Sage Journals: Discover world-class research

Abstract

Background:

Primary lymphedema is genetically heterogeneous. Two of the most common forms of primary lymphedema are Milroy disease (MD) and lymphedema-distichiasis syndrome (LDS). This study aims to look further into the pathogenesis of the two conditions by analyzing the lymphoscintigram images from affected individuals to ascertain if it is a useful diagnostic tool.

Methods and Results:

The lymphoscintigrams of patients with MD and LDS were analyzed, comparing the images and transport parameters of the two genotypes against a control population. Lymphoscintigrams were available for 12 MD and 16 LDS patients (all genetically proven diagnoses). Eight of the 12 (67%) lymph scans performed on patients with MD demonstrated little or no uptake from the initial lymphatics and poor visualization of the inguinal lymph nodes. These changes were consistent with a “functional aplasia,” that is, the lymphatic vessels were present but appeared to be ineffective in absorbing the interstitial fluid into the lymphatic system. In patients with LDS the lymphoscintigraphic appearances were different. In 12 of the 16 scans (75%), the lymph scans were highly suggestive of lymphatic collector reflux. Quantification revealed a significantly reduced uptake of tracer within the inguinal lymph nodes and a higher residual activity in the feet at 2 hours in MD compared with LDS and compared with controls.

Conclusion:

Lymphoscintigraphic imaging and quantification can be characteristic in specific genetic forms of primary lymphedema and may be useful as an additional tool for in-depth phenotyping, leading to a more accurate diagnosis and providing insight into the underlying mechanism of disease.

Get full access to this article

View all access options for this article.

References

Petrova

, Karpanen

, Norrmen

, Mellor

, Tamakoshi

, Finegold

, Ferrell

, Kerjaschki

, Mortimer

, Yla-Herttuala

, Miura

, Alitalo

. Defective valves and abnormal mural cell recruitment underlie lymphatic vascular failure in lymphedema distichiasis. Nat Med, 2004; 10:974–981.

Ferrell

, Levinson

, Esman

, Kimak

, Lawrence

, Barmada

, Finegold

. Hereditary lymphedema: Evidence for linkage and genetic heterogeneity. Hum Mol Genet, 1998; 7:2073–2078.

Evans

, Brice

, Sotirova

, Mortimer

, Beninson

, Burnand

, Rosbotham

, Child

, Sarfarazi

. Mapping of primary congenital lymphedema to the 5q35.3 region. Am J Hum Genet, 1999; 64:547–555.

Connell

, Ostergaard

, Carver

, Brice

, Williams

, Mansour

, Mortimer

, Jeffery

, Lymphoedema

. Analysis of the coding regions of vegfr3 and vegfc in Milroy disease and other primary lymphoedemas. Hum Genet, 2009; 124:625–631.

Gordon

, Spiden

, Connell

, Brice

, Cottrell

, Short

, Taylor

, Jeffery

, Mortimer

, Mansour

, Ostergaard

. Flt4/vegfr3 and Milroy disease: Novel mutations, a review of published variants and database update. Hum Mutat, 2013; 34:23–31.

Mellor

, Hubert

, Stanton

AWB

, Tate

, Akhras

, Smith

, Burnand

, Jeffery

, Makinen

, Levick

, Mortimer

. Lymphatic dysfunction, not aplasia, underlies Milroy disease. Microcirculation, 2010; 17:281–296.

Brice

, Child

, Evans

, Bell

, Mansour

, Burnand

, Sarfarazi

, Jeffery

, Mortimer

. Milroy disease and the vegfr-3 mutation phenotype. J Med Genet, 2005; 42:98–102.

Karkkainen

, Saaristo

, Jussila

, Karila

, Lawrence

, Pajusola

, Bueler

, Eichmann

, Kauppinen

, Kettunen

, Yla-Herttuala

, Finegold

, Ferrell

, Alitalo

. A model for gene therapy of human hereditary lymphedema. Proc Natl Acad Sci USA, 2001; 98:12677–12682.

