Hong Kong Med J 2014;20(6):519–28 | Epub 29 Aug 2014
DOI: 10.12809/hkmj134116
© Hong Kong Academy of Medicine. CC BY-NC-ND 4.0
 
REVIEW ARTICLE     CME 
Management of secondary lymphoedema
TW Chiu, FHKAM (Surgery)
Division of Plastic Aesthetic and Reconstructive Surgery, Prince of Wales Hospital, Shatin, New Territories, Hong Kong
 
Corresponding author: Dr TW Chiu (torchiu@surgery.cuhk.edu.hk)
 Full paper in PDF
Abstract
Lymphoedema is a chronic, progressive condition. There is no cure but it is most easily managed with early recognition and therapy; those who do not have treatment tend to worsen rapidly and advanced disease is more difficult to treat than early disease. Surgery for lymphoedema is often regarded as a last resort but traditional excisional techniques that have been slightly modified for modern practice have shown good results, whilst newer microsurgical reconstruction techniques show promise although long-term results are lacking. This report provides an update on the therapy of lymphoedema.
 
 
 
Introduction
Lymphoedema is characterised by an imbalance of lymphatic flow leading to accumulation of protein-rich fluid in the interstitium of subcutaneous tissues. The consequent swelling may cause cosmetic and functional impairment, with significant physical and psychological morbidity. There is progressive damage to the lymphatics with inflammation, fibrosis and more swelling, eventually leading to elephantiasis. Recurrent infection is a common complication whilst lymphangiosarcomas are rare, occurring in 0.03% of patients surviving more than 10 years after mastectomy.1
 
It is traditional to classify lymphoedema into primary or secondary forms—in the former there is congenital lymphatic dysfunction related to dysplasia/malformation whilst in the latter there is disruption of lymphatic outflow related to another disease process or due to iatrogenic mechanisms.
 
Primary lymphoedema
The traditional subdivision of primary lymphoedema according to the time of onset has little clinical significance. There is confusion in the literature regarding the terms used, particularly, the various eponymous syndromes that have been described; most cases of primary lymphoedema are not associated with specific syndromes.
  • Congenita (10% of cases): the swelling is often present at birth (any swelling that begins before the age of 2 years is included in this group).
  • Praecox (80% of cases): patients present with swelling before the age of 35 years.
  • Tarda (10% of cases): patients present after the age of 35 years with swelling that is usually bilateral. Lymphatic vessels tend to be hyperplastic.
  •  
    It is important to appreciate that primary lymphoedema is a heterogeneous group with many subtypes occurring due to many different causes which are generally poorly understood. The term Milroy’s disease is often used interchangeably with lymphoedema congenita—it should only be applied to the group of inherited congenital lymphoedemas that demonstrates autosomal dominant inheritance; it is linked to vascular endothelial growth factor (VEGF) receptor–3 mutations (FLT4 gene on locus 5q35.3)2 3 and some evidence reveals that there is a functional defect of absorption rather than a gross structural defect.
     
    Lymphoedema praecox is the commonest type (80% of cases) and the swelling may be unilateral and limited to the foot/calf region. Patients lack distal lymphatics (hypoplasia) and often have a strong family history, some demonstrating autosomal dominant inheritance with different mutations in FOXC2 gene on chromosome 16.4 Some patients with praecox have distichiasis (double row of eyelashes) and form a distinct syndromic entity—lymphoedema distichiasis (mutation on 16q24.3).5 Patients with Meige’s disease, which is a subset of lymphoedema, usually present at puberty and the term should be reserved for those with the familial form of the disease (with as-yet unknown mutation).
     
    Secondary lymphoedema
    Worldwide, the commonest cause of secondary lymphoedema is filariasis, caused by infection with Wuchereria bancrofti. However, this condition is rare in developed countries such as Hong Kong where lymphoedema is most commonly related to malignant disease and, particularly, its treatment with surgery and/or irradiation.6 Upper limb lymphoedema most often follows the treatment of breast cancer, typically after a latent period of variable duration—77% of cases present within 3 years of surgery7 but the condition can arise at any time.
     
    Although the exact mechanism of the response of lymphatic channels to trauma is unknown, in general, the more extensive the surgery the greater is the damage. Thus, a formal axillary node dissection carries a risk of up to 20% compared to 4% to 10% following sentinel node biopsy.8 9 10 11 Irradiation causes fibrosis and inhibits lymphangiogenesis and, approximately, doubles the risk of developing lymphoedema after nodal surgery. Lymph vessels do have some regenerative capacity12 and not all patients undergoing surgery and/or radiotherapy develop lymphoedema; it may be related to some underlying susceptibility that is as yet undefined, and may be, possibly, genetic.13 Patients with lymphoedema often have subtle lymphatic anomalies in the contralateral limb.14
     
    Staging
    The International Society of Lymphology staging is the most commonly used system (Table 115), but it is somewhat flawed in that it is based only on physical findings. Some experts suggest incorporating measures of quality of life (QOL) to improve its usefulness.16 The classification offered by Campisi et al17 shows congruence with indocyanine green (ICG) dermal backflow patterns, which provides an indication of lymphatic function (Table 2).17 18 19 Bioimpedance spectroscopy uses electric current to measure the degree of tissue fluid retention and is useful in detecting early-stage lymphoedema including stage 0 disease.
     

    Table 1. International Society of Lymphology (ISL) staging 2003 with ratification in 2009 consensus document; stage 0 (latent lymphoedema) is a recent addition15
     

    Table 2. Campisi staging 201017
     
    The most commonly used method of objectively assessing the swelling is some form of conal measurement, such as measuring the circumference at 4 cm intervals, which is more practical than water displacement methods20 21 but is, supposedly, similar in accuracy.22 A perometer uses infrared rays to measure limb cross-sections at multiple intervals and, thus, determine the volume of the limb.23 The author has been exploring the idea of using Kinect (part of the Microsoft Xbox game system) as a three-dimensional scanner to gauge volume in collaboration with the Department of Computer Science and Engineering at The Chinese University of Hong Kong.
     
