C Ridaura-Sanz scite author profile

C Ridaura-Sanz

5Publications

96Citation Statements Received

44Citation Statements Given

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Scleroderma ‘en coup de sabre’ and progressive facial hemiatrophy. Is it possible to differentiate them?

Orozco‐Covarrubias¹,

Guzmán-Meza²,

Ridaura-Sanz³

et al. 2002

Acad Dermatol Venereol

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The aim was to be able to evaluate the diagnosis of two diseases by a consensus of clinical opinion used in the Department of Dermatology of the National Institute of Paediatrics in Mexico City. To differentiate between scleroderma 'en coup de sabre' (SCS) and progressive facial hemiatrophy (PFH), colour slides of 13 patients diagnosed as SCS and nine as PFH were examined by two dermatologists and microscopic slides by two pathologists. In both cases, the slides were randomly presented and no clinical information was given. The clinical and histopathological findings were statistically compared with two-tailed tests and alpha = 0.05. Kappa coefficients were obtained to evaluate the concordance between dermatologists, pathologists, and in terms of the consensus diagnosis. The usefulness of photographic assessment is limited by the inability to palpate the consistency of lesions. The most important clinical feature that differentiated both conditions was cutaneous sclerosis present in eight of 13 patients with SCS and in none of the PFH patients (P < 0.005). Other clinical features more frequently found in SCS were cutaneous hyperpigmentation and alopecia. The more frequent clinical features in PFH were total hemifacial involvement and ocular changes. Statistically significant histopathological features were: connective tissue fibrosis present in all cases with SCS and two of nine patients with PFH (P < 0.0002); adnexal atrophy present in 11 of 13 patients with SCS, and in three of nine with PFH (P < 0.02), and mononuclear cell infiltrates in all patients with SCS cf. six with PFH (P < 0.05). Our results suggest that in most cases it is possible to differentiate SCS from PFH based on clinicopathological findings.

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Desmoplastic hairless hypopigmented naevus: a variant of giant congenital melanocytic naevus

Orozco‐Covarrubias¹,

Ridaura-Sanz²,

Durán‐McKinster³

et al. 2003

Br J Dermatol

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Desmoplasia has been described in melanoma and Spitz naevus but not in giant congenital melanocytic naevus (GCMN). In melanoma desmoplasia is associated with a better survival. Four paediatric patients with hard, ligneous, progressively hypopigmented and alopecic GCMN were seen among 143 cases of GCMN at the Department of Dermatology of the National Institute of Paediatrics, Mexico City. Clinically, induration was progressive in three patients and regressive in one. Pigmentation was regressive in all. Histopathologically, all four patients showed intense dermal fibrosis, scarce naevus cells, and hypotrophic or absent hair follicles. Follow-up and serial biopsies in three patients documented the progressive nature of fibrosis and naevus cell depletion. No evidence of malignant transformation was found. Naevus cell depletion resulted in pigment loss and may have reduced the risk of malignant transformation. Although the cause of fibrosis is unknown, the possibility of an immune reaction to naevus cells is postulated.

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The pathologist's approach to the diagnosis of metabolic disease

Ridaura-Sanz¹

1994

Pathology - Research and Practice

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Early clinical, histological, and immunohistochemical findings in suspected acute graft‐versus‐host disease and their association with patient outcomes

García‐Romero¹,

Sáez‐de‐Ocariz²,

Hernández-Zepeda³

et al. 2020

Pediatric Dermatology

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Background/ObjectivesAcute graft‐versus‐host disease (aGVHD) is a serious condition after allogeneic hematopoietic stem cell transplantation (HSCT), frequently involving skin, gut, and liver. It can be difficult to diagnose early, yet this is vital for adequate management. We sought to identify initial clinical and histopathological features in children with suspected GVHD and the association with clinical course and outcomes.MethodsRetrospective study of patients with skin biopsies for suspected aGVHD from 2006 to 2016. We collected demographic and clinical information, histologic, and immunohistochemical (IHC) findings, and outcomes during follow‐up. Bivariate and multivariate analyses were done to identify risk factors associated with remission, development of severe/life‐threatening aGVHD, and mortality.ResultsWe included 42 patients, 15 females. Skin manifestations occurred 51 days (median) after HSCT. On biopsy, 76.2% had mild (stage 1‐2) skin aGVHD; during the course of the disease, severity and systemic involvement increased to global grade III/IV in 66.6%. All patients received treatment; 15 are in remission from aGVHD and 23 have died. Histologic features were diagnostic in 83.3%. On bivariate and multivariate analysis, we identified initial clinical and histologic findings that were associated with the measured outcomes: odds of remission from aGVHD were increased when focal vacuolar changes were found on skin biopsy (OR 6.028; 95%CI:1.253‐28.992) but decreased by initial hepatic aGVHD (OR 0.112; 95%CI: 0.017‐0.748); severe/life‐threatening aGVHD was associated with initial gastrointestinal aGVHD (OR 6.054; 95%CI:1.257‐29.159); and odds of mortality were decreased with male donor (OR 0.056; 95%CI:0.004‐0.804), nulliparous female donor (OR 0.076; 95%CI:0.009‐0.669), and focal vacuolar changes on skin biopsy (OR 0.113; 95%CI:0.017‐0.770).ConclusionsWe found novel indicators predictive of remission, severity, and mortality in children with aGVHD. Further studies of this condition in children are needed.

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Expression of p53 in pediatric lymphomas from Mexico

Venkatesh¹,

Meza-Coria²,

López-Corella³

et al. 1997

Int J Oncol

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C Ridaura-Sanz

Scleroderma ‘en coup de sabre’ and progressive facial hemiatrophy. Is it possible to differentiate them?

Desmoplastic hairless hypopigmented naevus: a variant of giant congenital melanocytic naevus

The pathologist's approach to the diagnosis of metabolic disease

Early clinical, histological, and immunohistochemical findings in suspected acute graft‐versus‐host disease and their association with patient outcomes

Expression of p53 in pediatric lymphomas from Mexico

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