Mangion

, Rahman

, Mansour

, Brice

, Rosbotham

, Child

, Murday

, Mortimer

, Barfoot

, Sigurdsson

, Edkins

, Sarfarazi

, Burnand

, Evans

, Nunan

, Stratton

, Jeffery

. A gene for lymphedema-distichiasis maps to 16q24.3. Am J Hum Genet, 1999; 65:427–432.

10.

Fang

, Dagenais

, Erickson

, Arlt

, Glynn

, Gorski

, Seaver

, Glover

. Mutations in foxc2 (mfh-1), a forkhead family transcription factor, are responsible for the hereditary lymphedema-distichiasis syndrome. Am J Hum Genet, 2000; 67:1382–1388.

11.

Brice

, Mansour

, Bell

, Collin

, Child

, Brady

, Sarfarazi

, Burnand

, Jeffery

, Mortimer

, Murday

. Analysis of the phenotypic abnormalities in lymphoedema-distichiasis syndrome in 74 patients with foxc2 mutations or linkage to 16q24. J Med Genet, 2002; 39:478–483.

12.

Mellor

, Tate

, Stanton

AWB

, Hubert

, Maekinen

, Smith

, Burnand

, Jeffery

, Levick

, Mortimer

. Mutations in foxc2 in humans (lymphoedema distichiasis syndrome) cause lymphatic dysfunction on dependency. J Vasc Res, 2011; 48:397–407.

13.

Gloviczki

, Calcagno

, Schirger

, Pairolero

, Cherry

, Hallett

, Wahner

. Noninvasive evaluation of the swollen extremity: Experiences with 190 lymphoscintigraphic examinations. J Vasc Surg, 1989; 9:683–689; discussion 690.

14.

Williams

, Witte

, McNeill

. Radionuclide lymphangioscintigraphy in the evaluation of peripheral lymphedema. Clin Nucl Med, 2000; 25:451–464.

15.

Devoogdt

, Van den Wyngaert

, Bourgeois

, Lambrechts

, Van Kampen

, De Groef

, Geraerts

, Neven

, Vergote

, Tjalma

, Christiaens

, Stroobants

. Reproducibility of lymphoscintigraphic evaluation of the upper limb. Lymphat Res Biol, 2014; 12:175–184.

16.

Keramida

, Humphrys

, Ryan

, Peters

. “Stocking effect” in lymphoscintigraphy. Lymphat Res Biol, 2014; 12:194–196.

17.

Szuba

, Shin

, Strauss

, Rockson

. The third circulation: Radionuclide lymphoscintigraphy in the evaluation of lymphedema. J Nucl Med, 2003; 44:43–57.

18.

Modi

, Stanton

, Mortimer

, Levick

. Clinical assessment of human lymph flow using removal rate constants of interstitial macromolecules: A critical review of lymphoscintigraphy. Lymphat Res Biol, 2007; 5:183–202.

19.

Weissleder

, Weissleder

. Lymphedema: Evaluation of qualitative and quantitative lymphoscintigraphy in 238 patients. Radiology, 1988; 167:729–735.

20.

Keramida

, Winterman

, Wroe

, Aplin

, Peters

. Importance of accurate ilio-inguinal quantification in lower extremity lymphoscintigraphy. Nucl Med Commun, 2017; 38:209–214.

21.

Dale

. Primary lymphoedema when found with distichiasis is of the type defined as bilateral hyperplasia by lymphography. J Med Genet, 1987; 24:170–171.

22.

Burnand

, Glass

, Sundaraiya

, Mortimer

, Peters

. Popliteal node visualization during standard pedal lymphoscintigraphy for a swollen limb indicates impaired lymph drainage. Am J Roentgenol, 2011; 197:1443–1448.

Supplementary Material

Please find the following supplemental material available below.

For Open Access articles published under a Creative Commons License, all supplemental material carries the same license as the article it is associated with.

For non-Open Access articles published, all supplemental material carries a non-exclusive license, and permission requests for re-use of supplemental material or any part of supplemental material shall be sent directly to the copyright owner as specified in the copyright notice associated with the article.

0.00 MB

0.02 MB

Lymphoscintigraphic Abnormalities Associated with Milroy Disease and Lymphedema-Distichiasis Syndrome

Abstract

Background:

Methods and Results:

Conclusion:

Get full access to this article

References

Supplementary Material