    Imaging
    In most cases, diagnosis can be made from the clinical history and examination, although some co-morbidities may confound the clinical picture. Lymphoedema can be assessed by common imaging techniques including computed tomography, magnetic resonance imaging, and duplex ultrasonography that can reliably show volume differences between the affected and normal limbs, the presence of subcutaneous fatty fibrosis, and help exclude proximal obstruction in late-onset unilateral lymphoedema which may be due to an occult visceral tumour.
     
    Lymphangiography involves direct cannulation of a lymphatic vessel on the dorsum of the foot or hand (under magnification). An oil-based contrast material is then injected through this vessel and serial plain radiographs of the limb are taken, allowing the lymphatics to be precisely delineated. Due to the potential of damage to the lymphatic vessels, it can theoretically worsen lymphoedema and, thus, is not commonly used.
     
    Radionuclide lymphoscintigraphy is the current standard investigation for evaluation of lymphatic function. Technetium-labelled colloid is injected into the web spaces of the toes or fingers, and drainage of the colloid from the injection site and the time taken to move proximally are recorded using a gamma camera. It is minimally invasive and enables making both qualitative and quantitative analyses. It does not require dye injection, a method that has been occasionally complicated by allergic skin reactions or anaphylaxis.
     
    Magnetic resonance lymphangiography may replace lymphoscintigraphy as it does not require direct injection of contrast and avoids the use of ionising radiation using a magnetic contrast medium to provide a sharp image of lymphatic vessels. In our early experience with this investigation, reproducibility has been a potential issue and needs further evaluation.
     
    Near-infrared fluorescence imaging with ICG is a promising emerging imaging modality that allows dynamic study of even small lymphatics in the skin.
     
    Treatment
    There is no cure for lymphoedema but it is easily managed with early recognition and therapy. Those who do not have treatment tend to worsen rapidly and advanced disease tends to be more difficult to treat than early disease. Patients are best treated in a specialised clinic24; inexperienced staff may delay treatment, or worse, advocate inappropriate treatments.
     
    The standard of care for lymphoedema is, what is commonly referred as, complex (or combined or complete) physical therapy (CPT, sometimes called complex decongestive therapy [CDT]), which is a staged combination of various components in two phases. The actual treatment regimen varies significantly by locality but, in general, 60% to 70% of compliant patients will respond to CPT when administered by specially trained therapists, with an average volume reduction of 50%.25 26 However, the time and effort involved, as well as the associated moderate discomfort, lead to decreased patient compliance, particularly in the long term.
    (1) Phase 1, also known as the ‘decongestive phase’, often requires the patient to be admitted as an in-patient as the regimen is intensive. Treated 5 days a week, it may take 4 to 6 weeks or more to have an effect on the limb volume, depending on the severity of the disease. A lack of effect may be due to improper technique, non-compliance, or incorrect diagnosis.
  • Manual lymph drainage (MLD) is not the same as massage; it is a much lighter, slow and specific action that aims to promote lymph movement in the superficial tissues away from the swelling.
  • Compression bandage is applied to reduce limb size but the bandages used are not of the standard variety—they are short and non-stretch, and applied with more pressure distally than proximally. This aims to move fluid out of the limb (hence the proximal portions need to be emptied with MLD first). It is only really effective within a CPT programme; the efficacy is reduced considerably in advanced disease.
  • Nail/skin care and exercises with bandaging/pressure garments as tight as tolerated to oppose the filtration pressure and provide counterforce to muscle contractions. Concerns that exercise may exacerbate or trigger lymphoedema have not been proven in studies.
  • (2) Phase 2, or the maintenance phase, can be out-patient–based or as self-care in selected trained patients. Patients should wear pressure garments during the day and compression bandages at night (alternatives include specifically designed garments such as Reid sleeves). Intermittent pneumatic compression machines are sometimes used but care needs to be taken to ensure that they have appropriate design, action, and pressures (usually 30-60 mm Hg though pressures of >45 mm Hg can cause lymphatics to rupture). Pneumatic compression is to be avoided in those with chronic non-pitting disease or those with active infection.
     
    Systematic reviews support the use of CDT and MLD. Conservative therapy can give good results but the effects are temporary without the maintenance and continued compression. In Hong Kong, the climate may reduce patient compliance with pressure garments. General care is also important; patients are advised to avoid even minor degrees of trauma such as venepuncture, insect bites, and acupuncture. The evidence for some of the following preventive practices is low but they are simple to follow.
  • Air travel: maintain hydration and mobilisation, whilst some experts suggest wearing pressure garments.
  • Avoid overuse of the affected limb.
  • Avoid trauma; take care when cutting nails, avoid needlestick/venepuncture, and blood pressure measurement. Patients can wear medical alert bracelets to inform others of the condition.
  • Avoid extremes of heat/cold and overtight clothing.
  •  
    Medications such as benzopyrenes and diuretics are not useful and will not be discussed any further. Oral penicillins such as amoxicillin and dicloxacillin should be started early when there is evidence of infection in a lymphoedematous limb and continued until the signs of inflammation resolve. There is borderline support for the use of prophylactic antibiotics in those who have more than two to three episodes of infection a year. Many modalities have been promoted for the non-surgical treatment of lymphoedema but at present only low-level laser therapy has approval from the US Food and Drug Administration (FDA), although evidence of its long-term effects is lacking—it generates low-intensity light (650-1000 nm) that is believed to promote lymph vessel regeneration and increase lymph pumping. The typical response is moderate and slow, and requires repeated treatments. Near-infrared light therapy aims to increase nitric oxide in the tissues to improve tissue repair and lymph regeneration but has not received FDA approval, whilst electrical stimulation is not recommended based on current evidence.27
     
    Surgery
    For reasons such as concerns of scarring or perceived lack of effect, surgery has often been regarded as a ‘last resort’, meaning that there is often a delay before patients are referred28 by which time they may only be suited for ‘salvage’ procedures. Whilst initial attempts at ‘physiological’ reconstruction were met with disappointing late results, improved understanding of the pathophysiology accompanied by improved microsurgical techniques have seen the development of newer techniques that seem to potentially offer better outcomes.
     
