Mia McKinstry scite author profile

The honey bee is of paramount importance to humans in both agricultural and ecological settings. Honey bee colonies have suffered from increased attrition in recent years, stemming from complex interacting stresses. Defining common cellular stress responses elicited by these stressors represents a key step in understanding potential synergies. The proteostasis network is a highly conserved network of cellular stress responses involved in maintaining the homeostasis of protein production and function. Here, we have characterized the Heat Shock Response (HSR), one branch of this network, and found that its core components are conserved. In addition, exposing bees to elevated temperatures normally encountered by honey bees during typical activities results in robust HSR induction with increased expression of specific heat shock proteins that was variable across tissues. Surprisingly, we found that heat shock represses multiple immune genes in the abdomen and additionally showed that wounding the cuticle of the abdomen results in decreased expression of multiple HSR genes in proximal and distal tissues. This mutually antagonistic relationship between the HSR and immune activation is unique among invertebrates studied to date and may promote understanding of potential synergistic effects of disparate stresses in this critical pollinator and social insects more broadly.

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Definitive hematopoietic stem cells minimally contribute to embryonic hematopoiesis

Ulloa

Habbsa

Potts

et al. 2021

Cell Reports

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Hematopoietic stem cells (HSCs) are rare cells that arise in the embryo and sustain adult hematopoiesis. Although the functional potential of nascent HSCs is detectable by transplantation, their native contribution during development is unknown, in part due to the overlapping genesis and marker gene expression with other embryonic blood progenitors. Using single-cell transcriptomics, we define gene signatures that distinguish nascent HSCs from embryonic blood progenitors. Applying a lineage-tracing approach to selectively track HSC output in situ, we find significantly delayed lymphomyeloid contribution. An inducible HSC injury model demonstrates a negligible impact on larval lymphomyelopoiesis following HSC depletion. HSCs are not merely dormant at this developmental stage, as they showed robust regeneration after injury. Combined, our findings illuminate that nascent HSCs self-renew but display differentiation latency, while HSC-independent embryonic progenitors sustain developmental hematopoiesis. Understanding these differences could improve de novo generation and expansion of functional HSCs.

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Intrahepatic microbes govern liver immunity by programming NKT cells

Leinwand¹,

Paul²,

Chen³

et al. 2022

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The gut microbiome shapes local and systemic immunity. The liver is presumed to be a protected sterile site. As such, a hepatic microbiome has not been examined. Here, we showed a liver microbiome in mice and humans that is distinct from the gut and is enriched in Proteobacteria. It undergoes dynamic alterations with age and is influenced by the environment and host physiology. Fecal microbial transfer experiments revealed that the liver microbiome is populated from the gut in a highly selective manner. Hepatic immunity is dependent on the microbiome, specifically Bacteroidetes species. Targeting Bacteroidetes with oral antibiotics reduced hepatic immune cells by ~90%, prevented APC maturation, and mitigated adaptive immunity. Mechanistically, our findings are consistent with presentation of Bacteroidetes-derived glycosphingolipids to NKT cells promoting CCL5 signaling, which drives hepatic leukocyte expansion and activation, among other possible host-microbe interactions. Collectively, we reveal a microbialglycosphingolipid -NKT -CCL5 axis that underlies hepatic immunity.

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Divergent forms of endoplasmic reticulum stress trigger a robust unfolded protein response in honey bees

Johnston

Hooks

McKinstry

et al. 2016

Journal of Insect Physiology

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Retained metabolic activity in honey bee collected pollen has implications for pollen digestion and effects on honey bee health

et al. 2020

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The mechanisms by which pollen is digested by honey bees are incompletely understood. Potential methods are thought to include pseudogermination, mechanical disruption, enzymatic breakdown, or osmotic shock. Understanding the role of pseudogermination in this process has been hampered by a lack of tools demonstrating retention of metabolic activity in pollen collected by honey bees. Here, we show that pollen collected by honey bees produces reactive oxygen species (ROS) at robust levels upon germination, suggesting that ROS is a suitable marker of this process in pollen. ROS can be readily found in the digestive tract of honey bees and is localized to pollen grains within the lumen. Finally, manipulating pollen levels in the midgut can change ROS levels in the digestive tract. These data provide evidence of retained metabolic activity in bee-collected pollen that lends support to pseudogermination as a mechanism for pollen digestion in honey bees, and points to novel approaches for better understanding of pollen digestion in this species and beyond.

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Mia McKinstry

The heat shock response and humoral immune response are mutually antagonistic in honey bees

Definitive hematopoietic stem cells minimally contribute to embryonic hematopoiesis

Intrahepatic microbes govern liver immunity by programming NKT cells

Divergent forms of endoplasmic reticulum stress trigger a robust unfolded protein response in honey bees

Retained metabolic activity in honey bee collected pollen has implications for pollen digestion and effects on honey bee health

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