Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:1.1.1.1 (
alcohol dehydrogenase
)
9,284
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The patient was a 63-year-old male admitted for further evaluation of the bleeding esophageal tumor. Endoscopic biopsy revealed small cell carcinoma. CT scan of the abdomen demonstrated nodular enlargement at the celiac axis. Under diagnosis of small cell carcinoma of the esophagus at Stage IVa, neoadjuvant chemotherapy with FP (5-FU+CDDP) was given. Immediately after fluid load, levels of serum sodium decreased to 117 mEq/L and persisted during chemotherapy treatment despite aggressive corrections. Response and shrinkage of the distant
nodal
metastases were confirmed, and an esophagectomy was conducted. Pathological examination with IHC demonstrated positive staining for CD56, NSE and synaptophysin but negative for
ADH
. Lymph node and liver metastases recurred. Progression of the disease again triggered hyponatremia.
...
PMID:[A case of small cell carcinoma of the esophagus with SIADH]. 2008 45
Retinoic Acid (RA) is a small lipophilic signaling molecule essential for embryonic development and adult tissue maintenance. Both an excess of RA and a deficiency of RA can cause pathogenic anomalies, hence it is critical to understand the mechanisms controlling the spatial and temporal distribution of RA. However, our current understanding of these processes remains incomplete. Vitamin A is metabolized to RA via two sequential enzymatic reactions. The first requires retinol dehydrogenase (RDH) activity to oxidize Vitamin A (retinol) to retinal, and the second requires retinaldehyde activity (RALDH) to oxidize retinal into RA. The first reaction has previously been attributed to the
alcohol dehydrogenase
(
ADH
) family, whose genes are ubiquitously or redundantly expressed. Consequently, the specificity of RA synthesis was thought to reside exclusively at the level of the second reaction. To better understand the metabolism of Vitamin A into RA during embryogenesis, we generated new mouse models that disrupt this process. Here we describe a new targeted knockout of Rdh10 in which RA synthesis is severely impaired, particularly at critical early embryonic stages. We also introduce a new mutant allele of Aldh1a2. Both mutations produce similar developmental defects resulting in lethality around embryonic day 10.5 (E10.5). The severity of the Rdh10 null phenotype demonstrates that embryonic oxidation of retinol is carried out primarily by RDH10 and that neither ADHs nor other enzymes contribute significantly to this reaction. We also show that reduced RA production results in upregulation of Rdh10. These data demonstrate that RDH10 plays a critical role in mediating the rate limiting RDH step of Vitamin A metabolism and functions as a
nodal
point in feedback regulation of RA synthesis. Moreover, RDH10-mediated oxidation of retinol plays as important a role in the control and regulation of RA production during embryogenesis as does the subsequent RALDH-mediated reaction.
...
PMID:RDH10 oxidation of Vitamin A is a critical control step in synthesis of retinoic acid during mouse embryogenesis. 2231 78
The evolutionary relationships between
Peromyscus
,
Habromys
,
Isthmomys
,
Megadontomys
,
Neotomodon
,
Osgoodomys
, and
Podomys
are poorly understood. In order to further explore the evolutionary boundaries of
Peromyscus
and compare potential taxonomic solutions for this diverse group and its relatives, we conducted phylogenetic analyses of DNA sequence data from
alcohol dehydrogenase
(
Adh
1-I2), beta fibrinogen (
Fgb
-I7), interphotoreceptor retinoid-binding protein (
Rbp
3), and cytochrome-
b
(
Cytb
). Phylogenetic analyses of mitochondrial and nuclear genes produced similar topologies although levels of
nodal
support varied. The best-supported topology was obtained by combining nuclear and mitochondrial sequences. No monophyletic
Peromyscus
clade was supported. Instead, support was found for a clade containing
Habromys
,
Megadontomys
,
Neotomodon
,
Osgoodomys
,
Podomys
, and
Peromyscus
suggesting paraphyly of
Peromyscus
and confirming previous observations. Our analyses indicated an early divergence of
Isthmomys
from
Peromyscus
(approximately 8 million years ago), whereas most other peromyscine taxa emerged within the last 6 million years. To recover a monophyletic taxonomy from
Peromyscus
and affiliated lineages, we detail 3 taxonomic options in which
Habromys
,
Megadontomys
,
Neotomodon
,
Osgoodomys
, and
Podomys
are retained as genera, subsumed as subgenera, or subsumed as species groups within
Peromyscus
. Each option presents distinct taxonomic challenges, and the appropriate taxonomy must reflect the substantial levels of morphological divergence that characterize this group while maintaining the monophyletic relationships obtained from genetic data.
...
PMID:What Is
Peromyscus
? Evidence from nuclear and mitochondrial DNA sequences suggests the need for a new classification. 2693 47