    Physiological/reconstructive techniques
    Physiological techniques aim to repair the damage and increase the return of lymph to the circulation, by reconnecting the lymphatic pathways above and beyond the obstruction, either directly (lymphatic to lymphatic) or indirectly via another segment such as veins/venules. Campisi et al17 29 30 have been a pioneer of these microsurgical techniques and classified them into ‘derivative’ techniques (essentially a lymphovenous bypass) and ‘reconstructive’ techniques (lymphatic-to-lymphatic connections).
     
    Lymphovenous anastomosis or bypass
    When interpreting the literature describing lymphovenous bypass, it is important to note the fundamental difference between early (lymphovenous) and newer (lymphaticovenular) techniques. The bypass concept was first described in 1963 in a rat model31 whilst Yamada32 and O’Brien et al33 were the first to use it in patients. O’Brien et al33 anastomosed lymphatics to veins measuring approximately 1 to 3 mm diameter and reported an average volume reduction of 44% in this series with 14 years’ follow-up. Campisi et al30 reported an average of 67% reduction in volume and 87% reduction in cellulitis in this large long-term series. Overall, 85% of patients were able to stop conservative management. However, one criticism of these retrospective studies was patient heterogeneity.
     
    However, Damstra et al34 found no improvement in patients with postmastectomy lymphoedema who were treated with lymphovenous anastomosis/bypass; a prospective study of 10 patients demonstrated only a 4.8% volume reduction at 3 months that was further reduced to 2% after 1 year, with minimal improvement in reported QOL. Boccardo et al35 36 performed lymphovenous bypass at the time of breast surgery with the aim of preventing lymphoedema—they anastomosed tributaries of the axillary vein to lymphatics with a patency rate of 95.6% but found no difference in limb volume compared with controls at up to 18 months’ follow-up.
     
    Lymphaticovenular anastomoses
    In Koshima et al’s opinion,37 38 39 there were inherent problems in lymphovenous anastomoses: (1) it is difficult to find larger lymphatic trunks, most are 0.8 mm or under in diameter; (2) reduced lymphatic pumping function; and (3) increased venous pressure and high rate of thrombosis due to blood at anastomotic site. According to these authors, lymphaticovenular anastomosis (LVA) offered better vessel size match compared with lymphovenous anastomoses. In 52 patients with an average of 2.1 LVAs per patient, there was a mean reduction of 41.8% in leg circumference at a mean follow-up of 14.5 months. Benefit could be demonstrated even in patients with stage III/IV disease, with recurrent lymphangitis and fibrosis. Koshima et al37 38 39 have also applied the technique in early disease for prophylaxis against development of fibrotic disease.
     
    The Tokyo group uses ICG fluorescent lymphography to stage the disease severity based on the amount of dermal backflow, and thus, select patients for surgery.40 41 Subdermal vessels are explored through small (<3 cm) skin incisions, aiming to use lymphatic vessels of approximately 0.2 mm in diameter with venules sized 0.5 mm or less on the basis that smaller veins will have lower pressures. Some call this ‘supermicrosurgery’ although the use of the term is rather arbitrary. The procedure can be performed under local anaesthesia with short hospital stay, which, in the author’s opinion, is one of the biggest advantages of this technique.
     
    The studies from Koshima et al’s unit37 38 39 have demonstrated an average volume reduction of 82.5% in those not responding to CPT. The Chang’s series42 demonstrated a 35% reduction of lymphoedema in breast cancer patients 1 year after LVA. Cormier et al43 reviewed eight studies and calculated a mean volume reduction of 54.0%. It is generally accepted that microsurgery will offer better results in early disease when patients have some healthy lymphatics before progressing to the fibrotic stage when damage is irreversible.
     
    Lymph node transfer
    Wongtrungkapun44 performed lymph node transfer in patients with filariasis; one to two groin nodes were partially decapsulated and anastomosed to the saphenous vein. Becker et al45 46 described the transfer of lymph nodes from the groin to the axilla in 24 patients with postmastectomy lymphoedema; 62.5% of the patients were said to be ‘cured’ and able to discontinue physiotherapy. Overall, in Becker et al’s experience,45 46 98% of the patients had some improvement; only 2% had repeat infections. Whilst 40% of patients with stage 1 or 2 lymphoedema had complete normalisation and did not require additional conservative therapy, those with stage 3 lymphoedema needed conservative therapy. Lin et al47 anastomosed superficial circumflex iliac nodes at the wrist to treat upper limb lymphoedema and reported a 55% reduction in volume at 56 months, with fewer episodes of cellulitis.
     
    Proponents of node surgery say that LVA or lymphatic-lymphatic anastomosis eventually become occluded (possibly due to the effect of interstitial pressure on low-pressure thin vessels) whilst lymph nodes are supposedly less susceptible. The lymphatic vessels are not actually anastomosed; it seems that the transplanted nodes develop new drainage pathways—proposed theories for this drainage include nodes acting as suction pumps whilst others suggest they are a source of VEGF-C that promotes lymphangiogenesis.
     
    Some experts have developed a procedure to transfer lymph nodes as part of a breast reconstruction procedure48; there may be several other benefits of such a procedure including release of scar tissue in the axilla and the provision of vascularised tissue as a lymphatic bridge.49 Isotope scans at 3 and 6 months demonstrated improved function in all but one patient.48 With this type of surgery, it is important to only harvest nodes of lower abdomen and not the leg; axillary reverse mapping may help to spare limb lymphatics.50
     
    Overall, good long-term functional data are lacking and some authors have had difficulty reproducing published results,25 possibly, due to the significant learning curve. Some have found 38% risk of complications, although mostly transient (eg lymphocele and hydrocele); however, some complications such as iatrogenic lymphoedema and chronic pain may be more persistent.51 They also found no volume difference after a median follow-up of 40 months with interval CDT and pressure garments. Viitanen et al52 found reduced lymphatic flow in the donor site/limb with lymphoscintigraphy without overt clinical lymphoedema in a small group of 10 patients.
     
