Ruth Erskine scite author profile

Ruth Erskine

4Publications

54Citation Statements Received

51Citation Statements Given

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St. Mary's Hospital, St Mary's Hospital

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Adolescent boys with sickle cell disease: A qualitative study

Erskine

2011

Clin Child Psychol Psychiatry

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Sickle cell disease is a recessively inherited blood disorder associated primarily with black communities within the UK. This study investigated the experiences of adolescent boys with this condition. Eight participants were interviewed and their responses analysed using Interpretative Phenomenological Analysis. The emergent themes were watchfulness, holding onto normality, and connecting and disengaging. This analysis illustrated connections between physical symptoms, emotional responses and the development concerns of this participant group. The findings have implications for the nature and style of the delivery of health care services.

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Exposing racism, exploring race

Erskine¹

2002

Journal of Family Therapy

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Therapeutic practice cannot be neutral in the understanding of race. Living in a society that discriminates between the races affects the thoughts, feelings and experiences of all. By its emphasis on context, systemic practice offers a way to consider how social inequalities are reflected in personal dilemmas without perpetuating myths of black inferiority. A case example is used to illustrate a systemic approach which takes account of racial differences. The orientation is towards exposing the manifestations and effects of racism as well as exploring associated issues of racial identity. These ideas are linked to theoretical and research studies in related fields. A therapeutic stance of exposing racism and exploring race fits with current developments in family therapy and can be applied to the therapist's use of self.

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Bone Marrow Transplantation Arrests Cerebrovascular Disease Progression and Improves Psychometric Outcomes in Children with Sickle Cell Disease

Bhatnagar

Erskine

O'Boyle

et al. 2011

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11 Stem cell transplantation (SCT) is currently the only curative option for sickle cell disease. Cerebrovascular disease (CVD) is one of the main indications to undertake this procedure as even with best conventional approaches there is a significant risk of recurrence or progression and there is evidence that SCT arrests disease progression, though more detailed study of outcomes is awaited. Early studies of SCT in sickle cell disease showed a high rate of neurological complications that led to the optimization of protocols. We conducted a retrospective analysis of related SCT in children with severe SCD between 2001 and 2010 at our institution to study the effect of transplantation. 20 patients (11 male, 9 female) received a BMT for sickle CVD (n=11) or recurrent vaso-occlusive crises (n=9). One patient with CVD was a second procedure following primary graft failure in a previous sibling transplant. CVD was investigated with clinical history and examination, transcranial Doppler ultrasound, magnetic resonance imaging/magnetic resonance angiography and psychometric testing using WISC-IV: 7 patients had no evidence of CVD, 5 had silent infarcts, 6 ischaemic stroke and 2 Moya-Moya disease. The median age at transplantation was 136 months (range 34 – 210 months). Donor source was HLA-matched siblings in 18 patients, one 9/10 mismatched sibling and HLA-matched relative in another. Bone marrow was used in all (n=19) but one patient who received combined bone marrow and umbilical cord. All patients (n=18) but two received conditioning with oral busulfan 14 mg/kg, cyclophosphamide 200 mg/kg and alemtuzumab 0.3 mg/kg; 1 patient received fludarabine 160 mg/m2, treosulfan 42 mg/m2, thiotepa 10mg/kg and ATG (Thymoglobulin) 11.25 mg/kg and 1 patient received oral busulfan 16mg/kg, cyclophosphamide 200 mg/kg and antilymphocyte globulin (45 mg/kg). GvHD prophylaxis was provided with ciclosporin and short course methotrexate (n=18), ciclosporin and MMF (n=1) and ciclosporin alone (n=1). Mean cell dose was 3.70 × 108 TNC/kg (range 1.45 – 6.16 × 108 TNC/kg). Neutrophil engrafment (>0.5 × 109/L) occurred at a median of 19.5 days (range 12 – 28 days) and platelet engrafment (>50 × 109/L) at median of 26 days (range 21 – 52 days). The median follow up is 974 days (range 270 – 3622 days). 18 patients achieved stable donor haemopoiesis, one patient suffered secondary graft failure due to Parvovirus B19 infection and one patient died on day +21 post-transplant due to sepsis and multi-organ failure. No significant sickle related neurological events occurred during these transplants. All 18 patients with long-term engraftment achieved radiological stabilization of the underlying CVD. Imaging performed at least 12 months post SCT showed no further changes from pre-transplant images. There were no clinical neurological events after SCT. Psychometric testing demonstrated improvements in all areas in patients transplanted for silent infarcts, particularly those affecting processing speed. In summary, SCT appears safe even in patients with severe CVD, arrests further progression and shows functional improvement. Disclosures: No relevant conflicts of interest to declare.

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Emergency medical care.

Erskine¹,

Fleming²,

Morrison³

et al. 1976

BMJ

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Ruth Erskine

Adolescent boys with sickle cell disease: A qualitative study

Exposing racism, exploring race

Bone Marrow Transplantation Arrests Cerebrovascular Disease Progression and Improves Psychometric Outcomes in Children with Sickle Cell Disease

Emergency medical care.

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