical history: hypertension• Family history: father transplanted at the age of 55 y, eci
Genetic testing
HNF1 beta mutation• Broad phenotype
o “MODY 5”o ADTKD, RCAD, hypoplasia, CAKUTo Deletion more severe cognitive disorders (family 1) o Hepatic disorderso Tubular disorder hypomagnesemia (2/3 families)
Expanding renal diseases phenotypes• Expansions across disease categories
o COL4A mutations (FSGS/TBMN/Alport syndrome)o HNF1 beta: no clear genotypic/fenotypic correlation
(RCAD/ CAKUT/ ADTKD)o PAX2: CAKUT/SRNS
Increase in knowledge
Van Eerde et al, Kidney International 2016
~20% ESRD before age 25-30yr: monogenic hereditary
(Vivante et al, Nat Rev Nephr 2016; Van Eerde et al, Kidney International 2016)
Consequences :reclassification
Expanding renal diseases phenotypes• Expansions across disease categories
o COL4A mutations (FSGS/TBMN/Alport syndrome)o HNF1 beta: no clear genotypic/fenotypic correlation
(RCAD/ CAKUT/ ADTKD)o PAX2: CAKUT/SRNS
• Expansions within disease categorieso WT1: mutation type and location within gene
affects risk of wilms tumour and SRNSo Type of mutation severity of the disease
• Expansions within phenotypeso LMX1B: NPS,FSGS
• Leading cause of pediatricnephropathy
• In isolation or part of a syndrome
• First choice: chromosomalmicroarray/especially in syndromal form
• diagnostic yield increase in patients with parenchymaldefects
CAKUT
Risk variants: APOL 1• APOL1 (G1/G2) risk variants:
• Sub Saharan Africans
• “hypertensive” nephropathy/ non-diabetic CKD (FSGS OR 17, HIVAN OR 29-89, sickle cell nephropathy)
• Renal biopsy: FSGS and solidified glomerulosclerosis
• Renal donor: two APOL1 risk variants: higher risk of graft failure
Freedman et al: APOL-1 associated nephropathy: a keycontributor to racial disparities in CKD AJKD 2018
Therapeutic consequences• Reclassification• Treatment
o Avoidance of immunosuppressive regimens for SRNSo COQ2, COQ6, ADCK4 Coenzyme Q10o TRPC6 mutation CNI
• Management of renal transplantationo Avoidance of intense immunosuppressive regimens in SRNSo aHUS/FSGS recurrence risko AGXT mutations (Primary hyperoxaluria type 1)o Donor screening (penetrance, eg TRPC6 mutation)
• Extrarenal manifestationso HNF1 beta deletion/mutationo JAG1 mutationso Syndromal mutations
• Confirmation of diagnosis in other family members
• Presymptomatic or predictive testing
• Preimplantation genetic testing
• Carrier testing (AR/X-linked)
Therapeutic consequences
Yield in proteinuria (n=167) dd 2018
Broad inclusion…
Yield in proteinuria (n=167)
Negative92
Positive42 11
24
413211
UV33
Proteinurie (cl3 = UV)COL4A3 +INF2 +COL4A5 +COL4A4CLCN5 +ACTN4TRPC6PLCE1ANLN
Reclassification UV class IV
Nefrogeneticaraadpleging @uzleuven
Welke patiënten?
Bespreken resultaten zo geen twijfel over fenotype
Evaluatie voor start geneticascreening zo geen eenduidig fenotype
Predictieve testing
Prenatale/pre-implantatie genetische diagnostiek
Nefrogeneticaraadpleging
• Familiale anamnese
• Psychologische impact
• Kinderen?
• PGT?
• Legaal?
• Sociaal?
• Toevallige bevindingen?
From: Comparison of the Complexity of Patients Seen by Different Medical Subspecialists in a Universal Health Care SystemJAMA Netw Open. 2018;1(7):e184852. doi:10.1001/jamanetworkopen.2018.4852
Conclusions• 10% of adult and 70% of pediatric ESRD caused by inherited
kidney disease• An aid in the ‘diagnostic’ odyssey• Insight in pathogenesis, guide clinical management• Indicated: early onset ESKD and/or other clinical features
consistent with inherited kidney disease• Data sharing !!!!!!• Need for guidelines (clinical, ethical, social) and more research
ClinicalgeneticistsMedical experts
Moleculardiagnostics Genomics
Core
Extraction facilities
Acknowledgements
Dr A CorveleynE Vanhoof
Prof Dr K Devriendt
De collega’s