    Preliminary results suggest that node transfer is more successful if performed sooner after nodal dissection surgery.45 53 Saaristo et al48 regard it as largely experimental but can be justified if performed at the time of breast reconstruction. Some surgeons have looked at animal models, combining node transfer with additional VEGF-C and -D,54 55 and this may offer a new type of treatment; however, the effect on lymphatic metastasis is unknown and deserves attention.
     
    Lymphatic grafting/transplantation
    Other less commonly used procedures include lymphatic grafting. Baumeister et al56 57 58 59 have significant experience in using this technique to treat secondary lymphoedema with an average volume reduction of 65%.60 61 In the lower limb, a long segment of lymphatic vessel is dissected out from the upper inner thigh and tunnelled over to affected contralateral leg for a lymphatic-lymphatic anastomosis. The efficacy in the upper limb where the lymphatic tissue is used as a free graft has also been demonstrated with significant improvement in over 90% of patients, with a mean volume reduction of 22% to 31% whilst scintigraphy shows continued graft function.62 63 64 The dissection of lymphatics is technically challenging; Campisi65 used veins instead of lymphatic vessels to bridge lymphatics.
     
    Some experts have used flaps for lymphatic bridging; for instance, the inclusion of random lymphatics in tissues such as the omentum66 or an axial flap such as the deltopectoral.67 The use of omentum has largely been abandoned as there is no evidence that it actually promotes lymph drainage, and the surgery is associated with high rates of morbidity. Similarly, enteromesenteric bridge operations and tube/thread implants should be avoided, based on current evidence.
     
    Debulking or excision
    Early attempts at treating lymphoedema involved techniques that were mainly based on debulking, that is, removing the oedematous tissue to restore form. The underlying lymphatic dysfunction is not addressed and may actually lead to further deterioration of the condition.
     
    Charles procedure
    The Charles procedure used in 1912 has been wrongly attributed to Sir Richard Charles for the treatment of leg lymphoedema by McIndoe.68 The surgeon had primarily treated scrotal swelling69 and had only described one unsuccessful case involving the lower limb. In simple terms, the lymphoedematous tissue is excised down to the fascial level and the defect is covered with skin grafts. The grafts can be taken from the excised tissue if it is not grossly abnormal70; otherwise, it has to be harvested from another site. Complications include graft breakdown/ulceration, scarring, and recurrence. The aesthetic results are rather poor and, thus, usually reserved for cases with severe skin changes.
     
    Homans-Miller procedure
    The Homans-Miller procedure, first used in 1936, is based on a multistage procedure initially described by Sistrunk71—skin flaps are elevated along one border of the limb, and after the deeper swollen tissue has been excised along with the fascia, the skin flaps are replaced.72 73 It is a traditional practice to avoid surgery at or below ankle, taking care to avoid damage to the common peroneal and sural nerves. A study with 14 years’ follow-up showed that this type of surgery was capable of long-lasting reduction in size in 80% of the treated patients, and associated with improved function and reduced cellulitis.73 It is the most common excisional surgery for lymphoedema. Others have refined this further by preserving the perforator vessels during flap elevation, allowing the flaps to be thinner (5 mm) and, potentially, for both sides to be treated in one stage.74
     
    The Thompson technique used in 1962 involves similar tissue resection whilst also harvesting a dermal flap75 that is buried into the muscle next to the neurovascular bundle, with the aim of creating a bridge for lymphatic return. However, long-term results were similar to excision alone and did not support the theoretical aim of a physiological effect and, thus, has largely been abandoned.
     
    The proven benefits of excisional surgery are often ignored, in part due to misconceptions of morbidity and complications; these were mostly related to early aggressive use of the technique leading to almost total abandonment of procedures in the mid-20th century. Recently Karri et al76 demonstrated that good results are possible with modern application of the Charles procedure that may also be combined with negative-pressure wound therapy.77 Similarly, surgeons have modified the Homans-Miller procedure25 and combined this with postoperative pressure garments to achieve good results.
     
    Liposuction
    Liposuction is a relatively recently described debulking technique based on the observation that there is adipose hypertrophy in lymphoedema. The fat accumulation may be related to altered lipid transport78 79 and corresponds to a non-pitting type of swelling that is not responsive to compression.
     
    O’Brien et al80 were one of the first surgeons to use liposuction to treat lymphoedema, and reported a volume reduction of 23%. Brorson et al81 used liposuction to treat patients with post–breast cancer lymphoedema that had been resistant to conservative therapy with reasonable effects that were confirmed with volume measurements, computed tomographic scans, and plethysmography. Liposuction for lymphoedema is similar but not the same as cosmetic liposuction. The technique has evolved in several ways, particularly, with the adoption of a tumescent technique with injection of adrenaline combined with use of a tourniquet that causes less bleeding—13% versus 25% without tourniquet.82 More recently, Schaverien et al83 used the Brorson technique (1997) and demonstrated a 101% reduction compared to normal limb at 1 year, and that was maintained at 5 years.
     
    The technique seems to be straightforward and safe, and produces consistent results84 85 86 with treated patients reporting improved QOL and suffering from decreased episodes of cellulitis. Preliminary results with laser Doppler scanning seem to support the theory that liposuction can reduce the lymphatic load87 without damaging lymph function.88 The National Institute for Health and Care Excellence89 suggests that liposuction may be considered in those patients with severe disease (massive incapacitating disease, unresponsive to conservative therapy). The morbidity may be less than traditional debulking surgeries and, thus, it can be regarded as the first choice of a debulking operation, if the skin is normal. Its main disadvantage is that patients are required to wear lifelong compression garments90; otherwise, the treated limb enlarges again; this may make the modality less suited in regions such as Hong Kong.
     
