Establishing a clinical phenotype for cachexia in end stage kidney disease – study protocol

The aim of this study is to determine the clinical phenotype of cachexia specific to individuals with ESKD.

The objectives of the study are to:

This is a longitudinal study which will run over 2 years. All patients with ESKD who receive  haemodialysis and attend a single Regional Nephrology Unit within the United Kingdom, will be eligible for inclusion into this study to determine if they experience (and to what degree) the known characteristics associated with cachexia (Table 1). Key factors, such as: primary renal disease; comorbidities (eg Charlson Comorbidity Index); recent hospitalisation (within 3 months); drugs (particularly steroids, erythropoietin stimulating agents and immunosuppressive agents); urea clearance; residual renal function; and dialysis vintage will also be recorded.

The recruiting regional nephrology unit provides care to approximately 250 chronic haemodialysis patients per annum. Recruitment will take place over 7 months, with an expected recruitment rate of 145 patients. Suitable patients will be identified via inpatient wards and outpatient units at the recruiting regional nephrology unit. Inclusion/exclusion criteria are outlined below. Once recruited patients will be monitored for 1 year (or time to death if < 1 year).

This study is ‘ongoing’ and is currently carrying out recruitment. All measures will be assessed at baseline and will be repeated every 2 months for 12 months or until death (Fig. 1). Patients will be asked to complete validated tools to determine fatigue, quality of life and anorexia. We will measure: weight; lean muscle mass (bioelectrical impedance analysed via vector analysis, mid upper arm muscle circumference - from measures of mid arm circumference and tricep skin fold thickness); muscle strength (hand held dynamometer); and interrogate routine monthly clinical blood tests for abnormal biochemistry (Table 1).

Any dialysis unit is a busy clinical environment and patients attending for haemodialysis three times per week do not want to be delayed in entering or leaving the dialysis unit. Thus it is imperative that the study does not over burden the clinical area or participants. We have worked closely with the clinical team to plan how we will collect data from patients so as not to interrupt the clinical flow or delay the patient unnecessarily when they have completed a dialysis session. Where possible routinely collected clinical data will be used e.g. pre- and post-dialysis blood samples, weight pre- and post-dialysis. We will ask patients (or help patients) to complete the tools measuring quality of life, fatigue and anorexia while on dialysis and we will then measure hand grip strength, mid upper arm circumference, skin fold thickness and complete Bioelectrical Impedance Analysis (BIA) immediately post-dialysis. It is expected these assessments with take 15 min to complete. Inclusion criteria requires a confirmed diagnosis of stage 5 CKD (estimated GFR <15mL/min/1.73m²) receiving dialysis, over the age of 18 and able to read and write.  Exclusion criteria involves those who are Stage 1-4 CKD, Stage 5 CKD who are not receiving haemodialysis, lacking capacity to give consent, under the age of 18 or non-english speaking. 

Participants will be advised of the voluntary nature of their inclusion in this research and can withdraw from follow-up at their request. As stated within the information sheet, for any patient who does withdraw, we will use collected data up to the withdrawal point (with the participant’s consent) and this may be used for analysis. We will record all reasons for patient withdrawal during the data collection of this study.

Within this study we will use the World Health Organization’s (WHO) definition of quality of life which is “individuals’ perception of their position in life in the context of the culture and value systems in which they live and in relation to their goals, expectations, standards and concerns”. The tool we will use to measure quality of life will be the Kidney Disease Quality of Life instrument Short Form- KDQOL-SF36 [12]. This tool has been selected as it has confirmed reliability and validity in measuring quality of life in an end stage renal disease population [2]. The FACIT-fatigue scale, will be used to measure fatigue. It has proven psychometrics and is time efficient to complete and suitable to use for the purposes proposed [4]. We will also measure anorexia using the Functional Assessment of Anorexia/Cachexia Therapy (FAACT) questionnaire which is a validated appetite assessment tool for patients receiving dialysis [15].

This is a small scale longitudinal study. The data collected will provide information on ESKD participants who do and do not exhibit known characteristics of cachexia. The goal is to recruit and follow a population of ESKD patients who are receiving haemodialysis for 1 year (or until death) to identify those who exhibit characteristics of cachexia, to what degree, and to compare them to those without cachexia. The findings from this study will inform a disease-specific definition for cachexia in the ESKD population. Summary statistics will be calculated regarding the characteristics of participants. Analysis will be done comparing combinations of criteria (Table 1) and their outcomes using multivariate logistic regression and compare time to death with an age and sex matched parallel cohort of ESKD participants receiving haemodialysis without weight loss and associated characteristics of cachexia. Analysis of raw bioelectrical impedance data will be undertaken to estimate nutritional status and presence of a cachexia phenotype. Conversion of impedance readings into fat free mass, raw analysis by bioelectrical impedance vector analysis and bioelectrical impedance phase angle assessment will be undertaken. The longitudinal data collected will be analysed to develop a model potentially based on mortality and which factors best associate with this. This will then be prospectively tested in future studies.

This study will be conducted in compliance with Good Clinical Practice Guidelines. Governance approval for the study has been obtained from the host institution and the Office of Research Ethics Committees Northern Ireland (ORECNI) approval has been gained in preparation for the study commencing (REC reference: 16/NI/0233). Fundamental principles of good practice including the provision of user friendly information sheets, informed consent, voluntary participation, confidentiality and data protection procedures will be applied as a minimum standard within this study. Professional gatekeepers will establish primary contact with potential participates about this study. It is acknowledged that participants may find completion of questionnaires distressing and a distress protocol has been designed to manage such distress. The study is designed so that it will not be over burdensome for participants. For example, the validated tools can be completed whilst on dialysis, we will access routine clinical information were we can (bloods and weight post dialysis). All measures of lean muscle mass will be collected post-dialysis and we will adhere to the manualized techniques for the instruments used.

Members of the research team are also members of the Northern Ireland Kidney Patient Association (NIKPA) (JR, HN, PM, JS), Northern Ireland Kidney Research Fund (PM, JS) and the British Kidney Patient Association (HN). The NIKPA hold monthly meetings and are in regular e-mail contact with members. The programme of renal cachexia work has been discussed since inception with the NIKPA and had been presented to their members, by the lead researcher (JR), facilitated by an NIKPA member. The Northern Ireland Kidney Research Fund fully support the planned research and members have been able to discuss the proposal with the study team and have made practical suggestions to improve its design, such as the use of the term cachexia in patient facing material. Members of these organisations have actively contributed to the study proposal and have been influential in shaping its scope. Our patient and public involvement organisations were represented at our September 2014 “Defining Renal Cachexia” workshop led by the authors. A British Kidney Patient Association representative was a speaker at this workshop. Two NIKPA members were attendees and actively engaged with workshop discussions.