    Lymphoedema surgery in Hong Kong
    Since 1993, breast cancer has become the most common cancer in women in Hong Kong with an incidence of 79.4/100 000 in 2009.91 A local study presented at the 2010 Hospital Authority Convention found that 11.3% of patients had lymphoedema at 3 months after breast cancer surgery with axillary dissection.92 Mak et al93 found that previous infection-inflammation (odds ratio [OR]=4.49), surgery on the side of the dominant hand (OR=2.97), increased body mass index, and older age at the time of axillary dissection were significant risk factors for the development of moderate-to-severe lymphoedema in our local population.
     
    Despite the significant number of patients liable to suffer from breast cancer–related lymphoedema (BCRL), the general awareness of lymphoedema in Hong Kong is low among both health care professionals and patients. It is a common misconception that nothing can be done for the condition; thus, patients tend to be diagnosed late with symptomatic moderate-to-severe disease, and salvage-type surgical procedures are often the only therapeutic option.
     
    Medical costs for women with BCRL are substantially higher than for those without,94 with the difference mostly accounted for by the costs of treating infections. A local study95 found that instituting effective and standardised primary intervention for BCRL in the form of CDT/MLD would be beneficial to both patients and the health care institute, with savings of as much as HK$444 200 per year in a local hospital.
     
    Improvements in care for lymphoedema patients in Hong Kong require establishment of integrated treatment protocols which may include the following:
    (1) Education for caregivers and patients is important. Public/teaching hospitals should take the lead; in addition, support groups such as the Hong Kong Breast Cancer Foundation have a particularly important role. Medical staff with an interest in treating lymphoedema should keep themselves updated.
    (2) Establishment of multidisciplinary care units focusing around nurse-led clinics with formalised protocols following proven MLD/CDT programmes such as Foldi or Vodder that should be offered as a first option for lymphoedema patients. These clinics should be supported by medical staff who would offer medical advice, discuss surgical options, as well as treat complications when they occur.
    (3) Although CDT/MLD remains the mainstay of treatment for patients with lymphoedema, surgery may be considered in those patients who do not respond to conservative therapy. Newer microsurgical techniques (LVA and lymph node transfer) may be useful in early-stage disease though they have a significant learning curve and, therefore, should be undertaken only by experienced microsurgeons.
    (a) The author prefers offering LVA under local anaesthesia as a first option in stage I/II lymphoedema, with lymph node transfer for stage II/III disease.
    (b) Debulking surgery (Homans-Miller procedure with perforator preservation or Charles procedure with negative pressure dressings) may be considered in those with severe disabling swelling; the role of liposuction is likely to be minor in Hong Kong but can be offered to those willing to wear pressure garments continuously.
     
    A number of local surgeons have travelled to regional centres of excellence for training and our unit has organised courses in supermicrosurgery and lymph node transfer to encourage the uptake of these techniques among other surgeons. Lymphatic venous anastomosis has been performed in Hong Kong since 2012 (Figs 1 and 2) and the preliminary results are encouraging, with patients often describing early relief, particularly from symptoms of ‘tightness’. Given the short period of experience and small number of patients, it is too early to comment on local results; however, there is no reason to suggest that the results would not be comparable with international findings in the long term.
     

    Figure 1. A patient undergoing lymphaticovenular anastomosis procedure under local anaesthesia
     

    Figure 2. A completed lymphaticovenular anastomosis
     
    References
    1. de Jong MA, Oldenborg S, Bing Oei S, et al. Reirradiation and hyperthermia for radiation-associated sarcoma. Cancer 2012;118:180-7. CrossRef
    2. Karkkainen MJ, Ferrell RE, Lawrence EC, et al. Missense mutations interfere with VEGFR-3 signalling in primary lymphoedema. Nat Genet 2000;25:153-9. CrossRef
    3. Irrthum A, Karkkainen MJ, Devriendt K, Alitalo K, Vikkula M. Congenital hereditary lymphoedema caused by a mutation that inactivates VEGFR3 thyrosine kinase. Am J Hum Genet 2000;67:295-301. CrossRef
    4. Cederberg A, Grønning LM, Ahrén B, Taskén K, Carlsson P, Enerbäck S. FOXC2 is a winged helix gene that counteracts obesity, hypertriglyceridemia, and diet-induced insulin resistance. Cell 2001;106:563-73. CrossRef
    5. Yildirim-Toruner C, Subramanian K, El Manjra L, Chen E, Goldstein S, Vitale E. A novel frameshift mutation of FOXC2 gene in a family with hereditary lymphoedema-distichiasis syndrome associated with renal disease and diabetes mellitus. Am J Med Genet A 2004;131:281-6. CrossRef
    6. Warren AG, Brorson H, Borud LJ, Slavin SA. Lymphedema: a comprehensive review. Ann Plast Surg 2007;59:464-72. CrossRef
    7. Petrek JA, Senie RT, Peters M, Rosen PP. Lymphedema in a cohort of breast carcinoma survivors 20 years after diagnosis. Cancer 2001;92:1368-77. CrossRef
    8. Langer I, Guller U, Berclaz G, et al. Morbidity of sentinel lymph node biopsy (SLN) alone versus SLN and completion axillary lymph node dissection after breast cancer surgery: a prospective Swiss multicenter study on 659 patients. Ann Surg 2007;245:452-61. CrossRef
    9. Lucci A, McCall LM, Beitsch PD, et al. Surgical complications associated with sentinel lymph node dissection (SLND) plus axillary lymph node dissection compared with SLND alone in the American College of Surgeons Oncology Group Trial Z0011. J Clin Oncol 2007;25:3657-63. CrossRef
    10. Veronesi U, Paganelli G, Viale G, et al. A randomized comparison of sentinel-node biopsy with routine axillary dissection in breast cancer. N Engl J Med 2003;349:546-53. CrossRef
    11. Wilke LG, McCall LM, Posther KE, et al. Surgical complications associated with sentinel lymph node biopsy: results from a prospective international cooperative group trial. Ann Surg Oncol 2006;13:491-500. CrossRef
    12. Tammela T, Alitalo K. Lymphangiogenesis: molecular mechanisms and future promise. Cell 2010;140:460-76. CrossRef
    13. Newman B, Lose F, Kedda MA, et al. Possible genetic predisposition to lymphedema after breast cancer. Lymphat Res Biol 2012;10:2-13. CrossRef
    14. Aldrich MB, Guilliod R, Fife CE, et al. Lymphatic abnormalities in the normal contralateral arms of subjects with breast cancer–related lymphedema as assessed by near-infrared fluorescent imaging. Biomed Opt Express 2012;3:1256-65. CrossRef
    15. International Society of Lymphology. The diagnosis and treatment of peripheral lymphedema. 2009 Concensus Document of the International Society of Lymphology. Lymphology 2009;42:51-60.
    16. Lee BB, Laredo J, Neville RF. Combined clinical and laboratory (lymphoscintigraphic) staging. In: Lee B, Bergan J, Rockson SG, editors. Lymphedema: a concise compendium of theory and practice. London: Springer; 2011: 97-104. CrossRef
    17. Campisi C, Bellini C, Campisi C, Accogli S, Bonioli E, Boccardo F. Microsurgery for lymphoedema: clinical research and long-term results. Microsurgery 2010;30:256-60.
    18. Yamamoto T, Narushima M, Doi K, et al. Characteristic indocyanine green lymphography findings in lower extremity lymphedema: the generation of a novel lymphedema severity staging system using dermal backflow patterns. Plast Reconstr Surg 2011;127:1979-86. CrossRef
    19. Yamamoto T, Matsuda N, Doi K, et al. The earliest finding of indocyanine green lymphography in asymptomatic limbs of lower extremity lymphedema patients secondary to cancer treatment: the modified dermal backflow stage and concept of subclinical lymphedema. Plast Reconstr Surg 2011;128:314e-321e. CrossRef
    20. Stanton A, Modi S, Mellor R, Levick R, Mortimer P. Diagnosing breast cancer–related lymphoedema in the arm. J Lymphoedema 2006;1:12-5.
    21. Sander AP, Hajer NM, Hemenway K, Miller AC. Upper-extremity volume measurements in women with lymphedema: a comparison of measurements obtained via water displacement with geometrically determined volume. Phys Ther 2002;82:1201-12.
    22. Taylor R, Jayasinghe UW, Koelmeyer L, Ung O, Boyages J. Reliability and validity of arm volume measurements for assessment of lymphedema. Phys Ther 2006;86:205-14.
    23. Stanton AW, Northfield JW, Holroyd B, Mortimer PS, Levick JR. Validation of an optoelectronic limb volumeter (Perometer). Lymphology 1997;30:77-97.
    24. Garfein ES, Borud LJ, Warren AG, Slavin SA. Learning from a lymphedema clinic: an algorithm for the management of localized swelling. Plast Reconstr Surg 2008;121:521-8. CrossRef
    25. Lee BB, Kim YW, Kim DI, Hwang JH, Laredo J, Neville R. Supplemental surgical treatment to end stage (stage IV-V) of chronic lymphedema. Int Angiol 2008;27:389-95.
    26. Ko DS, Lerner R, Klose G, Cosimi AB. Effective treatment of lymphedema of the extremities. Arch Surg 1998;133:452-8. CrossRef
    27. Moseley AL, Carati CJ, Piller NB. A systematic review of common conservative therapies for arm lymphoedema secondary to breast cancer treatment. Ann Oncol 2007;18:639-46. CrossRef
    28. Lee BB. Contemporary issues in management of chronic lymphedema: personal reflection on an experience with 1065 patients. Lymphology 2005;38:28-31.
    29. Campisi C, Davini D, Bellini C, et al. Lymphatic microsurgery for the treatment of lymphoedema. Microsurgery 2006;26:65-9. CrossRef
    30. Campisi C, Boccardo F, Zilli A, Macciò A, Napoli F. Long-term results after lymphatic-venous anastomoses for the treatment of obstructive lymphoedema. Microsurgery 2001;21:135-9. CrossRef
    31. Laine JB, Howard JM. Experimental lymphatico-venous anastomosis. Surg Forum 1963;14:111-2.
    32. Yamada Y. The studies on lymphatic venous anastomosis in lymphoedema. Nagoya J Med Sci 1969;32:1-21.
    33. O’Brien BM, Sykes P, Threlfall GN, Browning FS. Microlymphaticovenous anastomoses for obstructive lymphoedema. Plast Reconstr Surg 1977;60:197-211. CrossRef
    34. Damstra RJ, Voesten HG, van Schelven WD, van der Lei B. Lymphatic venous anastomosis (LVA) for treatment of secondary arm lymphedema. A prospective study of 11 LVA procedures in 10 patients with breast cancer related lymphedema and a critical review of the literature. Breast Cancer Res Treat 2009;113:199-206. CrossRef
    35. Boccardo F, Casabona F, De Cian F, et al. Lymphedema microsurgical preventive healing approach: a new technique for primary prevention of arm lymphedema after mastectomy. Ann Surg Oncol 2009;16:703-8. CrossRef
    36. Boccardo FM, Casabona F, Friedman D, et al. Surgical prevention of arm lymphedema after breast cancer treatment. Ann Surg Oncol 2011;18:2500-5. CrossRef
    37. Koshima I, Nanba Y, Tsutsui T, Takahashi Y, Itoh S. Long-term follow-up after lymphaticovenular anastomosis for lymphoedema in the leg. J Reconstr Microsurg 2003;19:209-15. CrossRef
    38. Koshima I, Nanba Y, Tsutsui T, Tahahashi Y, Itoh S, Fujitsu M. Minimal invasive lymphaticovenular anastomosis under local anesthesia for leg lymphedema: is it effective for stage III and IV? Ann Plast Surg 2004;53:261-6. CrossRef
    39. Koshima I, Kawada S, Moriguchi T, Kajiwara Y. Ultrastructural observations of lymphatic vessels in lymphedema in human extremities. Plast Reconstr Surg 1996;97:397-405; discussion 406-7. CrossRef
    40. Mihara M, Uchida G, Hara H, et al. Lymphaticovenous anastomosis for facial lymphoedema after multiple courses of therapy for head-and-neck cancer. J Plast Reconstr Aesthet Surg 2011;64:1221-5. CrossRef
    41. Furukawa H, Osawa M, Saito A, et al. Microsurgical lymphaticovenous implantation targeting dermal lymphatic backflow using indocyanine green fluorescence lymphography in the treatment of postmastectomy lymphedema. Plast Reconstr Surg 2011;127:1804-11. CrossRef
    42. Chang DW. Lymphaticovenular bypass for lymphedema management in breast cancer patients: a prospective study. Plast Reconstr Surg 2010;126:752-8. CrossRef
    43. Cormier JN, Rourke L, Crosby M, Chang D, Armer J. The surgical treatment of lymphedema: a systematic review of the contemporary literature (2004-2010). Ann Surg Oncol 2012;19:642-51. CrossRef
    44. Wongtrungkapun R. Microsurgical lymphonodovenous implantation for chronic lymphedema. J Med Assoc Thai 2004;87:877-82.
    45. Becker C, Assouad J, Riquet M, Hidden G. Postmastectomy lymphedema: long-term results following microsurgical lymph node transplantation. Ann Sur 2006;243:313-5. CrossRef
    46. Becker C, Vasile JV, Levine JL, et al. Microlymphatic surgery for the treatment of iatrogenic lymphedema. Clin Plast Surg 2012;39:385-98. CrossRef
    47. Lin CH, Ali R, Chen SC, et al. Vascularized groin lymph node transfer using the wrist as a recipient site for management of postmastectomy upper extremity lymphedema. Plast Reconstr Surg 2009;123:1265-75. CrossRef
    48. Saaristo AM, Niemi TS, Viitanen TP, Tervala TV, Hartiala P, Suominen EA. Microvascular breast reconstruction and lymph node transfer for postmastectomy lymphedema patients. Ann Surg 2012;255:468-73. CrossRef
    49. Card A, Crosby MA, Liu J, Lindstrom WA, Lucci A, Chang DW. Reduced incidence of breast cancer–related lymphedema following mastectomy and breast reconstruction versus mastectomy alone. Plast Reconstr Surg 2012;130:1169-78. CrossRef
    50. Klimberg VS. A new concept toward the prevention of lymphedema: axillary reverse mapping. J Surg Oncol 2008;97:563-4. CrossRef
    51. Vignes S, Blanchard M, Yannoutsos A, Arrault M. Complications of autologous lymph-node transplantation for limb lymphoedema. Eur J Vasc Endovasc Surg 2013;45:516-20. CrossRef
    52. Viitanen TP, Mäki MT, Seppänen MP, Suominen EA, Saaristo AM. Donor-site lymphatic function after microvascular lymph node transfer. Plast Reconstr Surg 2012;130:1246-53. CrossRef
    53. Slavin SA, Van den Abbeele AD, Losken A, Swartz MA, Jain RK. Return of lymphatic function after flap transfer for acute lymphedema. Ann Surg 1999;229:421-7. CrossRef
    54. Tammela T, Saaristo A, Holopainen T, et al. Therapeutic differentiation and maturation of lymphatic vessels after lymph node dissection and transplantation. Nat Med 2007;13:1458-66. CrossRef
    55. Lähteenvuo M, Honkonen K, Tervala T, et al. Growth factor therapy and autologous lymph node transfer in lymphedema. Circulation 2011;123:613-20. CrossRef
    56. Baumeister RG, Seifert J, Hahn D. Autotransplantation of lymphatic vessels. Lancet 1981;1:147. CrossRef
    57. Baumeister RG, Seifert J, Wiebecke B, Hahn D. Experimental basis and first application of clinical lymph vessel transplantation of secondary lymphedema. World J Surg 1981;5:401-7. CrossRef
    58. Baumeister RG. Microsurgery of the lymphatic system [in German]. Chirurg 1983;54:374-8.
    59. Baumeister RG, Siuda S. Treatment of lymphedemas by microsurgical lymphatic grafting: what is proved? Plast Reconstr Surg 1990;85:64-74; discussion 75-6. CrossRef
    60. Baumeister RG, Siuda H, Bohmert H, Moser E. A microsurgical method for reconstruction of interrupted lymphatic pathways: autologous lymph-vessel transplantation for treatment of lymphedemas. Scand J Plast Reconstr Surg 1986;20:141-6. CrossRef
    61. Kleinhans E, Baumeister RG, Hahn D, Siuda S, Büll U, Moser E. Evaluation of transport kinetics in lymphoscintigraphy: follow-up study in patients with transplanted lymphatic vessels. Eur J Nucl Med 1985;10:349-52. CrossRef
    62. Weiss M, Baumeister RG, Hahn K. Post-therapeutic lymphedema: scintigraphy before and after autologous lymph vessel transplantation: 8 years of long-term follow-up. Clin Nucl Med 2002;27:788-92. CrossRef
    63. Weiss M, Baumeister RG, Hahn K. Dynamic lymph flow imaging in patients with oedema of the lower limb for evaluation of the functional outcome after autologous lymph vessel transplantation: an 8-year follow-up study. Eur J Nucl Med Mol Imaging 2003;30:202-6. CrossRef
    64. Baumeister RG, Frick A. The microsurgical lymph vessel transplantation [in German]. Handchir Mikrochir Plast Chir 2003;35:202-9.
    65. Campisi C. Use of autologous interposition vein graft in management of lymphedema: preliminary experimental and clinical observations. Lymphology 1991;24:71-6.
    66. Goldsmith HS, De los Santos R. Omental transposition in primary lymphoedema. Surg Gynecol Obstet 1967;125:607-10.
    67. Withey S, Pracy P, Wood S, Rhys-Evans P. The use of a lymphatic bridge in the management of head and neck lymphoedema. Br J Plast Surg 2001;54:716-9. CrossRef
    68. Dumanian GA, Futrell JW. The Charles procedure: misquoted and misunderstood since 1950. Plast Reconstr Surg 1996;98:1258-63. CrossRef
    69. Charles R. Elephantiasis scroti. In: Latham A, English TC, editors. A system of treatment. London: Churchill; 1912.
    70. Gibson T, Tough JS. A simplified one-stage operation for the correction of lymphedema of the leg. AMA Arch Surg 1955;71:809-17. CrossRef
    71. Sistrunk WE. Further experience with the Kondoleon operation for elephantiasis. JAMA 1918;71:800-6. CrossRef
    72. Homans J. The treatment of elephantiasis of the legs. A preliminary report. N Engl J Med 1936;215:1099-104. CrossRef
    73. Miller TA, Wyatt LE, Rudkin GH. Staged skin and subcutaneous excision for lymphedema: a favorable report of long-term results. Plast Reconstr Surg 1998;102:1486-98; discussion 1499-501. CrossRef
    74. Salgado CJ, Mardini S, Spanio S, Tang WR, Sassu P, Chen HC. Radical reduction of lymphedema with preservation of perforators. Ann Plast Surg 2007;59:173-9. CrossRef
    75. Thompson N. Surgical treatment of chronic lymphoedema of the lower limb. With preliminary report of new operation. Br Med J 1962;2:1566-73. CrossRef
    76. Karri V, Yang MC, Lee IJ, et al. Optimizing outcome of Charles procedure for chronic lower extremity lymphoedema. Ann Plast Surg 2011;66:393-402. CrossRef
    77. van der Walt JC, Perks TJ, Zeeman BJ, Bruce-Chwatt AJ, Graewe FR. Modified Charles procedure using negative pressure dressings for primary lymphedema: a functional assessment. Ann Plast Surg 2009;62:669-75. CrossRef
    78. Brorson H. Surgical treatment of postmastectomy lymphedema—liposuction. In: Lee BB, Bergan J, Rockson SG, editors. Lymphedema: a concise compendium of theory and practice. London: Springer; 2011: 409-18. CrossRef
    79. Dixon JB. Lymphatic lipid transport: sewer or subway? Trends Endocrinol Metab 2010;21:480-7. CrossRef
    80. O’Brien BM, Khazanchi RK, Kumar PA, Dvir E, Pederson WC. Liposuction in the treatment of lymphoedema; a preliminary report. Br J Plast Surg 1989;42:530-3. CrossRef
    81. Brorson H, Ohlin K, Svensso B. The facts about liposuction as a treatment for lymphoedema. J Lymphoedema 2008;3:38-47.
    82. Wojnikow S, Malm J, Brorson H. Use of tourniquet with and without adrenaline reduces blood loss during liposuction for lymphoedema of the arm. Scand J Plast Reconstr Surg Hand Surg 2007;41:243-9. CrossRef
    83. Schaverien MV, Munro KJ, Baker PA, Munnoch DA. Liposuction for chronic lymphoedema of the upper limb: 5 years of experience. J Plast Reconstr Aesthet Surg 2012;65:935-42. CrossRef
    84. Brorson H. Liposuction in arm lymphoedema treatment. Scand J Surg 2003;92:287-95.
    85. Brorson H, Svensson H. Complete reduction of lymphoedema of the arm by liposuction after breast cancer. Scand J Plast Reconstr Surg Hand Surg 1997;31:137-43. CrossRef
    86. Brorson H, Svensson H. Liposuction combined with controlled compression therapy reduces arm lymphoedema more effectively than controlled compression therapy alone. Plast Reconstr Surg 1998;102:1058-67; discussion 1068. CrossRef
    87. Brorson H. Liposuction gives complete reduction of chronic large arm lymphedema after breast cancer. Acta Oncol 2000;39:407-20. CrossRef
    88. Brorson H, Svensson H, Norrgren K, Thorsson O. Liposuction reduces arm lymphoedema without significantly altering the already impaired lymph transport. Lymphology 1998;31:156-72.
    89. National Institute for Health and Clinical Excellence. Liposuction for chronic lymphoedema, February 2008. Available from: http://www.nice.org.uk/guidance/ipg251/resources/guidance-liposuction-for-chronic-lymphoedema-pdf. Accessed Jan 2014.
    90. Brorson H, Ohlin K, Olsson G, Långström G, Wiklund I, Svensson H. Quality of life following liposuction and conservative treatment of arm lymphoedema. Lymphology 2006;39:8-25.
    91. Hong Kong Cancer Registry. Available from: http://www3.ha.org.hk/cancereg/statistics.html. Accessed Jan 2014.
    92. Leung SY. A prospective cohort study on physiotherapy service to identify service gaps for post-operative breast cancer patients. Proceedings of the Hospital Authority Convention 2010; 2010 May 10-11; Hong Kong.
    93. Mak SS, Yeo W, Lee YM, et al. Predictors of lymphedema in patients with breast cancer undergoing axillary lymph node dissection in Hong Kong. Nurs Res 2008;57:416-25. CrossRef
    94. Shih YC, Xu Y, Cormier JN, et al. Incidence, treatment costs, and complications of lymphedema after breast cancer among women of working age: a 2-year follow-up study. J Clin Oncol 2009;27:2007-14. CrossRef
    95. Tang KS. A clinical guideline for management of lymphoedema using nurse-led manual lymphatic drainage therapy. Hong Kong: The University of Hong Kong; 2013.